Participants

A total of 381 individuals were recruited from the in-patient and out-patient clinical services of the Zucker Hillside Hospital, a division of the North Shore–Long Island Jewish Health System. The Structured Clinical Interview for DSM–IV Axis I disorders (SCID, version 2.0) ^{Reference First, Spitzer, Williams and Gibbon21} was administered by trained raters. All participants were screened, recruited and assessed by the same ratings team at a single site, the Zucker Hillside Hospital. On average, participants had spent 13.52 years (s.d.=8.91) in treatment at our institution (in-patient and out-patient), therefore allowing us to capture the majority of their illness course with our own medical records. All available family members (over age 18) were also interviewed to enhance diagnostic validity. Thus, the diagnostic process included the SCID, detailed medical record review, interviews with family members, consultation with the clinical treatment team and formulation of a detailed two to three page case summary of each participant that was discussed in a diagnostic consensus conference led by the project principal investigator (A.K.M.).

We have also operationalised DSM–IV Criterion C for schizoaffective disorder, which differentiates it from schizophrenia. ²² Criterion C requires that mood symptoms meeting criteria for a mood episode ‘must be present for a substantial portion of the entire period of illness’ for a diagnosis of schizoaffective disorder to be made. Our operationalised criteria took ‘a substantial portion’ to be greater than 20% of duration of illness. Following these procedures, all but three individuals (0.8%) were assigned a consensus diagnosis of schizophrenia, schizoaffective disorder, bipolar disorder or unipolar major depressive disorder. The consensus diagnosis and demographic information for these 378 individuals are presented in Table 1.

Table 1

Demographics of the five participant groups (total n=600)

	n (% male)	Mean age (s.d.)
Schizophrenia	211 (73.9)	38.3 (10.3)
Schizoaffective disorder	61 (52.5)	38.6 (12.2)
Bipolar I	77 (53.2)	36.6 (11.8)
Major depressive disorder	29 (44.8)	42.4 (9.4)
Healthy controls	222 (41.0)	47.6 (18.6)

Healthy controls (n=222) were recruited by use of local newspaper advertisements, flyers and community internet resources and underwent initial telephone screening to assess eligibility criteria. Participants who met eligibility criteria were administered the non-patient SCID (SCID–NP) to rule out the presence of an Axis I psychiatric disorder; a urine toxicology screen for drug use and an assessment of the participant's family history of psychiatric disorders were also performed. ^{Reference First, Spitzer, Williams and Gibbon23} Exclusion criteria included (current or past) Axis I psychiatric disorder, psychotropic drug treatment, substance misuse, a first-degree family member with an Axis I psychiatric disorder and the inability to provide written informed consent. All participants were White by self-report and drawn from a single geographic location (surrounding Glen Oaks, New York, USA). After complete description of the study, written informed consent was obtained from all participants. As shown in Table 1, the groups significantly differed in age (F_4,558=15.5, P<0.001). By design, somewhat older individuals were selectively recruited for the healthy control group so that they might be outside the window of maximal risk for onset of schizophrenia, schizoaffective disorder and bipolar disorder. As is typical in schizophrenia studies, males were over-represented among those with schizophrenia compared with the other groups (χ²=49.6, d.f.=1, P<0.001).

Genotyping

Genotyping was performed by 5′-exonuclease assay with allele-specific flourescence detection probes. As shown in online Fig. DS1, five single nucleotide polymorphisms (SNPs) encompassing the single protein-coding exon of BDNF were genotyped (listed in order of chromosomal position): rs4923463, rs6265 (the Val66Met polymorphism), rs11030104, rs2049045 and rs7103411. Single nucleotide polymorphisms were selected on the basis of three considerations:

1. (a) availability of reliable TaqMan assays at the time of initiation of the study, which was prior to the completion of the HapMap;

2. (b) coverage on both sides (3′ and 5′) of the single protein-coding exon; and

3. (c) minor allele frequency of at least 10% in White populations, to permit adequate power.

Genotyping reactions (5 μl) were performed in 384-well plates containing 10 ng of genomic DNA, 0.5 μmol of primers, 0.2 μmol of probes, and 2.5 μl of Master Mix (Applied Biosystems Inc.). The reaction thermal cycle programme consisted of 50°C for 2 min, 95°C for 10 min, followed by 40 cycles of 95°C for 15 s, 59°Cor 60°C for 1 min. End-point amplification genotypes were determined using an Applied Biosystems 7900 Sequence Detector with Sequence Detection System 2.0 software. Genotyping accuracy was verified by regenotyping at least 10% of the DNA samples, randomly selected. Genotyping accuracy was >99% and genotyping completion was >99%. All SNPs were in Hardy–Weinberg equilibrium in controls (all P>0.30).

