Guidelines JPsychopharm
21(1) (2007) 10–41 2007 British Association
hyperactivity disorder in adolescents in ISSN 0269-8811
SAGE Publications Ltd,London, Thousand Oaks,
adults: recommendations from the British Association for Psychopharmacology
D. J. Nutt Psychopharmacology Unit, University of Bristol, Bristol, UK. K. Fone University of Nottingham, Nottingham UK. P. Asherson MRC Social Genetic Developmental Psychiatry, Institute of Psychiatry, King’s College London, UK. D. Bramble Telford & Wrekin PCT, Shrewsbury, UK. P. Hill London, UK. K. Matthews University of Dundee, Dundee UK. K. A. Morris c/o Psychopharmacology Unit, University of Bristol, Bristol, UK. P. Santosh Institute of Psychiatry, London, UK. E. Sonuga-Barke University of Southampton, Southampton, UK. E. Taylor Institute of Psychiatry, London, UK. M. Weiss University of British Columbia, Vancouver, Canada. S. Young Bethlem Royal Hospital, Kent, UK.
For the Consensus Group (other invited participants at the consensus meeting ‘ADHD in transitionfrom child to adult’ are listed in the Acknowledgements). Abstract
Attention-deficit/hyperactivity disorder (ADHD) is an established
growing literature on ADHD in older age groups. Much of this initial
diagnosis in children, associated with a large body of evidence on the
guidance on managing ADHD in adolescents in transition and in adults is
benefits of treatment. Adolescents with ADHD are now leaving children’s
based on expert opinion derived from childhood evidence. We hope that,
services often with no readily identifiable adult service to support them,
by the time these guidelines are updated, much evidence will be
which presents problems as local pharmacy regulations often preclude
available to address the many directions for future research that are
the prescription of stimulant drugs by general practitioners (GPs). In
addition, adults with ADHD symptoms are now starting to present toprimary care and psychiatry services requesting assessment and
Keywords
treatment. For these reasons, the British Association for
ADHD, hyperkinetic disorders, hyperactivity, impulsivity,
Psychopharmacology (BAP) thought it timely to hold a consensus
psychostimulants, psychotherapy, co-morbidities
conference to review the body of evidence on childhood ADHD and the
Corresponding author: Prof. David J. Nutt, Psychopharmacology Unit, Dorothy Hodgkin Building, Whitson St, Bristol BS1 3NY, UK. ADHD management in adolescents to adultsIntroduction
quate, or otherwise to flag the area as a direction for futureresearch. A draft of the taped proceedings was drawn up by an
In recent years, UK health services have proven inadequate in
attending clinician writer and circulated to all speakers and other
meeting the needs not only of children with ADHD in transition
participants for comment. Key subsequent publications were
from children’s services, but also of the growing number of adults
added by the writer and speakers at draft stage. All comments
newly presenting with ADHD symptoms, often after their child
were incorporated as far as possible in the final document, which
has been given the diagnosis. Specialist services are now being
represents the views of all participants, although the authors take
established to manage adolescents in transition and adults with
final responsibility for the document.
ADHD. The BAP thought it helpful to act as the vehicle to prepare
Categories of evidence for causal relationships, observational
a consensus document on best practice in an area that is both con-
relationships and strength of recommendations are given in Table 1
and are taken from Shekelle et al. (1999). The strength of
The BAP is an association of psychiatrists, psychopharmacolo-
recommendation reflects not only the quality of the evidence, but
gists and pre-clinical scientists who are interested in the broad
also the importance of the area under study. For example, it is pos-
field of drugs and the brain. BAP is the largest national organ-
sible to have methodologically sound (category I) evidence about
ization of its kind worldwide, and publishes the Journal of Psy-
an area of practice that is clinically irrelevant, or has such a small
chopharmacology. The association started publishing consensus
effect that it is of little practical importance and therefore attracts a
statements more than a decade ago, and the first BAP guidelines
lower strength of recommendation. However, more commonly, it
on depression were considered a landmark publication when pub-
has been necessary to extrapolate from the available evidence (e.g.
lished in 1993 (Montgomery et al., 1993). That document, which
in childhood) leading to weaker levels of recommendation (B, C
was updated in 2000 (Anderson et al., 2000), has become the stan-
or D) based upon category I evidence statements.
dard of care in many countries because it is considered an accessi-ble consensus to guide practising psychiatrists. The BAP now has
a target of publishing one consensus statement per year in theJournal of Psychopharmacology. Recent guidelines have covered
Our intention is to present a comprehensive statement to guide cli-
management of bipolar disorder (Goodwin, 2003) and drug treat-
nicians, who are managing adolescents with ADHD in transition
ments for addiction (Lingford-Hughes et al., 2004), with guide-
from children’s services, and adults newly presenting with ADHD
lines on anxiety published late last year (Baldwin et al., 2005).
symptoms. Although rigorous evidence exists in a few areas,
Forthcoming consensus conferences are planned on child psy-
overall there is a dearth of evidence that pertains to adolescents
chopharmacology, old age psychopharmacology and schizo-
and especially adults. Many of the statements in this document are
phrenia, all of which will utilize a similar style and process.
therefore based on the experience of experts who are currently
All guidelines are available via the BAP website
treating this adolescent or adult group, with extrapolation from the
(http://www.bap.org.uk) and the intention is to update each guide-
greater body of rigorous data in children. We anticipate that the
situation with regard to research on adult ADHD is likely tochange markedly in the future. Until that time, these guidelines
must be considered a first attempt to reach consensus in an areathat continues to attract controversy, and in which we cannot be
A consensus conference was held at the Novartis Foundation
certain that childhood findings will be confirmed in older age
building, London on 24 February 2005. The meeting was spon-
groups. We hope that the body of evidence may be considered far
sored by unrestricted educational grants from Cephalon, Janssen,
more definitive when these guidelines are due for updating.
Lilly, Shire UK and Shire US pharmaceutical companies, which
Our consensus on adolescents in transition and adults with
had no input into and no responsibility for the meeting and its
ADHD is based on the premise that a clinical entity, ADHD,
content. Those invited to attend the meeting included BAP
exists in childhood and, moreover, that the condition may persist
members, representative clinicians from services with a strong
in some form in older age groups. The meeting recognized the fact
interest in ADHD, and other recognized experts and advocates in
that even ADHD in childhood is a controversial diagnosis to make
the field, including a representative from Canada who had recently
in some quarters of society; thus, a diagnosis in older age groups
participated in that country’s consensus statement on adult ADHD
might be more controversial in these quarters. The crux of the con-
(www.caddra.ca). Observers from the sponsoring companies were
troversy seems to be whether the symptoms of ADHD need to be
invited to attend but not to participate in the proceedings or in
understood as a medical condition or whether the behaviours iden-
drafting the guidelines. All attendees completed conflict of interest
tified as ADHD are an extreme of the normal spectrum of human
statements that are held at the BAP office as per usual BAP policy.
behaviours (e.g. ‘very naughty little boys’). A further dimension is
Speakers were asked to present a review of the literature and
whether such behaviours necessitate pharmacological treatment or
identification of the standard of evidence in their area, with an
whether non-pharmacological modifications are sufficient to
emphasis on meta-analyses, systematic reviews and randomized
controlled trials (RCTs) where available. Each presentation was
The consensus of the meeting is that the extreme behaviours
followed by a lengthy discussion that aimed to reach consensus
characterized under current diagnostic systems represent a clinical
where the evidence and/or clinical experience was considered ade-
condition in so much as the behaviours cause problems for the
ADHD management in adolescents to adults
Categories of evidence and strength of recommendations
Categories of evidence for causal relationships and treatment
Evidence from meta-analysis of randomized controlled trials
Evidence from at least one randomized controlled trial
Evidence from at least one controlled study without randomization
Evidence from at least one other type of quasi-experimental study
Evidence from non-experimental descriptive studies, such as comparative studies, correlation studies and case-control studies
Evidence from expert committee reports or opinions and/or clinical experience of respected authorities
Categories of evidence for observational relationships
Evidence from large, representative population samples
Evidence from small, well-designed, but not necessarily representative samples
Evidence from non-representative surveys, case reports
Evidence from expert committee reports or opinions and/or clinical experience of respected authorities
Directly based on category II evidence or extrapolated from category I evidence
Directly based on category III evidence or extrapolated from category II evidence
Directly based on category IV evidence or extrapolated from category III evidence
affected individual, are identified as problematic by others and
marked disparities between subgroups. This may indicate that cau-
may respond to various forms of clinical treatment or other forms
sation is likely to show marked heterogeneity, and/or that tradi-
of management, such as environmental restructuring. A diagnosis
tional theories on cause and effect in ADHD, that regard ADHD
of ADHD is thus warranted to allow affected individuals to access
as a homogeneous condition characterized by a single causal
appropriate forms of support from health care and other systems.
pathway, are inadequate (Sonuga-Barke, 2003, 2005; Coghill
We hope the controversy will be lessened over ADHD in older
et al., 2005; Castellanos et al., 2006).
age groups, because in many cases, the affected individual will bethe one to initiate clinical contact. Indeed, it is partly in response
to the growing number of such requests that this consensusmeeting was arranged.
