In Iran, a study was performed which determined the risk of ADHD in siblings of patients with this disorder.12 The authors compared three groups: 200 patients diagnosed with ADHD, all treated with methylphenidate with no dose alteration during the study, 200 of their siblings and 200 controls (aged 8–14 years). Diagnoses were made based on the criteria of the Diagnostic and Statistical Manual of Mental Disorders, Fourth Edition, Text Revision (DSM-IV-TR) and they carried out semi-structured interviews on parents administering the ADHD rating scale-IV and Conners’ Parent Rating Scale, a direct assessment of the children and a review of their school reports. Adjustments were made for age, sex and the presence of other psychiatric disorders, and patients with a history of central nervous system diseases and psychiatric disorders such as autism, depression, anxiety and ODD were excluded. Ultimately, they found that the risk of ADHD in siblings of patients with ADHD is greater compared to the controls (odds ratio [OR]=13.50; 95% confidence interval [95% CI], 3.15–57.94). It was also discovered that children with ADHD whose siblings had the same diagnosis presented higher scores for oppositional behaviour, anxiety, perfectionism and psychosocial and psychosomatic problems than children with ADHD and siblings without, thereby indicating greater severity. However, in the total ADHD rating scale-IV score, there were no significant differences between the index cases and affected siblings as regards impulsivity and hyperactivity.

Yang et al.13 took 136 children from Taiwan with a diagnosis of ADHD as per the DSM-IV-TR (mean age, 12.8 years), 136 siblings and 136 controls of similar ages. Children with autistic spectrum disorders, psychosis or an intelligence quotient (IQ)<80 were excluded. The authors assessed all of the subjects using the Kiddie Schedule for Affective Disorders and Schizophrenia for School-Age Children, Epidemiologic Version (K-SADS-E) and classified the siblings as either affected or unaffected by the following disorders: ADHD, conduct disorder (CD), major depressive disorder (MDD), ODD, sleep disorders and substance use disorders (SUD). The percentage of siblings found to have ADHD was 34.6%.

A previous study published by Faraone et al.14 in 1996 compared 174 siblings of ADHD patients and 129 siblings of controls. All of the subjects were Caucasian and aged 6–17. Adopted children, subjects who presented neurodegenerative diseases, psychosis, autism or an IQ <80 were excluded, as well as those from low socioeconomic classes (to avoid confounding due to psychosocial adversity). After the initial assessment, follow-up at one year was performed (retention: 169 index case siblings and 135 control siblings) as well as at four years (retention: 169 index case siblings and 143 control siblings). They were diagnosed according to the DSM-III-R, administering the K-SADS-E interview to parents and patients (except for children younger than 12 years of age, who were not directly interviewed). The authors found that 26% of the index population's siblings had the same diagnosis at four years, compared to 10% of the control population's siblings (p=0.01).

In concordance with previous studies, in 2014 Lino Palacios et al.15 published a study performed on the Mexican population in which they assessed 84 biological siblings (aged 13–19 years) of ADHD patients undergoing psychiatric follow-up. Twins, patients diagnosed with a chronic CNS disease and those who had a previous psychiatric diagnosis or who were receiving psychiatric medication or psychotherapy were excluded. A mental health professional (clinical psychologist with a Master's degree or psychiatrist) carried out the assessments and, to diagnose any form of mental disorder, the following criteria were used: DSM-IV and the Brief Psychiatric Rating Scale for Children (BPRS-C), 25-item Mexican version, which includes four more aspects than the original scale: (a) elimination disorders; (b) hyperthymia; (c) use and abuse of alcohol, tobacco and other drugs, and (d) psychological and sexual abuse. Moreover, each case assessed underwent diagnostic confirmation by another certified expert psychiatrist. Variables such as severity of ADHD symptoms, functioning in various areas (school, social and family) and psychosocial adversity were measured. It was found that 45.2% of the siblings also had ADHD, most of which had the combined subtype (68.4%), with the rest having the inattentive subtype. On the other hand, 17.9% of these siblings had no psychiatric disorder. These figures are striking given the study's inclusion criteria: only siblings who had not asked for professional help.

Based on these four studies, we can conclude that, although the risk of ADHD in siblings of patients with this diagnosis is variable, they all agree that these siblings have an increased risk compared to the general population. This confirms the influence of both genetic and environmental or psychosocial variables on ADHD risk.