Statistical analysis

Haplotype block structure was determined using Haploview version 3.32. ^{Reference Barrett, Fry, Maller and Daly24} Haplotype blocks were defined in accordance with Gabriel method ^{Reference Gabriel, Schaffner, Nguyen, Moore, Roy and Blumenstiel25} using default settings for all criteria. Using this method, a single haplotype block was identified with a very tight linkage disequilibrium structure (Fig. 1). A common haplotype (AGAGT), containing the valine-coding allele for rs6265, had a 74% frequency in the overall sample. The complementary haplotype (GAGCC) was the only other common haplotype (18% frequency), with several rare haplotypes also detected. PHASE 2.1.1 ^{Reference Stephens and Donnelly26} was then used to determine phase of alleles and assign haplotypes for each participant individually. Seven participants' samples (three with schizophrenia, two healthy controls, one with schizoaffective disorder and one with bipolar disorder) could not be phased with greater than 95% confidence and were excluded from subsequent analyses.

Fig. 1

Linkage disequilibrium plot of the five single nucleotide polymorphisms (SNPs) genotyped in the present study; inter-SNP r ² is displayed for each pair. D′ is at or near unity for all pairs of SNPs.

To reduce the number of multiple comparisons, analyses were conducted in a hierarchical fashion. Primary analyses were conducted comparing number of copies (zero, one or two) of the AGAGT haplotype, across members of each of the diagnostic groups. Pearson chi-squared tests permuted 500 000 times were used to empirically determine P-values. Groups were first examined individually (full matrix), and then certain groups were combined (e.g. all individuals with a major affective component to disorder) in order to test the hypothesis described above. Subsequent to significant effects of haplotype for a given comparison, individual genotypic effects of each constituent SNP were examined.

Limitations

As described above, our primary findings represent novel extensions of the BDNF association literature. However, it is important to emphasise that the genetic association occurs at the group level, and is not diagnostic for any individual case. Additionally, it should be noted that the sample sizes of the individual affective disorders groups were relatively modest for genetic association studies, and larger samples will be needed to confirm our results. Nonetheless, sample size for the primary, full-group comparisons was robust (total n approaching 600), yielding statistically significant results. In this context, it is notable that significant differences were obtained in sub-comparisons with smaller numbers (Table 2), but not in the largest two-group comparison (schizophrenia group v. controls, total n>400). This contrast suggests that Type I error is not a likely explanation of our results, and that significant results for the affective disorders group were less likely to be a result of an atypical healthy control sample. Although our results are consistent with prior theory and literature as described above, lack of additional replication samples means that the possibility of false-positive findings cannot be excluded. In designing replication studies, it is important to acknowledge the trade-off between large multisite studies (with increased ascertainment, diagnostic and environmental heterogeneity) v. the ascertainment of smaller yet potentially more reliably ascertained cohorts of participants (patients and controls). ^{Reference Brzustowicz42}

Population stratification is a potential confound in any case–control study. In our recent genomewide association study of a case–control cohort collected at our institution, ^{Reference Lencz, Morgan, Athanasiou, Dain, Reed and Kane43} we tested for stratification using 210 ancestry informative markers selected for maximal informativeness (minor allele frequencies >0.50 between ethnic groups) and did not observe any deviation from that predicted by chance, suggesting that undetected substructure is not present in our geographically homogeneous population. Moreover, none of the participants ascertained at the Zucker Hillside Hospital deviated from a single population as assessed by the structure program (http://pritch.bsd.uchicago.edu/software.html). We also note that, although undetected substructure in US White populations is a theoretical concern, empirical data collected to date suggests that self-identified race/ethnicity (SIRE) is sufficient with which to match study groups from the US population. Tang and colleagues ^{Reference Tang, Quertermous, Rodriguez, Kardia, Zhu and Brown44} examined this question in 3636 people assessed with SIRE information, genotyped with 326 microsatellite markers and analysed with the structure program. These investigators reported ‘a nearly perfect correspondence between genetic cluster and SIRE for major ethnic groups living in the United States’ (p. 273), and suggested that the critical information needed to avoid confounding is SIRE, not necessarily additional genetic marker information.