ADHD is highly heritable, with heritability estimates from twin
With current science, it is not possible to determine whether
studies in the range of 65–90% (Thapar et al., 2001) and average
ADHD is an extreme variant of normal behaviour or in a distinct
across 20 studies of 76% (Faraone et al., 2005b). Family studies
category. However, current science does support the improvement
report that both parents and siblings of a child with ADHD are
of ADHD symptoms with treatments, particularly but not exclu-
around four to five times more likely to have ADHD than the
sively pharmacological. It is in this spirit that this consensus docu-
general population (Faraone et al., 2000). Although ADHD is
ment is presented. The question of who should provide and pay for
diagnosed using operational diagnostic criteria, measures of
service provision is a matter of health policy and thus beyond the
ADHD symptoms are continuously distributed in the general
scope of our consensus, although we hope that this consensus will
population. Mathematical modelling using De Fries and Fulker
(DF) analysis supports the hypothesis that ADHD is the extremeof behaviours that vary genetically throughout the entire popu-lation (Gjone et al., 1996; Levy et al., 1997; Willcutt et al., 2000;
Neurodevelopmental background
Price et al., 2001). These data suggest that genetic influences onADHD are distributed throughout the population and correlate
The exact cause(s) of ADHD are unknown but the growing liter-
with quantitative trait measures of ADHD symptoms. This is
ature on genetics, neuroimaging and neuropsychology suggests
important since this implies that ADHD is best perceived as a
features consistent with a neurodevelopmental condition in which
quantitative trait, or series of quantitative traits, rather than a cate-
multiple environmental and biological factors, of individually
gorical disorder. The implication for clinical practice is that,
small effect, interact to produce an abnormal brain condition that
similar to other common psychiatric disorders such as anxiety and
manifests as cognitive and behavioural deficits (Sonuga-Barke
depression, appropriate clinical cut-offs need to be established that
et al., 2005). Subsequent bidirectional interactions then occur
link ADHD symptoms to significant clinical impairments; given
between these deficits and environmental and biological factors to
that ADHD is a developmental disorder, this will require estab-
modify the phenotype further, resulting in various diagnostic sub-
lishment of age- and gender-specific norms. A particular issue for
groups under the umbrella term ADHD. Overall, the literature on
the diagnosis of ADHD in adults is that the age-appropriate
genetic, neurobiological and neuropsychological deficits shows
expression of clinical symptoms has yet to be firmly established. ADHD management in adolescents to adults
Genetic influences on ADHD are likely to be the result of mul-
tiple genes of small effect size and are expected to interact withenvironmental risk factors (Asherson et al., 2005). Four linkage
Detailed coverage of the diverse literature on the influence of
scans have been completed and highlight a number of potential
environmental factors was beyond the scope of the meeting and
chromosomal regions containing genes that increase risk for
thus is briefly reviewed in this document. It is noted that environ-
ADHD, although there is as yet no clear consensus across the
mental factors of significance include pregnancy and birth factors,
various data sets, and no genes have been identified that account
prematurity, diet, institutional care and other aspects of the
for linkage signals (Fisher et al., 2002; Smalley et al., 2002;
psychosocial environment (see Biederman, 2005 for a recent
Bakker et al., 2003; Ogdie et al., 2003; Arcos-Burgos et al., 2004;
review). Several studies also suggest that childhood environmental
Ogdie et al., 2004; Hebebrand et al., 2005). Genetic association
factors shape the phenotypic expression of ADHD, and co-
studies have focused on the analysis of monoamine system genes,
morbidity with other behavioural disorders, by acting on genetic
due to the marked and rapid response of ADHD symptoms to stim-
influences (e.g. Hudziak et al., 2005; Burt et al., 2005; Dick et al.,
ulants that block the reuptake of dopamine and norepinephrine (see
2005; Jester et al., 2005 I–II). Furthermore, predictors of persist-
later). Several genes have been reported to be associated with
ence into adulthood include family history of ADHD, psychiatric
ADHD in multiple studies, with small but significant effects con-
co-morbidity and psychosocial adversity (Biederman, 2005). In
firmed by meta-analysis (Asherson et al., 2005; Faraone et al.,
terms of treatment, various dietary manipulations can improve
2005b, Thapar et al., 2005a). The best evidence for association is
ADHD symptoms in at least some children (Egger et al., 1985;
with DNA variants of the dopamine D4 (DRD4) and D5 (DRD5)
Carter et al., 1993; Boris and Mandel, 1994; Rowe and Rowe,
receptors and the dopamine transporter (DAT1), with strong addi-
1994; Schmidt et al., 1997; Dykman and Dykman, 1998; Richard-
tional evidence for associations with the serotonin IB receptor
son and Puri, 2002 Ib), although the mechanism of these improve-
(5-HT ), serotonin transporter (SERT) and synaptosomal associ-
ments is unknown. Activities in natural ‘green’ settings have been
ated protein-25 (SNAP-25). Gene–environment interactions have
linked with symptom improvement in a national sample (Kuo and
been reported between DAT1 and maternal use of tobacco (Kahn
Taylor, 2004 I). These and other findings (e.g. that brain abnor-
et al., 2003) and alcohol (Brookes et al., 2006) during pregnancy
malities may not determine phenotype (Castellanos et al., 2002
on the risk of ADHD, and between catechol O-methyltransferase
IIa)) could suggest a greater importance of environmental factors
and low birth weight on risk for antisocial outcomes among ADHD
in some individuals, both in childhood and in older age groups.
cases (Thapar et al., 2005b). Although most studies have focused
Environmental restructuring might be particularly important as
on children with ADHD, it is interesting to note that the only two
part of the management of adults with ADHD, in our experience
studies to investigate the DRD4 association in adults with ADHD
(see ‘Psychotherapeutic approaches’ below).
were both positive (Muglia et al., 2000; Lynn et al., 2005).
Neuroimaging studies (Bush et al., 2005) have documented
significant overall and regional reductions in white matter volumesbetween unmedicated ADHD patients, including those never
Neuropsychological research, mainly in children, has documented
exposed to relevant medication, and healthy controls (Castellanos
various deficits in executive function (especially inhibition), moti-
et al., 2002). Medicated patients differ from unmedicated patients,
vation and reinforcement, attention, timing, memory and energet-
but not from healthy controls, in overall and regional (frontal,
ics (covered in detail in ‘Neuropsychological assessment’ below
parietal and temporal) white matter volumes. These studies have
(Doyle et al., 2005)). This research has clarified that although
clearly demonstrated differences in the anatomy and processing of
about a third of patients have difficulties with one or another neu-
patients with ADHD compared with controls, although these dif-
ropsychological test of executive functioning, this is neither uni-
ferences do not have the sensitivity or specificity in individuals to
versal nor diagnostic. Functional neuroimaging studies have often
contribute to differential diagnosis (Seidman et al., 2005).
suggested that brain activation is abnormal during affected tasks
Several neuroimaging studies, though not all (van Dyck et al.,
compared with controls, and specifically is more diffuse than in
2002), have indicated that striatal DAT binding is increased com-
controls with failure of inhibitory functions. For example, Tamm
pared with controls in ADHD patients (Krause et al., 2000;
et al. (2004) have linked a key deficit – abnormal response inhibi-
Madras et al., 2002; Spencer et al., 2005a; Volkow et al., 2005)
tion on a Go/No Go task – with abnormal activation patterns in
including studies in adults (Dougherty et al., 1999; Dresel et al.,
specific temporal regions compared with controls. This has led to
2000; Krause et al., 2000), suggesting increased density of the
the hypothesis that individuals with ADHD may have to use other
transporter protein in the striatum. In addition, there is evidence
brain regions, when faced with attention demanding tasks, that are
from two out of four studies that the DAT1 risk genotype for
perhaps less efficient (Bush et al., 2005). Recent evidence also
ADHD is associated with increased striatal DAT binding (Heinz et
suggests that this is reversible with medication. al., 2000; Jacobsen et al., 2000; Martinez et al., 2001; Cheon et
Various studies are aimed at linking the specific neuropsycho-
al., 2003). Moreover, other groups have reported that
logical traits (known as endophenotypes – e.g. delay aversion,
methylphenidate treatment, which increases extracellular
executive motor inhibition, deficit in arousal/activation regulation)
dopamine in the human striatum (Volkow et al., 2001), is accom-
that may underpin symptoms and behaviours, with neurobiological
panied by reductions in DAT binding to control values (Dresel
changes (e.g. dysfunction in frontostriatal circuitry, reward
et al., 2000; Spencer et al., 2005a; Volkow et al., 2005).
systems and catecholamine function (Waldman, 2005; Willcutt etADHD management in adolescents to adultsal., 2005)). The effects of the identified genetic variants on brain
ing the DSM-IV definition of ADHD in partial remission were
functioning and resultant phenotypic traits remain unclear, so the
included, referring to the persistence of some symptoms associ-
possibility remains that such variants could contribute to several
ated with significant clinical impairments. Prevalence rates of
phenotypes of which one is currently classified as ADHD.
adult ADHD estimated at around 4% have been found in several
Finally, neuropsychological deficits neither consistently predict
different studies, using DSM-IV criteria, but will vary depending
behaviours nor outcome of treatment (e.g. Rhodes et al., 2004,
on clinical measures used and the precise way in which the diag-
2005). This could reflect a lack of specificity of the deficit tested
nostic criteria are applied (Hill and Schoener, 1996; Gallagher and
to the diagnostic group under study or the fact that treatment effi-
Blader, 2001; Bloom and Dey, 2004; Faraone and Biederman,
cacy is not mediated via those structures and functions involved in
2005; Kooij et al., 2005; Kessler et al., 2006; Faraone et al.,
While some symptoms (e.g. hyperactivity) tend to diminish or
present differently with age, perhaps due to self-medication, adap-tation and neurodevelopment, other symptoms, especially inatten-
Several major prospective follow-up studies have documented the
tion, (Millstein et al., 1998) are more likely to persist and may
natural history of ADHD, especially as patients transit through
have a greater impact on adults. Community follow-up of young
adolescence into adulthood (Hechtman and Weiss, 1983; Barkley
people with untreated ‘hyperactivity’ suggests that impulsiveness
et al., 1990; Weiss and Hechtman, 1993; Biederman et al., 1996a;
declines in absolute terms, but remains deviant relative to that of
Biederman et al., 1996b; Faraone et al., 1996; Biederman et al.,
age-matched peers (Taylor et al., 1996). These studies have inves-
1998; Mannuzza et al., 1998; Mick et al., 2004; Faraone et al.,
tigated the frequency of these symptoms in adults but no study to
2006). These studies suggest that a large proportion of child
date has evaluated the relative impairment caused by continuation
patients show ADHD symptoms that persist to adolescence (esti-
of the various symptoms that do remain in the adult population.
mated variously at 50–60%) or adulthood (10–66%; Hill and
Attentional difficulties are likely to persist at least in their impact
Schoener, 1996; Spencer et al., 1996; Faraone et al., 1996; Bieder-
on functioning. Symptoms diminish in frequency and severity as a
man et al., 2000; Barkley, 2002; Faraone et al., 2006). A recent
consequence of natural developmental processes seen in all chil-
meta-analysis of studies that followed children identified with
dren and may further diminish, at least in part, due to learned
ADHD and matched controls into adulthood has been completed
skills, coping strategies and environmental restructuring.
(Faraone et al., 2006). When the definition of ADHD included
However, the overall impact may worsen due to the increased
only those that met full diagnostic criteria for ADHD, the rate of
demands of an adult environment. While the full complement of
persistence was approximately 15% at age 25 years. However the
diagnostic deficits can often disappear in adulthood, at an age-
rate was far higher, approximately 65%, when individuals fulfill-
related rate dependent on criteria, impairment persists and may
Consensus: ADHD as a neurodevelopmental condition •
ADHD is a neurodevelopmental psychiatric condition that most likely results from the interaction of multiple genetic andenvironmental factors, each of small effect, with different patterns creating multiple pathways to symptoms each marked andmediated by different deficit profiles (B).