The siblings of ADHD patients are not only more at risk of ADHD, but other types of psychiatric disorders too. In the study by Yang et al.13 it was found that the frequency of any other psychiatric disorder (ODD, tics, anxiety and CD) stood at 82.4% in the index patients; 72.3% in siblings with ADHD; 42.7% in siblings without ADHD; and 33.1% in the control subjects. On comparing index cases to unaffected siblings, the risk of suffering another psychiatric disorder was high (OR=6.38; 95% CI, 3.43–11.88). This was also the case compared to the control population (OR=9.60; 95% CI, 5.31–17.34). Moreover, said disorders were more common in siblings with ADHD than siblings without ADHD (OR=3.58; 95% CI, 1.61–7.98) and control subjects (OR=5.38; 95% CI, 2.5–11.6). By specific psychiatric disorders, the frequency of ODD was 44.7% among siblings with ADHD, 11.4% among siblings without ADHD and 9.6% in control subjects. The frequency of CD was 21.3% among siblings with ADHD, 2.4% among siblings without ADHD and 2.9% in control subjects. With respect to tics, the frequency was 8.5% among affected siblings and 2.9% in the control population. As regards affective disorders, the subjects with MDD were 10.6% of the siblings with ADHD, 8.2% of the siblings without ADHD and 10.3% of the controls. The frequency of generalised anxiety disorder (GAD) was 4.3% among affected siblings, 1.2% among unaffected siblings and 0.7% in control subjects. Greater rates of alcohol abuse were also found in siblings with ADHD than in the control population (61.7% versus 41.2%), a risk which is comparable to the index cases.

In the publication by Faraone et al.,14 three groups of subjects were compared: siblings of patients with ADHD with the same disorder, siblings without ADHD and control subjects. A greater prevalence was found in the first group: CD (25% versus 6% versus 4%), ODD (59% versus 19% versus 2%), MDD (36% versus 10% versus 8%), BAD (25% versus 3% versus 4%), anxiety disorders (32% versus 20% versus 10%) and psychoactive substance use (25% versus 17% versus 16%).

Palacios15 found that only 17.9% had no psychiatric disorder at the time of the study and that over 40% of the ADHD patients’ siblings had two other mental disorders besides ADHD. Nevertheless, when adjusted for gender, age and number of psychosocial adversities, only ODD was statistically significant (OR=2.98; 95% CI, 1.8–10.9). Moreover, it was also shown that the siblings with a ADHD diagnosis had a greater frequency of learning difficulties (OR=5.09; 95% CI, 1.28–20.28) even after adjustment for the abovementioned variables. Impaired self-concept and social and family relationships were also observed, but with no statistical significance (p=0.288).

Schuler et al.16 described the psychopathology of subjects with ADHD and their affected siblings in a genetically isolated population from Costa Rica's Central Valley. They selected a sample of 95 index cases and 62 siblings aged between 6 and 26, whom they divided into two groups: children (6–12 years) and adolescents (13–26 years). The subjects were assessed according to the DSM-IV diagnostic criteria, for both ADHD and any other psychiatric disorder, and it was found that the most associated comorbidities in the index cases were anxiety disorders (55.9%), tics (34%), mood disorders (11.7%) and conduct disorders (30.9%); only 16% did not have psychiatric comorbidities. On assessing the disorders individually, it was found that ODD was the most common (26.6%), followed by a specific phobia and social phobia (each 17.2%), Tourette's syndrome (17%), GAD (14%) and separation anxiety (12.9%). Generally speaking, there were no differences between the age groups, except for disruptive disorders which were more prevalent in children than adolescents, a difference that is largely due to ODD (35% versus 16.2%; p=0.03). On comparing the index cases to their siblings, it was found that they did not differ significantly in terms of comorbidities except for tic disorders, which were more common in the former (31.9% versus 11.5%). Moreover, a greater proportion of siblings were found to have no psychiatric comorbidities (26.3% versus 16%), although the difference was not statistically significant (p=0.12). There was also a significant concordance between anxiety disorders and mood disorders, which indicates heritability in these families; for anxiety disorders this heritability estimate was 0.81 and, for mood disorders, 0.49. Anxiety disorders were also more common if the index case had said comorbidity (OR=6.39; 95% CI, 1.65–24.7). These data contradict other study series in which comorbid ODD or SUD are more common, thus indicating that certain genetic, environmental and sociocultural factors specific to this sample might have an impact on the subjects’ psychopathology.