Mechanism

It is worth noting that the risk haplotype in the present study contains the Val66Met valine allele. Therefore, results of the present study and others listed above could be described as demonstrating that the Met allele (or haplotypes that carry it) may be protective against affective disorders. The Val66Met substitution is a logical candidate for a causative variant, in one or more ways. First, this polymorphism may diminish the dendritic localisation and secretory activity of BDNF, thereby altering the amount of mature protein available for activation of the TrkB pathway. ^{Reference Egan, Kojima, Callicott, Goldberg, Kolachana and Bertolino12} Second, it may affect the level and extracellular processing of proBDNF that acts through p75^NTR, downregulating synaptic plasticity through long-term depression via a bidirectional pathway. ^{Reference Woo, Teng, Siao, Chiaruttini, Pang and Milner45} Diminished synaptic strength among certain circuits, in particular excitatory glutamatergic networks, may contribute to a protective mechanism against development of affective disorders.

Although this mechanism is clearly speculative in terms of the pathophysiology of affective disorders, recent animal studies support this possibility. For example, BDNF and its receptor have been found in terminals critical to associative learning within the amygala, ^{Reference Agassandian, Gedney and Cassell46} and changes in BDNF expression in the amygdala have been linked specifically to the acquisition of fear-conditioned responses. ^{Reference Rattiner, Davis and Ressler10} Similarly, BDNF knockdown in the nucleus accumbens abolishes the learned avoidance response to aggression (social defeat stress); ^{Reference Berton, McClung, Dileone, Krishnan, Renthal and Russo11} chronic, but not acute, administration of antidepressants had the same effect. Future studies in humans can extend these observations by examining the relationship of BDNF variation with neuroanatomic and functional measures of the amygdala and basal ganglia.

This line of research holds promise to enhance our understanding not only of the mechanisms underlying affective disorders, but also their treatment. ^{Reference Duman and Monteggia20} Several recent studies have demonstrated that treatment with antidepressants or mood stabilisers upregulates BDNF expression. ^{Reference Chen, Peng, Li, Yang, Wu and Wang47} Moreover, BDNF polymorphisms may also affect response to both mood stabilisers and antidepressants. ^{Reference Choi, Kang, Lim, Oh and Lee48}

Finally, although results of the present study are consistent with prior data concerning the functional effects of the Val66Met polymorphism, it should be noted that the haplotype contained several markers that have not been previously examined. Whereas all five markers, including Val66Met, significantly differentiated healthy controls from the combined sample of people with affective illnesses (fourth row of Table 2), only rs7103411 consistently differentiated the diagnostic groups as effectively as the entire haplotype. It is possible that the conflicting results of prior studies examining only Val66Met reflect effects of different haplotypic backgrounds.

It should be noted that our survey of genetic variation at the BDNF locus was not exhaustive: the Phase II HapMap indicates that additional haplotypes exist within the region examined in the present study, and potential splicing variants in the 5′ region of the gene were not examined in the present study. It also cannot be ruled out that prior associations of Val66Met to affective disorders reflect linkage disequilibrium with a distal variant.

Nevertheless, results of the present study suggest that negative conclusions of recent meta-analyses ^{Reference Kanazawa, Glatt, Kia-Keating, Yoneda and Tsuang31,Reference Chen, Lawlor, Lewis, Yuan, Abdollahi and Timpson49} of BDNF Val66Met may be premature; notably, these meta-analytic reports combined studies across multiple ethnicities with very different baseline allele frequencies and excluded several positive reports from family-based samples. Moreover, the combined sample sizes in the psychiatric genetics literature may be inadequate at this point to reach definitive conclusions. A prominent recent example from the diabetes literature illustrates a seeming paradox in the relationship between sample size and detection of genetic associations. Specifically, the association of the PPARG Pro12Ala polymorphism with type 2 diabetes was initially identified in a sample of 91 people. ^{Reference Deeb, Fajas, Nemoto, Pihlajamäki, Mykkänen and Kuusisto50} Although several subsequent studies with hundreds or even thousands of participants failed to replicate the association, the most recent analysis of tens of thousands of participants has definitively confirmed the association. ^{Reference Zeggini, Scott, Saxena, Voight, Marchini and Hu51} Thus, further research on BDNF as a promising candidate for affective psychopathology is warranted, especially in samples that may be informative for future nosological refinements.