ADHD is currently understood to be a life-long condition and currently a diagnosis of adult ADHD needs to include childhoodimpairment (either prospectively or retrospectively) (C). The status of disorder of later onset needs to be established.
In the absence of specific markers common to the entire group of ADHD patients, assessment and treatment are guided by phe-notype (symptoms/behaviours/impairments).
Co-morbidity is common in both childhood and adulthood, and may determine outcomes (D). Clinical assessment of ADHDneeds to include careful evaluation for other disorders.
Expression of ADHD and co-morbidities is highly heterogeneous, thus management needs to be individualized (C). Key uncertainties •
A better aetiological theory is needed that accounts for the causal heterogeneity in the condition (Coghill et al., 2005; Sonuga-Barke, 2005)
Is ADHD a categorical difference or the end of spectrum of a population trait?
How does phenotype match to genetic, neuropsychological and neuroimaging markers?
What are the best ways to subdivide ADHD into subtypes?
What underpins the relation between ADHD and environmental factors, such as diet and sleep?
How many adults with adult ADHD currently receive alternative diagnoses and treatments within adult psychiatric andprimary care services?
Should screening of parents and children of referred patients be considered, and what would be the resource implications ofthis?
ADHD management in adolescents to adults
worsen in a subset. In such patients, impairment is usually pervasive
not considered sufficient to make a diagnosis of ADHD; although
or affects more than one domain of activities and may manifest as:
the criteria for hyperkinetic disorders better predicts treatment
educational, organizational or occupational failures; substance use
response than the criteria for ADHD, treatment response varies
disorders and other dependent, risky, antisocial or forensic behav-
between individuals, while other disorders can respond to current
iours; emotional and relationship difficulties and increased medical
morbidity (Millstein et al., 1998; Swensen et al., 2000).
The two diagnostic systems have various limitations, not least
Co-morbidity is widely considered to be a common finding in
the internal tautology that the definition of ADHD or hyperkinetic
adolescent and adult ADHD patients, and will affect outcomes
disorders rests solely on the criteria that have been established.
(see ‘Comorbid disorders and special situations’). Epidemiological
For example, the possibility exists that boys are diagnosed with
and clinical studies have shown that more than 80% of adults with
ADHD more often than girls because the diagnostic criteria relate
ADHD will have another disorder, and the finding that co-morbid-
to disruptive behaviours as markers that are more prevalent in
ity in adults is similar to that in children, but increases with time,
male children. Importantly, these systems do not include associ-
raises the question of whether some of this co-morbidity may be
ated symptoms, reported by patients which could arguably be the
driven by untreated ADHD. Common co-morbid disorders in
adulthood include anxiety, depression and antisocial behaviourdisorders, and persisting neurodevelopmental disorders such as
dyslexia (Heiligenstein and Keeling, 1995; Biederman et al.,1996b; Marks et al., 2001; Biederman, 2004; McGough et al.,
Although DSM-IV-TR and ICD-10 have criteria to diagnose
2005; Kessler et al., 2006). The frequency of self-medication and
childhood ADHD, these have not been adapted to be appropriate
substance use disorders is thought to increase with age but no
to adults – e.g. there is no age adjustment to the criteria appropri-
studies have confirmed this supposition.
ate to adults. The associated symptoms are similar in the two clas-sifications and full criteria are given in the Appendix. Diagnosis and assessment DSM-IV-TR
The DSM-IV-TR (APA, 2000) requires all the
following criteria for a diagnosis of ADHD:
Several issues arise when considering the diagnostic process foradult ADHD. Two major sets of criteria are used worldwide to
Either at least six of nine symptoms of inattention or at least
diagnose conditions characterized by inattention and/or hyperac-
six of nine symptoms of hyperactivity/impulsivity persisting
tivity – the Diagnostic and Statistical Manual of Mental
for at least 6 months to a maladaptive degree, inconsistent
Disorders, fourth edition text revision (DSM-IV-TR, APA, 2000),
with developmental level. DSM-IV-TR allows for ADHD ‘in
which recognizes ADHD, and the International Classification of
partial remission’ that can usefully be applied to adults who
Diseases, tenth edition (ICD-10, WHO, 1992), which encom-
had ADHD and have persistence of some of the symptoms
passes hyperkinetic disorders. Due to differences in criteria, each
associated with continued clinical impairments, but who no
system identifies different clinical entities with different names –
ADHD (APA, 2000) or hyperkinetic disorders (WHO, 1992); the
Some symptoms that caused impairment were present before
latter generally describes a more restricted and severe subset of
DSM-IV combined-type ADHD. We have chosen to use the term
Some impairment from symptoms is present in at least two
ADHD as shorthand for ADHD and hyperkinetic disorders, except
settings (e.g. at home and at school/work).
Clear evidence of clinically significant impairment in social,
In the absence of any definitive and objective test (e.g. genetic
academic or occupational functioning.
or neuropsychological), the purpose of the diagnostic process
Symptoms do not occur exclusively during a pervasive
needs consideration. Currently, diagnosis is a process of identify-
developmental disorder or psychotic disorder and are not
ing extreme behaviour that requires and is amenable to profes-
better accounted for by another mental health disorder.
sional help. However, this process can be used to validateobservers’ views of extreme behaviour rather than to identify
DSM-IV-TR distinguishes three subtypes of ADHD on the basis
markers of an underlying pathological process, with manifesta-
of clinical symptoms: (a) predominantly inattentive type, (b) pre-
tions that map to the label of ADHD. As in most areas of medi-
dominantly hyperactive/impulsive type or (c) combined type
cine, ADHD is diagnosed clinically. The only valid ‘test’ for
(presence of inattention and hyperactivity/impulsivity). These sub-
ADHD is the use of rating scales that have been normed on large
types are defined by the absence of a six of nine symptom cut-off
populations, and can identify whether the child is affected by this
in any one of the domains, although the patient may still have
disorder, other disorders and functional impairment compared
significant symptoms (five of nine), impairment, or be markedly
with age- and gender-matched peers. The use of rating scales com-
discrepant for age and gender norms in the area in which they fail
bined with a developmental history, observation, family and other
risk factors, and impairments consistent with the disorder allows ahigh level of diagnostic certainty between clinicians and predict-
ICD-10
Two types of WHO criteria exist (WHO, 1992) – the
ing response to treatment (Barkley, 2006). Treatment response is
general criteria and the diagnostic criteria for research (DCR),
ADHD management in adolescents to adults
which are more specific than the general criteria and closer to theDSM-IV-TR criteria. The diagnostic basis of ICD-10 hyperkinetic
Proposed BAP extended adult symptom checklist
disorders is the existence of both impaired attention and overactiv-
Lack of attention to detail or carelessness
ity evident in more than one situation (e.g. home, educational set-
Inattention in tasks or activities the patient finds tedious
tings, clinic). The presence or absence of conduct disorder
constitutes the basis for the main subdivision of hyperkinetic dis-
orders – disturbance of activity and attention versus hyperkinetic
Starting many tasks while having difficulty finishing
For the general ICD-10 diagnosis, behavioural problems
should be longstanding and have started before age 6 years. The
Avoidance of, dislike of, or inability to expend sus-
caveat is made that due to wide normal variation in activity, only
extreme degrees of hyperactivity should lead to a diagnosis in pre-
school children. Associated features are not necessary or sufficient
for the diagnosis but help sustain the disorder, including; disinhi-
bition in social relationships, recklessness in situations involving
some danger, and impulsive flouting of social rules (as shown by
Restlessness or an inability to sit still in low-stimulation
intruding on or interrupting others’ activities, prematurely answer-
ing questions before they have been completed or difficulty in
Inappropriate or excessive activity or an internal feeling
Difficulty keeping quiet; talking out of turn
The ICD-10 DCR recognizes seven criteria:
Unfocused mental activity; difficulty turning thoughtsoff
Demonstrable abnormalities at home: at least three of five
Blurting out responses; poor social timing in dialogue
problems of inattention, at least three of five problems of
Trouble waiting if there is nothing to do
hyperactivity, at least one of three problems of hyperactivity.
Demonstrable abnormalities at school or nursery: at least two
of four attentional problems and at least three of five activity
Directly observed abnormality of attention or inactivity.
Does not meet criteria for pervasive developmental disorders,mania, depressive or anxiety disorder.
purposes but may be useful in conjunction with a formal clinical
evaluation, or serially to evaluate symptom changes. Several dif-
ferent types of scales may be helpful: screens for adult ADHDsymptoms, screen for co-morbidity (Gadow et al., 1999), and
Thus the DSM-IV-TR criteria identify a broader group of patients
examination of impact of ADHD on functional impairment (Weiss
than the ICD-10 (Tripp et al., 1999). No definitive system exists to
and Weiss, 2004). Generic functioning scales have shown poor
diagnose adult ADHD, while use of these childhood diagnostic
correlation with ADHD symptoms, making it clear that ADHD
systems in adults raises various difficulties, not least the alteration of
specific functional scales are needed (Gordon et al., 2006).
symptoms in adulthood. Thus, the consensus group thought it would
Two shorter scales have been developed to allow a rapid initial
be helpful to present an extended checklist of adult symptoms in this
screen in various clinical settings, and are based on the 18 symp-
document, based on childhood diagnostic symptoms plus additional
toms listed in both the DSM-IV-TR and the ICD-10 DCR criteria.
adult symptoms (APA, 2000; WHO, 1992; Wender, 1995).