Milberger et al.17 searched for a relationship between ADHD and SUD in index case siblings and control population siblings. A sample of white, non-Hispanic males aged 6–17 was selected. A group of 140 index cases and their 174 siblings (referred to as high-risk siblings) were compared to a group of 120 controls and 129 siblings. Adopted children and those with major CNS disorders, psychosis, autism or an IQ<80 were excluded, as well as children from a low socioeconomic class in order to minimise the potential confounding of social adversity. Diagnoses were made using a semi-structured Kiddie SADS-E interview based on the DSM-III-R criteria, with a psychiatric assessment also performed to establish alcohol and drug abuse or dependence. Parents and children were interviewed separately, except for children younger than 12 years of age, who were not directly interviewed. The high-risk siblings were found to have significantly higher rates of ADHD than the control group siblings (18% versus 5%). Moreover, four groups were compared: (a) high risk+ADHD; (b) high risk without ADHD; (c) control siblings+ADHD; (d) control siblings without ADHD. No significant differences were found in the prevalence of substance use between the high-risk population and control siblings (17% versus 16%). However, marked differences were observed between siblings with ADHD and without ADHD, regardless of the degree of risk (36% versus 15%). The prevalence of SUD in all siblings with ADHD was 41%, compared to 16% among siblings without ADHD, with high scores in all categories of abuse or dependence in the first group. No significant differences were found in the preferred drugs of the high-risk siblings and siblings with ADHD. The drug most frequently used in all groups was marijuana; 92% of the siblings with drug abuse or dependence also had a history of tobacco or alcohol use and, of these, 88% were dependent on cigarettes or alcohol alongside drug abuse or dependence. The age at onset of substance use was also compared, but no significant differences were found between the high-risk siblings and those of the control group. However, siblings with ADHD generally had an earlier onset of all categories of SUD compared with siblings without ADHD. These results were also adjusted for different variables and high-risk status was not found to be a significant predictor of SUD (hazard ratio [HR]=0.6; p=0.1), whereas having ADHD at baseline (HR=2.7; p=0.01), CD (HR=4.7; p=0.001) and anxiety disorders (HR=2.2; p=0.04) were. In addition, siblings with ADHD and a comorbid CD had significantly higher rates of SUD (89%), with an earlier onset of substance use (13.6 years), compared to ADHD siblings without CD (24%), who had an age at onset of 15.6 years.

Steinhausen et al.18 published a study with the objective of determining the behavioural profile of children with ADHD and of their siblings with and without the disorder. They used a sample of 172 children aged 8–16 (69 index cases, 32 siblings with ADHD and 35 siblings without ADHD, compared to 36 controls). All of the index cases had ADHD combined type, while the siblings had any subtype, and there were no significant IQ differences between the groups. The Conners’ Rating Scale was used for the assessment, as well as the Strengths and Difficulties Questionnaire (parent and teacher version) and the Child Behaviour Checklist; diagnoses were made according to the DSM-IV. The authors found that, with the exception of hyperactivity, which was marked among the index cases, there were no differences between the index subjects and their siblings with ADHD on any scale. Moreover, scores on the Conners’ Rating Scale were similar in siblings without ADHD and control subjects across all the domains. However, siblings without ADHD scored significantly higher than the controls on other scales measuring anxiety, shyness, perfectionism and emotional lability. The index subjects and their affected siblings had equal scores for social withdrawal, somatic complaints, affective problems (anxiety and depression), thought problems and delinquent behaviour, but index children scored higher than their affected siblings for inattention and aggression.

Biederman et al.19 examined the relationship between ADHD and obsessive-compulsive disorder (OCD) by means of a familial aggregation study. The authors used a sample of index subjects (6–17 years): 256 with ADHD but without OCD, 12 with both ADHD and OCD and 235 controls; they also included their first-degree blood relatives (parents and siblings): 791, 33 and 716, respectively. They found that the risk of ADHD was similarly elevated among relatives of ADHD patients with and without OCD (19.9% and 20.1%) compared to the control group (4.6%), but that the risk of OCD was only significantly elevated in relatives of subjects with ADHD and OCD (13%) versus the controls (0.5%). Moreover, they also discovered that relatives with ADHD had a greater risk of OCD than unaffected relatives (7.4% versus 1.3%), thus indicating co-segregation between these disorders.

Finally, a Swedish study8 explored the risk of ADHD, BAD and schizophrenia in first- and second-degree blood relatives. A sample of 61,187 patients with ADHD was identified and matched by gender and age with a group of control subjects without ADHD (aged 7–65 years) and their respective first- and second-degree relatives. Diagnoses were made according to the criteria of the eighth, ninth and tenth editions of the International Classification of Diseases (ICD), and patients who already had a history of either of these two disorders were excluded. In the relatives of patients with ADHD, the authors found a stronger history of BAD in 51% of parents (OR=1.84; 95% CI, 1.72–1.97), 12% of children (OR=2.54; 95% CI, 1.92–3.35) and 23% of siblings (OR=2.22; 95% CI, 1.98–2.50), and a stronger history of schizophrenia in 16% of parents (OR=2.22; 95% CI, 1.99–2.47), 5% of children (OR=1.89; 95% CI, 1.13–3.15) and 13% of siblings (OR=1.71; 95% CI, 1.44–2.04). This risk was lower among second-degree blood relatives.