The six-item Adult ADHD Self-Report Scale screener (ASRS-v1.1, Adler et al., 2004; Kessler et al., 2005) is patient-rated while
Rating scales
Various rating scales have been developed to help
the ADHD Rating Scale (ADHDRS-IV-Inv, Adler et al., 2005b) is
diagnose adult ADHD, including three self-report scales. The 61-
clinician administered with good reliability and moderate
item Wender Utah Rating Scale focuses on retrospective symp-
agreement between raters. The ASRS (available at www.med.
toms in childhood plus current hyperactivity, inattention and other
nyu.edu/psych/assets/adhdscreen18.pdf) and the Canadian Con-
symptoms. It relies on retrospective recall by the individual but
sensus screening checklist (www.caddra.ca) are given in the
has been validated against parent report and found to be reliable
Appendix. Other scales can be downloaded from www.caddra.ca
(Ward et al., 1993). Others include the Adult Self Report Scale
(Adler et al., 2004; Kessler et al., 2005), Conners Adult ADHDRating Scale (Conners et al., 1998), the 40-item Brown Adult
Attention Deficit Disorder Scale (Brown, 1996) and the BarkleySelf, Other and Past ADHD symptom checklists (Barkley and
Many studies in children but few in adolescents have documented
Murphy, 2006). None of these scales is sufficient for diagnostic
various deficits of neuropsychological testing. The limited liter-
ADHD management in adolescents to adults
Summary of evidence on neuropsychological assessment
Quality: quantitative review (A); qualitative review (B); no review (C); no studies (D)Quantity: more than ten studies (A); five to ten studies (B); two to four studies (C); one study (D); no studies (E)Strength: I = no effect d < 0.2; II = small effect d 0.2–0.4; III = moderate d 0.4–0.7; IV = large d 0.7–1.0; V = very large d > 1.0Tests are: Continuous Performance Test commission errors; Continuous Performance Test ommission errors; Stop Signal Reaction Times; Spatial workingmemory; Verbal working memory; Tower of London/Hanoi; Trials-B; Stroop interference; Wisconsin card sorting task; Time discrimination; Timereproduction; Interstimulus interval effects; responses to reward, punishment; Choice for delayed rewards
ature in adults reports similar patterns, although marked hetero-
2003, 2005; Coghill et al., 2005). Alternate theories include a
geneity exists (Schoeclin and Engel, 2005; Frazier et al., 2004;
failure of specific response-inhibition mechanisms (Willcutt et al.,
Harvey et al., 2004; Seidman et al., 2004; Nigg, 2005).
2005), altered reward or motivational pathways (Luman et al.,
Commonly reported impairments are found in tasks involving
2005), abnormal processing of time-related cues (Toplak and
executive functions, selective and sustained attention, response
Tannock, in submission), non-working memory (Rhodes et al.,
inhibition, working memory and reward-related motivation. Find-
2004, 2005) and diffuse abnormalities in energetics (Seargant,
ings on specific tests in various domains are shown in Table 2.
2005). Current thinking is that these impairments may reflect dys-
However as suggested above, the traditional neuropsychologi-
regulation in distinct underlying neural circuitries, that is: frontal,
cal model of ADHD, which holds that symptoms are the product
(dorsolateral prefrontal cortex), dorsal and medial striatal function
of a common core deficit expressed by all affected individuals, is
reflecting executive function deficits; cerebellum and its outputs
now contentious (Sonuga-Barke, 2002, 2003, 2005; Castellanos et
affecting timing (with modulation by norepinephrine); ventro-stri-
al., 2006). The emerging consensus is that ADHD is a neuropsy-
atal-prefrontal (orbito-frontal) circuitry affecting reward and pun-
chologically heterogeneous disorder, with different patterns of
ishment processing, motivation and delay aversion (with
impairments seen in different individuals (Sonuga-Barke, 2002,
modulation by dopamine); temporal and amygdalo-hippocampal
ADHD management in adolescents to adults
circuitry affecting non-working memory; and distributed circuitry
individual, which can then be explored further with rating scales,
implicated in abnormal cognitive energetics.
and where indicated neuropsychology. Treatment response is not
While little is known about the value of neuropsychological
thought to be sufficiently specific to form part of the diagnostic
assessment in differential diagnosis in adults and adolescents
(Lovejoy et al., 1999) most studies in children reveal that tests ofexecutive function and attention show good positive predictive
Diagnostic difficulties in adults
power but poor negative predictive power (Barkley et al., 1992;
may be made under several circumstances. The most straight-
Sharma et al., 1991; Grodzinsky and Barkley, 1999; Rielly et al.,
forward scenario is the persistence of symptoms or problem
1999; Doyle et al., 2000; Dickerson Mayes et al., 2001; Berlin et
behaviours in individuals in transition from child and adolescent
al., 2004). Thus, use of such tests alone will lead to false-negative
mental health services. Individuals that present in adulthood may
diagnoses (children without neuropsychological executive impair-
self-report symptoms of ADHD or observations of others. ADHD
ment will still have the condition), which is unsurprising given the
might also be identified through presentation with a co-morbid
heterogeneity of neuropsychological findings.
diagnosis such as substance use disorders or a difficulty in a
The effect of co-morbidities on such tests is not well
domain of functioning (e.g. referral from occupational health serv-
researched. General intelligence testing can be useful to relate IQ
ices). The availability of management strategies suggests the pos-
to the level of academic and occupational achievement and to
sibility of screening – either in the parents or siblings of those
investigate or exclude learning disabilities. However, it raises the
identified with ADHD or in children and adults with problem
issue of labelling based on IQ testing alone. This is particularly
behaviours. This latter strategy might present a potential source of
important for individuals with ADHD since it is possible that IQ
gender bias since a focus on conduct disorder and related behav-
testing results will show increased variation in this group and are
iours might be one explanation of the high male: female ratio
likely to be affected by the attention and motivation of individuals
among children diagnosed with ADHD (Pineda et al., 1999;
and/or by underachievement in education. For example, a recent
Jackson and King, 2004). Some evidence suggests that equal
study of the WISC-IV in 118 children showed the working
numbers of women and men are affected with ADHD as adults
memory tests to be the lowest score in all 118 children, thus low-
(Murphy and Barkley, 1996; Rowland et al., 2002), which raises
ering the overall IQ score secondary to a deficit considered spe-
the possibility that girls with ADHD are underdiagnosed.
cific to ADHD (Mayes and Calhoun, 2006).
Diagnosis of ADHD in adults raises other issues in addition to
Until the heterogeneity of ADHD is better characterized and an
those already identified. The importance of making a diagnosis in
optimal battery of tests in multiple domains is compiled, the prac-
adults is the identification of impairments that are amenable to
tical value of experimental neuropsychological assessment may lie
treatment. Moreover, being given a diagnosis of adult ADHD may
in profiling areas of particular deficits in individual cases, which
help individuals understand why their attainment has failed to cor-
may then help to indicate specific solutions to task-related impair-
relate with that expected of them, but can also reduce self-esteem,
ments, and then to monitor outcomes. Further, neuropsychological
which may itself have an adverse impact on functioning. The diag-
subtyping of patterns of deficits might shed more light on the
nostic and assessment process is further complicated by differ-
underlying pathological processes and potentially help tailor treat-
ences in co-morbidities, which may be a more important focus for
To make a diagnosis of ADHD in adults, current diagnostic
systems require the presence of ADHD symptoms from childhood. Assessment and differential diagnosis
Whilst this is unlikely to be a problem for individuals in transition
The importance of a full clinical assessment needs to be emphas-
from children’s services, presentation for the first time in adult-
ized, including neurodevelopmental history (Weiss and Murray,
hood raises the question of whether ADHD is always a continuum
2003, 2004; Biederman, 2005; Asherson, 2005). It may be worth
from childhood deficits or whether adult-onset ADHD can occur.
setting aside any preconceptions of an individual’s diagnosis from
A view shared by many clinicians is that whilst symptoms are
previous contacts with health services and starting from first prin-
likely to have been present throughout development, there are
ciples, using standard assessment techniques available in psychi-
groups for whom these symptoms only become impairing at
atric services. The presence of ADHD symptoms needs to be
particular stages of development, often around significant trans-
elicited plus symptoms of differential and co-morbid disorders
itions, e.g. from primary to secondary school or from school to
(see also ‘Co-morbid disorders and special situations’), and their
college or to work. Whilst the current diagnostic frameworks
impact on various domains of functioning needs to be assessed.
would not formally recognize these cases as late-onset ADHD,
The differential diagnosis of ADHD includes neurodevelopmental
they will meet all criteria for diagnosis excepting that for onset of
disorders (learning disability, autistic spectrum disorders, commu-
nication difficulties, etc.), anxiety, depression, bipolar disorder,
Another requirement for diagnosis is the number of symptoms
substance use disorders and personality disorders. Some clinicians
reported but, given the natural history of the disorder and other
also advocate a full examination including neurology, since subtle
sources of heterogeneity, many adults may not reach full diagnos-
deficits like gaze instability and word-finding defects have been
tic criteria. Furthermore, adults have a greater ability to adapt to
reported (Weiss and Murray, 2004 IV). The clinical assessment
their environment and the demands that this places on them, which
may generate hypotheses about specific disorders or deficits in an
may alter the ways in which symptoms are expressed. However,
ADHD management in adolescents to adultsRecommendations – diagnosis and assessment Diagnosis in adulthood requires specialist skills – i.e. those used by psychiatrists – but should involve primary care practitioners, who should be trained to be aware of the diagnosis (D). Assessment includes symptoms (past and present), impairments in different contexts, influence of changing demands through life, exclusion of differentials, and application of clinical examination, rating scales and other tools as indicated.
Diagnosis has a major impacts, so the purpose of diagnosis is to identify those who are likely to benefit from treatment optionswhere these are available (D).
Preferable diagnostic and assessment criteria are an extended checklist based on DSM-IV-TR and ICD-10 and adult symptoms(D) (see panel and Appendix).
Assessment needs to confirm impairment in different scenarios: (a) a history of childhood ADHD or suggestive symptoms(impairments/failure of attainment/demands and co-morbidity), (b) current evidence of symptoms leading to pervasive impair-ment in more than one domain (given context demands and skills) (D).
Multiple informants need to be used where possible (at least one contemporary and one developmental) with consent, espe-cially for younger patients (D).
Current neuropsychological tests based solely on executive function are likely to be of limited diagnostic value, though testbatteries that assess multiple domains of neuropsychological performance may be useful to determine individual deficits and tosuggest tailored management strategies (D).
Sensitive use of general intelligence tests can be useful to ascertain potential attainment, and to diagnose co-morbid learningdisabilities (D). Interest, reward and educational achievement are important complicating factors (D).
Clinicians need to be aware of the impact of diagnosis and testing on the individual, particularly on self-esteem (D).
Treatment response cannot be used to make a diagnosis of ADHD (D). Key uncertainties •
What criteria and checklists are required to incorporate better subjective adult symptomatology, to highlight possible neuropsy-chological deficits and to map treatment responses?
What will be the impact of extending the symptom checklists on sensitivity and specificity of diagnosis?
How can the diagnostic process avoid gender and other biases and match to an underlying pathological process reflected insymptoms rather than to external complaints?
What is the practical place of neuropsychology (who to test, with what, and when with what value)?
What can neuropsychological subtyping tell us about different neuropsychological traits (endophenotypes) within ADHD andtheir relationship with causation, behaviours, co-morbidity and treatment responses?
What are the natural history or neurodevelopmental milestones in different domains of neuropsychological functioning espe-cially in relation to transitions between childhood/adolescence and adulthood?
Can a diagnostically useful battery of tests that measures across domains of functioning, be compiled to improve diagnosis?
What are the useful thresholds regarding diagnosis to determine whether symptoms will or will not be amenable to treatment?
Since the current subtypes are based on male child norms that are problematic, what further research is needed on subtypes? Ofnote, the inattentive subtype includes patients who have never had problems with hyperactivity, but also those who have sub-threshold hyperactivity and impulsive symptoms that are representative of the combined type. There are very few patients whoare just hyperactive and no research to indicate that these people are impaired or simply not reporting problems with attention.
some will still have substantial impairments amenable to treat-
thus narrowing diagnostic criteria to those who are actually having
ment, which will not be highlighted by use of diagnostic systems
but rather through a detailed assessment of associated impairments
Use of the current childhood diagnostic systems (APA, 2000;
(Weiss and Murray, 2004). Epidemiological data support the
WHO, 1992) in adults requires validation of ADHD symptomatol-
validity of applying a lower threshold in adults (e.g. four or five
ogy from observers since self-reported symptoms are not included.
out of nine criteria), as this lower threshold correlates significantly
However, individuals who present in adulthood with ADHD
with impairment (Kooij et al., 2005). The emphasis on functional
report their symptoms but may also lack insight into their current
impairment has several effects. First, it permits recognition of the
symptoms (Magnusson et al., 2006). In addition, the need to
need for treatment in those patients who are impaired but subsyn-
collect data on possible impairments as a child raises the possibil-
dromal. Second, it raises questions about the value of treatments in
ity of recall bias in the individual, especially for symptoms such as
patients with symptoms and no evidence of current impairment,
impulsivity and their impact. Use of informants, if available, to
ADHD management in adolescents to adults
report on current and childhood behaviour requires consent and
meta-analysis. Qualitative assessment suggests that all agents are
could be unreliable depending on the nature of the informant and
more effective than placebo and have similar efficacy, although
their relationship to the individual (e.g. partner, parent, employer,
there have been few head-to-head comparisons. Cost-effectiveness
modelling indicates that use of all three agents sequentially is ben-eficial, and although the order of sequential prescribing is not clearon a clinical basis, dexamfetamine would be first line on the basis
Treatment
of cost alone. However, these agents are not equivalent in terms ofside effects (for example, dexamfetamine is considered by many
Physicians identify and treat patients based on symptoms.
to have greater abuse potential than methylphenidate), and the
However, patients come to clinical practice with the hope of func-
response to different agents varies both between individuals and at
tional change, which is the key goal of management. Change in
psychological functioning and functioning in other domains is
The effects of drug treatment require careful monitoring and
essential since ‘pills don’t build skills’ and treatment of inattention
dose adjustment. Scales such as the Clinical Global Adjustment
and other core symptoms is not beneficial if patients have nothing
Scale (Shaffer et al., 1983), the ADHD checklists (Adler et al.,
to do. A package of care needs to be developed from available
2005; Barkley, 2006) and Conners’ scales (Conners et al., 1998)
options on an individual basis after a thorough assessment (Weiss
are useful tools for disease monitoring and service audit. Patients
and Murray, 2004; Asherson, 2005, IV).
and parents should be questioned for concordance over reportedeffects, as well as compliance. Any history of tolerance or diurnal
changes in symptom control should be specifically elicited. Ado-lescents need to be advised of the potential interaction with recre-
Drug treatment for children with ADHD has substantially
ational drugs, including possibly cannabis, although strong
increased in the past decade, in part due to increased recognition
warnings against substance use might need to be balanced against
of the disorder and perhaps also due to changing views on the
the need to engage the patient with treatment. Substance use or
impairment thresholds for drug treatment. In the UK, GP prescrib-
dependence might need to be addressed prior to being able to
ing of methylphenidate has increased sixfold (PPA data www.
publications.doh.gov.uk/prescriptionstatistics/index.htm), although
Various questions remain open over prescribing in childhood,
rates remain about 20 times lower than in the USA for both pre-
and would benefit from future research. Comparable data on cost
scribing and treatment. Therapeutic agents licensed in the UK and
effectiveness of different drugs are lacking, as are data on long-
comparative costs are listed in Table 3, and are all used in primary
term effects, including adverse events and effects on different
care. These agents plus mixed amfetamine salts (Adderall) are
symptom domains, including broader areas of functioning such as
generally available elsewhere. Safety alerts have been issued over
social adjustment. Data are also lacking regarding the effects of
atomoxetine use in childhood, concerning rare hepatotoxicity (one
longer acting preparations on phenomena such as tolerance and
possible case, one probable case in 3.8 million) and, recently,
sensitization. The mechanisms of diurnal and long-term changes
increased suicidal thoughts (five cases out of 1357 cases) or
in symptoms per se are not well understood nor is the basis of
behaviour (one case). All of these rare events are below the preva-
variation in effective medication dosages, though increasing dose
lence of similar events in the general population.
with increasing body size is well recognized. Better outcome
An appraisal for the National Institute for Clinical Excellence
measures are required to assess broader effects, including quality
(NICE, 2006 Ia) has identified 65 acceptable trial reports on the
of life measures because the QALY is inadequate in this scenario.
first-line agents, although most are of low quality, and the hetero-geneity of measures, methods and participants has precluded a
Drug treatment of adults with ADHD is relatively new, having
Agents licensed in children (data from the British National
been prompted by the entry into adult services of people previ-
ously treated in children’s services. However, clinical experience
in specialist adult ADHD clinics suggests that the majority ofadult patients are diagnosed as adults, while most adolescent
patients stop or are taken off medication. While it is not known
whether all findings in children can be extrapolated to adults, psy-
chostimulants have comparable effects in adults as in children and
adolescents (Faraone et al., 2004; Kooij et al., 2004; Spencer
et al., 2005b 1a). Global functioning and adult symptoms such as
unstable mood and ceaseless mental activity are thought to
respond as well to psychostimulants as do other core symptoms(Asherson, 2005).
Note – prices may change and the dosages given are not necessarily
Prescribing and monitoring strategies are no more complex
than those used in the management of children, and can be based
ADHD management in adolescents to adults
on usual approaches utilized in adult services. However, a rigor-
than DAT, (Thomason and Michelson, 2004; Gehlert et al., 1995).
ous approach to diagnosis is warranted since adult patients are per-
Neuroimaging studies in humans have failed to clarify the relative
ceived to present commonly with and be treated for anxiety and
therapeutic benefit resulting from targeting DAT or NET inde-
depression either as the primary disorder or as part of a personality
pendently. In particular, no high-affinity ligands exist to visualize
disorder. It is important that such patients are correctly diagnosed
the norepinephrine transporter in the human brain making it diffi-
and treated within adult psychiatric services, since symptoms can
cult to establish the therapeutic importance of NET inhibition.
respond to treatment. Moreover, specialist services are able to
Nonetheless, imaging studies indicate that methylphenidate binds
monitor treated patients in a similar manner to those with other
strongly to DAT and indirect evidence suggests that this elevates
conditions, for compliance, response and potential adverse effects,
dopamine levels within an hour when given in therapeutic doses
including physical side effects like hypertension and weight loss,
by oral administration (Volkow et al., 1998; Krause et al., 2000).
and effects on co-morbid symptoms. The best outcomes for moni-
These changes are accompanied by an increase in synaptic
toring response within trials and for individuals are not known but
dopamine that is dependent on cell-firing rates. Thus, following
may include ratings of core and co-morbid symptoms and effects
methylphenidate administration, a salient stimulus is found to
on various domains of functioning. In general, compliance may be
elicit greater synaptic dopamine levels than a neutral stimulus
better in adults than in children, although the reverse may also be
true. Patients may discontinue treatment due to disorganization,
Animal studies show that psychostimulants induce an increase
difficulty with persistence, negative and uninformed media
in cFos-like immunoreactivity consistent with it causing neuronal
(leading for example to employer prejudice), fears over
activation in the striatum, including the caudate, and in the
dependency, mistaking the treatment as the cause of the stigma of
mediofrontal cortex (Lin et al., 1996). However, microdialysis in
the disorder, and lack of knowledge on other long-term effects.
rats shows that intraperitoneal methylphenidate increases the
Atomoxetine is licensed in the USA for the treatment of adult
synaptic overflow of hippocampal norepinephrine and striatal
ADHD and in the UK for the treatment of adults who have previ-
dopamine efflux to a similar magnitude (Kuczenski and Segal,
ously been treated for ADHD as children. No agent is currently
2001). Furthermore, with oral methylphenidate, hippocampal nor-
licensed in the UK for adults newly diagnosed with ADHD so pre-
epinephrine efflux is evoked by lower doses than are required to
scribing is off-label. The drugs of first choice for the treatment of
elicit nucleus accumbens dopamine efflux (Kuczenski and Segal,
adult ADHD are classified as either psychostimulants (e.g.
2002). In contrast, atomoxetine causes a selective increase in cFos
methylphenidate, amfetamines (Maidment, 2003a)) or non-stimu-
within the prefrontal cortex without increasing expression within
lant (e.g. atomoxetine (Thomason and Michelson, 2004)) (see Table
the nucleus accumbens or striatum, consistent with it being a
3). Other non-stimulant agents reported to have some efficacy
selective inhibitor of NET as indicated from in vitro data (Bymas-
include alpha2 adrenoceptor agonists (clonidine and guanfacine),
ter et al., 2002). Yet, systemic atomoxetine administration
tricyclic antidepressants, bupropion, modafinil and venlafaxine
produced an equivalent threefold increase in prefrontal norepi-
(Maidment, 2003b). No efficacy has been found for selective sero-
nephrine and dopamine efflux measured by microdialysis (Bymas-
tonin-reuptake inhibitors, which may be because effective agents
ter et al., 2002), whereas extracellular norepinephrine but not
generally act via dopamine and/or norepinephrine as discussed next.
dopamine is increased in other brain regions, including the hip-
In general, core symptoms are thought to respond better to psychos-
pocampus (Swanson et al., 2006). The prefrontal cortex contains
timulants and atomoxetine than to antidepressants, although no
very low levels of DAT but dopamine and norepinephrine have
head-to-head studies have been done (Biederman and Spencer,
very similar affinity for NET, so it is possible that dopamine reup-
2001; Maidment, 2003a; Maidment, 2003b).
take may occur via NET in this brain area. Furthermore, adreno-ceptor agonists (guanfacine and clonidine), which are thought to
Mechanisms of drug action
activate prefrontal cortex postsynaptic alpha2 adrenoceptors, have
fied act on dopamine and/or norepinephrine neurotransmission,
been shown to improve performance of non-human primates in a
either as agonists or as reuptake inhibitors with the exception of
spatial working memory task (Avery et al., 2000).
modafinil, whose mechanism of action remains unclear (Fone andNutt, 2005). Methylphenidate is a potent inhibitor of dopamine
Clinical efficacy
Discussions on clinical efficacy are limited by
reuptake (Andersen, 1989; Thomason and Michelson, 2004), by
the lack of head-to-head studies with adequate and unbiased
binding to the cocaine-binding site on the DAT, but in vitro data
methodology. In general, all agents with evidence of efficacy in
on reuptake inhibition suggest that it also has a very high affinity
adults can reduce core symptoms, although effects on different
for the norepinephrine transporter (NET). The primary action of
symptoms and global functioning may vary between agents and
dexamfetamine is inhibition of dopamine reuptake but in addition,
individuals. In the absence of any obvious prescribing hierarchy,
amfetamines can cross the cell membrane by a mechanism
choice of agent may depend on pharmacological factors other than
independent of the transporter, and interact with the vesicular
efficacy (particularly abuse potential, side-effect profile and toxic-
monoamine transporter 2 (VMAT2), thereby displacing vesicular
ity in overdose), as well as individual factors (such as patient
dopamine and causing the release of newly synthesized intraneu-
choice and co-morbidity). The effect of genotype on treatment
ronal monoamine (Ferris and Tang, 1979; Fleckenstein and
response is unclear, although a poor response to methylphenidate
Hanson, 2003). Atomoxetine is a relatively selective NET
has been reported in children homozygous for the less common
inhibitor, having approximately a 300-fold higher affinity for NET
nine-repeat DAT1 genotype (Stein et al., 2005). ADHD management in adolescents to adults
In children and adolescents, over 200 trial reports indicate
in adults (Michelson et al., 2003; Faraone et al., 2005a Ib).
around a 70% short-term response rate with methylphenidate treat-
However, effects on overall functioning are debated, while no
ment (Smith et al., 2000 Ib; Schachter et al., 2001). A recent
long-term efficacy trials have yet been reported, although an
meta-analysis of several adult trials of methylphenidate indicates
interim analysis in adults has been reported (Adler et al., 2005a).
that response rates and effect size of treatment in adults is compa-
Thus, its place in clinical practice is not yet fully defined. Other
rable with, although somewhat lower than, those in children
norepinephrine uptake blocking agents such as desipramine
(Faraone et al., 2004 Ia). Notably, greater response rates were
(Wilens et al., 1996 Ib) have similar effects in trials while open
identified by physician ratings compared with self-report, and in
studies on venlafaxine report comparable responses (Adler et al.,
global functioning rather than core symptomatology. Long-acting
1995; Hedges et al., 1995; Findling et al., 1996 IIb). It is not
preparations are reported to have similar response rates and effect
known whether other noradrenergic agents like reboxetine, dulox-
sizes to standard methylphenidate (Santosh and Taylor, 2000 Ib).
etine and lofepramine have any efficacy in ADHD. Guanfacine is
It should be noted, however, that the long-acting preparations may
reported in one small trial to have similar efficacy to dexamfeta-
improve compliance, minimise abuse, diminish rebound symp-
mine (Taylor and Russo, 2001 Ib), as is the non-stimulant wake-
toms and address impairment later in the day, which has been
fulness-promoting agent modafinil (Taylor and Russo, 2001 Ib)
shown to lead to preferential effectiveness in children (Steele et al., 2006). Monitoring and adverse effects
The meta-analysis found response rates varied between trials
ments, patients should be specifically questioned about efficacy on
(25–78%); this report and a subsequent trial (76%) indicate that
core symptoms and in various domains of functioning, as well as
greater responses are found with higher dosing regimes (1 mg/kg)
effects on co-morbid symptoms and side effects noted. The find-
that are comparable with those effective in children (Faraone et
ings of the MTA study strongly suggest that active and fairly
al., 2004; Spencer et al., 2005b Ia). Other factors found to corre-
intensive monitoring of drug treatments improves effectiveness
late with response include reduced level of functioning (psychi-
(MTA Cooperative Group, 1999). Patients do not always report
atric outpatients versus high functioning academic underachievers)
psychiatric effects, which they may not realize can be induced by
and psychiatric co-morbidity, although the latter was not con-
medication. Therefore, direct questioning about changes in affect,
firmed in the latest trial (Spencer et al., 2005b).
anger or personality should be part of the follow-up interview. The
Similar but more limited findings are reported for dexamfeta-
physician also needs to ask directly about difficulty with com-
mine (dextro- or D-amfetamine) (Arnold et al., 1989; Paterson et
pliance, since this is often problematic in ADHD and may not be
al., 1999; Taylor and Russo, 2000, 2001 Ib), Adderall mixed
reported spontaneously. Diurnal changes in effects should also be
amfetamine salts (Spencer et al., 2001; Biederman et al., 2005 Ib),
sought, since these may be ameliorated by adjustment of dose
the psychostimulant pemoline (Wilens et al., 1999b Ib), and the
timing or with longer-acting preparations. In addition, long-term
dopaminergic agent bupropion (Wender and Reimherr, 1990;
monitoring of blood pressure, pulse and weight is indicated. All
Wilens et al., 2001 Ib). However, pemoline is associated with
the treatments for ADHD are associated with mild statistical
hepatotoxicity (Marotta and Roberts, 1998 III) and has been with-
increases in blood pressure and pulse which may not be problem-
atic in children, but could be problematic in those with antecedent
Several randomized, double-blind placebo-controlled trials
cardiac disease, hypertension or those who engage in extreme
have confirmed the efficacy of atomoxetine in children and adoles-
sports. Treatment adjustment should be guided by report of symp-
cents (Thomason and Michelson, 2004 Ib), and similar findings
toms and functioning in various domains as well as rating scores.
with an effect size of 0.35–0.4 have been reported from two trials
Optimal outcome is the dose which leads to best functional
Guidance on prescribing Off-label. Prescribing for adult ADHD is necessarily off-label since no agent is licensed for this indication – although atomoxetine is licensed for use in adults but only when ADHD treatment was initiated in childhood. The BNF (Joint Formulary Committee, 2005) states: ‘Unlicensed use of medicines becomes necessary if the clinical need cannot be met by licensed medicines; such use should be supported by appropriate evidence and experience.’ However, the BNF also states that prescribing medicines outside the recommenda- tions of marketing authorization alters (and probably increases) the doctor’s professional responsibility. This latter statement might explain a reluctance to prescribe beyond marketing authorization by clinicians, particularly in primary care. Although controlled evid- ence for prescribing in adults is not extensive, this consensus statement can be considered to meet the criteria for adequate evidence and experience in prescribing standard medications to adults with ADHD, when done in the context or with support of specialist psychiatric services. However, it is noted that supplementary prescribers are not contracted for unlicensed prescribing. Controlled drugs. Prescriptions for psychostimulants (CD) are subject to prescription requirements, which might be altered in the future, notably for computer prescribing. Currently in the UK, prescriptions must be indelible, signed and dated by the prescriber with their address, and must always state in the prescriber’s own handwriting: name and address of patient; the form and strength of a preparation (e.g. 10 mg tablets); total quantity or number of dose units in words and figures (e.g. 900 mg = nine hundred milligrams OR Ϫ90 = ninety doses); the dose (e.g. 10 mg tds). ADHD management in adolescents to adults
outcome, balancing adverse effects against benefits for that indi-
Diversion of psychostimulants is reported, in particular for
short-acting preparations. Very few clinical studies have evaluated
Various concerns have been raised over long-term treatment
the risk/benefit ratio of long-term stimulant medication at thera-
effects, including the potential for tolerance over time, and
peutic doses on human brain and behaviour (Volkow and Insel,
adverse effects of psychostimulants such as psychosis, sensitiza-
2003) – imaging studies indicate that cocaine induces a similar
tion, dependency and withdrawal reactions (Ashton et al., 2006).
blockade of striatal DAT to that seen with methylphenidate
Few data exist to guide clinicians since no long-term treatment
(Volkow et al., 1999). Circumstantial evidence exists for sensiti-
trials have been conducted in adults with ADHD. The long-term
zation and tolerance, which can be precursors to dependency; in
effects were reviewed in an analysis of existing short- and long-
particular, from baseline data of COMACs (Swanson et al., 2004;
term follow-up studies of stimulants in children with ADHD
Sonuga-Barke et al., 2005) and from the titration phase of the
(Hechtman and Greenfield, 2003). The conclusions were that chil-
MTA (Galanter et al., 2003), in which possible rebound was seen
dren with ADHD treated with stimulants for as long as 2 years
that might be due to tolerance (Sonuga-Barke et al., 2004).
continue to benefit from the treatment, with improvements
Co-morbid substance use is common in untreated ADHD (see
observed in ADHD symptoms, co-morbid oppositional defiant dis-
also ‘Substance use disorders’ below). Treatment in children has
order and academic and social functioning, with no significant
been repeatedly shown to be linked to a reduction in acquiring
problems of tolerance or adverse effects. Long-term, prospective
substance misuse, but the effect of treatment at other ages is not
follow-up studies into adulthood show that stimulant treatment
known. A meta-analysis of six trials in children found a 1.9-fold
in childhood has slight benefits regarding social skills and reduction in incidence of substance use in medicated comparedself-esteem. Long-term adverse effects from stimulant treatment in
with unmedicated patients (Wilens et al., 2003 Ia). Notably,
childhood regarding adult height or future substance abuse have
studies of methylphenidate-treated rats have found that treatment
not been supported by existing studies.
during the equivalent age to human childhood reduces the reward-
Substance use is a particular concern, both surrounding the
related effects of cocaine (Carlezon et al., 2003), while treatment
abuse potential of psychostimulants and the effect of treatment on
during the equivalent age to adulthood enhances cocaine reward
co-morbid substance use disorders. Abuse potential is related to
(Brandon et al., 2001). However, clinical experience suggests
the route of administration and the rate of absorption/bioavailabil-
probable lower use of recreational drugs in medicated adults,
ity of the drug, and may relate to the resultant rate of dopamine
although adolescence might carry a differing vulnerability. Thus,
release, which is higher for dopamine releasers than pure reuptake
rigorous studies are needed to determine the long-term effects of
inhibitors (Kollins, 2003). Slow-release preparations have less
pharmacotherapy in different age groups, particularly on co-
abuse potential and are less amenable to use through abused routes
morbid recreational substance use. Research is also needed to
such as snorting. They are to be preferred for patients with a
determine whether treatment of ADHD in patients currently using
history of, or risk factors for, drug misuse.
cannabis and/or alcohol on a daily basis is effective. Recommendations – drug treatments •
Proven drug treatments in children include psychostimulants (A) and atomoxetine (A) as first-line treatments, with imipramine,which is metabolized to desipramine, (B) and bupropion (B) as second-line treatments and clonidine and guanfacine as pos-sible adjunctive treatment (D).
Adult patients with ADHD are most likely to present to primary care, but drug treatment is best initiated and optimized by sec-ondary/specialist services (D).
Drug treatment needs to be chosen and adapted to best fit the individual, including the patient’s preferences and concerns (D).
Meta-analysis of methlyphenidate in adults demonstrates similar drug response effect sizes to that seen in children (A).
The limited evidence in adults suggests that agents that enhance synaptic dopamine have far better efficacy than other treat-ments for core symptoms – amfetamines, methylphenidate and atomoxetine are all effective but not equivalent, since they havedifferent actions and hazards (A).
Drug prescribing in adults is usually off-label but clinicians are supported in prescribing by these BAP guidelines (D).
Drug treatment requires regular, preferably structured, monitoring and review (e.g. for dose adjustment). For uncomplicatedcases this should be every 6–12 months.
Clinicians need regularly to assess patients on medication for ADHD and other symptoms, global and specific functioning,adverse effects, concordance of effects (e.g. between patient, doctor, informants), psychiatric side effects, cardiovasculareffects, compliance and tolerance (daily and long term) (D, S).
Drug treatment should NOT be initiated if the diagnosis is uncertain or benefit is unlikely (D).
Abuse potential is related to drug action and formulation – abuse by patients seems low, but diversion can occur with stimu-lants for performance enhancement or weight loss (D). Slow-release preparations of these agents or atomoxetine are to be pre-ferred for patients with a history or who are at risk of drug misuse (D). Controlled studies are required to confirm theseobservations. ADHD management in adolescents to adultsKey uncertainties •
Can we extrapolate from treatment studies in children?
Can drug treatment be continued and monitored in primary care with training and support? With such an arrangement, whatwould the workload and resources implications be for both primary and secondary care?
How is individual outcome of drug treatment best assessed?
How do classes of drugs compare with each other in head-to-head comparisons and with psychotherapeutic approaches inadults?
What factors underlie individual differences in drug response, tolerance and other side effects and how is treatment bestmatched to individuals and types of impairments?
What is the effectiveness of various drug treatments beyond clinical ADHD trials?
Do different drug treatments have differential effects on different underlying deficits (endophenotypes)?
What are the effects of different drug treatments on symptoms beyond ADHD core (e.g. functioning/impairment), risk–benefitanalysis and tolerance?
What are effects of long-term drug treatment and how feasible are long-term follow-up studies given likely high dropout rates?
What are better measures of effectiveness and cost effectiveness for drug trials?
What are the important interactions with other prescribed psychoactive medications (e.g. SSRIs) and with recreational drugs?
When are drug treatments best avoided (e.g. women of child-bearing age, certain age groups, patients with nothing to do)?
chotherapeutic approach led to decreased self-esteem andincreased frustration. In a review of 36 patients improved but not
The Multimodal Treatment Study in ADHD (MTA Cooperative
remitted on medication, 85% of those who also had co-morbidity
Group, 1999) has provided definitive evidence on the role of psy-
found benefits of adapted cognitive–behavioural therapy on
chotherapy in childhood, with the conclusion that psychotherapy
anxiety, depression and functioning (Wilens et al., 1999a III).
provides a small additional benefit when added to drug treatment.
Two controlled, non-randomized studies are reported. Seventeen
Compared with children, adults are mostly self-referred and thus
patients given psycho-education and organizational skills teaching
are self-selected and generally more motivated. However, adults
versus no treatment found improvements in organization, attention
have usually left the education system where skills are taught and
and emotional stability but a reduction in self-esteem (Wiggins
may also be affected by lifetime failures and effects of co-morbidity. et al., 1999 IIa). In 15 patients, dialectical behaviour therapy
Good evidence of the effects of psychotherapy in adulthood is
showed improvements in ADHD symptoms, depression and func-
sparse. Moreover, the usefulness of published studies is limited
tioning compared to control treatment (Hesslinger et al., 2002 IIa).
due to small numbers, lack of evidence on long-term unmedicated
Three RCTs are published, with some good effect sizes
patients, failure to consistently rate effects beyond core and co-
reported in terms of core symptoms, and providing some insights
morbid symptoms, exclusion of patients with extreme symptoms
into the interaction of psychotherapy with medication. A cognitive
or co-morbidity, and analysis of completers only.
remediation programme using a brain injury model in 44 patients
Clinical experience indicates that general psychotherapeutic
versus waiting list controls showed moderate effects on core
support and psycho-education around the time of adult diagnosis,
symptoms and organization with minimal improvement of self-
treatment initiation and review seems helpful. Aims of psycho-
esteem and anger (Stevenson et al., 2002 Ib). Notably, effects on
education are to inform on the condition, natural history and prog-
core symptoms and organizational skills were maintained at 1 year
nosis, to prevent further negative effects on self-esteem or
while effects on anger were not. A retrospective examination of
unrealistic expectations of treatment and to give perspective to
the effects of cognitive remediation found no difference between
individual neurodevelopmental history. Advice to and screening of
medicated and unmedicated patients but numbers were small
family members may also be initiated at this time. A review of the
psychosocial environment is essential to assess specific limitations
Weiss and the ADHD Research Group have examined the
in various domains, the level of executive demands and coping
effects of individualized problem-focused therapy in 33 patients
skills already acquired. Assistance with improving coping skills
on dexamfetamine versus those on placebo (unpublished data Ib).
and efforts at environmental restructuring may have a powerful
Problem-focused therapy was found to be more effective in redu-
impact on the functioning of adults with ADHD. Group therapy,
cing core symptoms and improving functioning in medicated
where available, may help with social isolation, especially around
patients than controls. Modified cognitive–behavioural therapy
the critical period where treatment initiation can enhance
plus medication demonstrated greater benefits than psychotherapy
experience of failure and lead to loss of self-esteem, depression
or medication alone particularly on ADHD symptoms, with lesser
and substance use (Safren et al., 2005a).
effects on anxiety and depression in 32 patients (Safren et al.,
In terms of psychotherapy, an initial retrospective notes review
conducted by Ratey et al. (1992 III) found that a dynamic psy-
ADHD management in adolescents to adultsRecommendations – psychotherapeutic approaches •
General psychotherapeutic support to the individual, family and others around time of diagnosis and treatment initiation ishelpful to inform on the condition and prognosis, to prevent negative effects on self-esteem or unrealistic expectations of treat-ment, to adapt positive and negative coping strategies and to give perspective to individual neurodevelopmental history (D).
Structured, adapted psychotherapies may be useful to build confidence, develop executive skills, address anxiety and depres-sion and improve functioning (B), while group therapy may help for social isolation (C/D).
Evidence in childhood suggests that psychotherapies are beneficial for co-morbid anxiety and for functional outcomes beyondthe core symptoms, when added to drug treatment (B). Since adults are self-referred, may no longer have access to school orskills development and are motivated once symptoms improve, there is reason to suggest that non-pharmacological treatmentsmay be useful in augmenting the functional outcomes of medication alone (D).
Involvement of educational/occupational psychologists and other relevant personnel for environmental restructuring can maxi-mize functioning at college/work (D). Key uncertainties •
Whether and what types of therapy might best work for the different aspects of ADHD (different core symptoms, global func-tioning) and for different co-morbidities?
How best to combine drug treatments, psycho-education, psychotherapeutic approaches, and environmental restructuring?
Can psychotherapy be used with good effect in adults unable to take, or who do not respond to, medication?
What is the natural history of the outcomes of psychotherapeutic approaches and what follow-up approaches are needed toreinforce effects over time?
Thus, various forms of structured, intensive, skills-based treat-
background and natural history of ADHD, and many common co-
ment may improve likelihood of remission, especially when com-
morbidities, an accurate diagnostic attribution could also inform on
bined with medication. Effects of psychotherapy on core
the likely course and complications of the disorder. Much
symptoms including disorganization seem substantial, with
experience with co-morbidity comes from specialist paediatric
potential effects on functioning and modest effects on co-morbid
clinic populations, which are likely to have increased co-morbidity
symptoms. The effect on self-esteem seems often poor or even
compared with the general population. Specialist clinics need to
negative, since skills-based treatment may reveal low function-
have skills to differentiate or exclude key co-morbidities, as these
ing. Psychotherapy data have particular implications for patients
will impact on management, which in turn will impact on co-
who have a poor response to or who are unable to take medica-
morbidities. This is an argument for establishment of neurodevelop-
tion (e.g. women who wish to become pregnant), while such
mental clinics that can provide appropriate specialist training in
interventions might be particularly helpful for patients who are
assessment and management to patients of all ages (IV).
parents and others with a high-level need for learned skills,including those with few activities in their lives. A future direc-tion for research is on therapies that emphasize interventions to
address disinhibition and impulsivity, interpersonal skills andstress management.
Evidence on co-morbidities is fairly strong – at all ages, the dis-ruptive and antisocial behaviours predominate; in childhood andadolescence, other neurodevelopmental disorders are the main
Co-morbidity and special situations
additional co-morbidities, while in adults substance use and mooddisorders predominate. Several co-morbid studies of adults with
Co-morbidity could be considered the rule rather than the exception
ADHD have been completed (Kooij et al., 2001; Biederman,
when ADHD persists into adulthood (IV), yet much of the available
2004; Secnik et al., 2005; Kessler et al., 2005, 2006; Torgersen
evidence is from childhood populations. A key difficulty in the
et al., 2006). Co-morbid disorders in adults can be classified into
diagnostic process is determining the relationship between symp-
(1) ongoing developmental disorders such as learning disabilities,
toms attributable to ADHD and other symptoms. Thus, symptoms
oppositional defiant disorder, conduct disorder, autism spectrum
may represent core ADHD symptomatology, complications or con-
conditions, Tourette and tic disorders, and developmental delay,
sequences of ADHD, including self-medication, a separate co-mor-
and (2) disorders that may first present in childhood but are famil-
bidity, a differential diagnosis or even the effects of prescribed
iar to adult psychiatry such as anxiety and mood disorders, post-
medication. An accurate diagnostic attribution is important to deter-
traumatic stress disorder, substance use/dependence, sleep
mine the likelihood of a given treatment modality improving spe-
disorders and personality disorders. Up to 90% of adults will have
cific symptoms as well as to determine an individual diagnostic
one or another of these co-morbidities. Epidemiological data
hierarchy for targeting treatments. Given the neurodevelopmental
suggest that at least a third of patients will have had a lifetime
ADHD management in adolescents to adults
history of mood or anxiety disorders or other disruptive behaviour
A common finding in childhood is that stimulant medication
disorders. The prevalence of current co-morbid disorders is lower
does work in some individuals with neurodevelopmental co-
than a history of co-morbid disorders. Some co-morbid presenta-
morbidity but that non-response or adverse effects may be more
tions such as problems with sleep and learning disabilities in
common. If stimulants prove unsuitable in the individual case, med-
adults have not yet been researched although they may be quite
ication aimed at the co-morbid disorder or combined medication
common. Clinically, this is of major importance since ADHD in
might overall provide a better response than medication aimed at
adults rarely exists in isolation and outcome may be determined by
ADHD, as argued with autistic spectrum disorders and bipolar
co-morbid disorders that either preclude treatment, require treat-
symptoms. This begs the question of whether a diagnostic hierarchy
ment in their own right or are more severe than ADHD itself. A
exists for co-morbid disorders and the effect this has on treatment –
good assessment for ADHD in adults therefore requires a full
for example, bipolar symptoms, autistic spectrum disorders and
mental status and psychiatric exam for other disorders as well as
epilepsy treated before ADHD, which may be targeted before or
familiarity with both the co-morbid conditions of childhood and
alongside substance use disorders, conduct disorder and opposi-
the co-morbid conditions of adulthood.
tional defiant disorder. Sleep problems, anxiety and depression may
Childhood proportion of co-morbidities are given as follows:
arise as a consequence of ADHD but may still require separate
oppositional defiant disorder (40%); language disorders (30–35%);
treatment, including antidepressants. Complex cases need to be con-
conduct disorder (20%); specific learning disability (15–25%);
sidered on an individual basis and may need further specialist refer-
anxiety disorder (20–25%); mood disorder (15–20%); smoking
ral (e.g. for sleep assessment), especially in adulthood, where
(19%); substance use disorder (15%); autistic spectrum disorders
existing evidence and experience is even less than in childhood.
(10%); tics (15–20%), often associated with Tourette’s syndrome
Evidence on management of bipolar symptoms comes mainly
and obsessive–compulsive disorder; epilepsy; sleep disorders;
from expert experience outside Europe. One concern in this group is
the potential for psychostimulants to enhance the likelihood of psy-
Conversely, ADHD as a co-morbidity correlates strongly with
chosis (DelBello et al., 2001), whether in children with prominent
some disorders and needs to be specifically sought in these popu-
mood instability or in those with a strong family history of bipolar
lations. For example, with Tourette’s or chronic tic disorder,
disorder. Risperidone and other atypical antipsychotics help with
roughly one in two to three children will have ADHD while one in
psychotic symptoms, mania and aggression but ADHD symptoms
three will have obsessive–compulsive disorder, which will further
respond poorly. Sodium valproate may be useful in rapid cycling
impact on management. Many more may have poor social skills.
and mixed states. Since psychostimulants carry a potential risk of
Autistic spectrum disorders is another area in which ADHD symp-
worsening or triggering bipolar symptoms, expert paediatric groups
toms occur commonly in the symptom profile, including: stereo-
in Boston and Cincinnati treat mania prior to addressing the ADHD
typed mannerism (70%), stereotyped utterances (65%), inattention
separately; however, their views remain controversial.
(60%), morbid/unusual preoccupation (65%), compulsions or
Depression can be treated with antidepressants, such as the
rituals (50%), anxiety or fears (50%), hyperactivity (40%), depres-
SSRIs, which can be used safely with psychostimulants. Nora-
sion/irritability/agitation (25%), self-injury (30%), tics (8%).
drenergic agents (atomoxetine, reboxetine) might be sensible for
In Europe, bipolar disorder is a controversial diagnosis along-
use in people with co-morbid anxiety and depression, though no
side a diagnosis of ADHD in childhood, and yet experts in other
research studies have been done to confirm this supposition, while
areas recognize that children with unstable mood and ADHD
methylphenidate was used as an antidepressant in the 1950s.
symptoms do exist (Geller et al., 2000a, 2000b; Craney and
With autistic spectrum disorders, one in two children respond
Geller, 2003; Post et al., 2004). Moreover, the combination of
to medication compared with two in three of children with ADHD
hypersexuality, grandiosity and a family history of bipolar illness
alone. Psychostimulant side effects are more common in autistic
is common in paediatric bipolar presentations, particularly in the
spectrum disorders, typically dysphoria and perseveration or cog-
context of neurodevelopmental disorders. A subgroup of these
nitive rigidity, which needs to be monitored. A final dose of 20 to
children may therefore be at risk of later adult bipolar disorder,
30 mg/day of methylphenidate is usually sufficient. The key prin-
which is conceptualized differently from childhood mood-related
ciples with dosing are to start low, go slow and monitor more fre-
symptoms, such as dysphoric conduct disorder, in which ADHD
quently. Conversely, the effect of atypical antipsychotics on
symptoms, conduct disorder and depression co-exist. Thus the
ADHD symptoms particularly hyperactivity in ASD is good, with
possibility exists that bipolar disorder is also a neurodevelopmen-
an effect size of 1.4 (McCracken et al., 2002 Ia).
tal disorder that produces dysregulation of affect. This also implies
Evidence on the link between ADHD and children with
that an early mood complication or a strong family history is more
epilepsy is somewhat stronger, occurring commonly in the context
likely to predict a mood co-morbidity in the future.
of learning disabilities. Adequate anticonvulsant cover is essential,
In initiating medication for co-morbidities, it is important to con-
and treatment of ADHD with stimulants may be indicated once
sider on an individual basis the effectiveness, risk–benefit ratio and
anticonvulsant hyperactivity is ruled out. Little research exists in
the likelihood of tolerance and other effects of a given treatment. Co-
this area, and the research that does exist has studied
morbidity may increase the need for a combined treatment strategy
methylphenidate only (Gross-Tsur et al., 1997; Gucuyener et al.,
with one or more medications plus a specific psychotherapeutic man-
2003; Tan and Appleton, 2005; van der Feltz-Cornelis and
agement – e.g. behavioural programmes for conduct disorder or cog-
Aldenkamp, 2006). However, psychostimulants, atomoxetine and
nitive–behavioural therapy for co-morbid mood disorders.
antidepressants can lower seizure threshold. ADHD management in adolescents to adults
Sleep disorders are a common complaint with some 40% of
versely, medication for co-morbid disorders might impact on
children with ADHD having sleep symptoms, which may be due
ADHD. For example, our experience suggests that anticonvulsants
to stimulant medication or due to inability to settle down at night
might increase hyperactivity and restlessness as might drugs for
due to ADHD. The latter will respond to a later dose of stimulant
sleep disorders, while atypical antipsychotics can worsen many
medication, although care should be given when administering
late doses of psychostimulants as failure to clear medication com-pletely by the time of the next morning dose might lead to the
development of a steady state, which may increase risks of toler-ance and sensitization. Another key co-morbidity that presents
Substance use disorders are common in ADHD and may persist
with sleep symptoms is an undiagnosed anxiety disorder (e.g.
into or arise in adulthood. Substance use may reflect a core deficit
phobia of darkness). Treatment options include non-pharmacolog-
in ADHD, i.e. reduced reward mechanisms and impulsivity, it can
ical measures to regulate sleep (‘sleep hygiene’), melatonin, cloni-
arise via conduct disorder and antisocial behaviours, or develop
dine, trazodone and zolpidem. Recent clinical trials have
through self-medication with stimulants, alcohol, cannabis or
demonstrated that patients with co-morbid ADHD and anxiety or
other sedatives. Substance use disorders thus represent a diagnos-
tics may show improvement in both disorders with atomoxetine
tic difficulty in people with possible ADHD; in the presence of
core symptoms of ADHD, substance use disorders could be con-
At follow-up, clinicians need to assess the effects of ADHD
sidered a complication of ADHD. In childhood, stimulant medica-
treatment on all key symptoms, including those of other diag-
tion does not cause but in fact reduces the incidence of substance
noses, since ADHD medication may have either a positive or
use disorders (Wilens et al., 2003 Ia). However, effects in adult-
negative impact on co-morbid diagnoses. Psychostimulants often
hood may vary among individuals – adult substance use may
worsen sleep, mood, appetite, emotional lability, cognitive rigidity
reduce with ADHD medication but others could be predisposed to
and other symptoms in practice so assessment of such effects is
the development of tolerance, sensitization and increased sub-
needed in future clinical trials and in populations that are excluded
stance use, particularly with higher doses of psychostimulants (see
from clinical trials. The relationship between tics and ADHD
‘Monitoring and adverse effects’ above).
grows stronger with time. Although research indicates that there is
In general, substance use needs to be stable prior to initiating
no statistically significant worsening of tics with stimulants or ato-
medication treatment of ADHD, especially in primary care. Few
moxetine in children, individuals may nonetheless experience
trials have examined the effects of treatment in adults with sub-
either improvement or deterioration in tics which needs to be
stance use disorder but methylphenidate has been used effectively
treated accordingly (Gadow et al., 1995; Allen et al., 2005). Con-
in cocaine users (Levin et al., 1998 Ib), while history of drug
Recommendations – co-morbid conditions •
Clinicians need to screen for autistic spectrum, developmental disorders, communication difficulties, learning disabilities, ticsand Tourette’s syndrome, anxiety and affective disorders, substance use disorders and others (e.g. epilepsy, sleep disorders,sensory problems), but symptoms cannot be counted twice for ADHD and co-morbid disorders (C/D).
Further specialist input or advice may be needed regarding co-morbidity (e.g. learning disability teams), since co-morbiditycan have a greater impact on functioning than ADHD (D).
Likely co-morbidities vary according to age of presentation and will alter treatment responses and outcomes, including adverseeffects, but co-morbidity is not necessarily a barrier to treatment of ADHD (C/D).
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