Possible Association between Serotonin Transporter Gene Polymorphism and Suicide Behavior in Major Depressive Disorder

Article information

Psychiatry Investig. 2015;12(1):136-141
Publication date (electronic) : 2015 January 12
doi : https://doi.org/10.4306/pi.2015.12.1.136
1Department of Psychiatry, Soonchunhyang University College of Medicine, Seoul, Republic of Korea.
2Department of Psychiatry, University of Ulsan College of Medicine, Asan Medical Center, Seoul, Republic of Korea.
3Department of Psychiatry, Gangnam Eulji Hospital, Eulji University, Seoul, Republic of Korea.
4Department of Psychiatry, Korea University College of Medicine, Seoul, Republic of Korea.
Correspondence: Yong-Ku Kim, MD, PhD. Department of Psychiatry, College of Medicine, Korea University, Ansan Hospital, 123 Jeokgeum-ro, Ansan 425-020, Republic of Korea. Tel: +82-31-412-5140, Fax: +82-31-412-5144, yongku@korea.ac.kr
*These authors contributed equally to this work.
Received 2013 July 09; Revised 2013 December 18; Accepted 2014 March 26.

Abstract

Objective

The serotonin transporter (5-HTT) genes are major candidate genes for modulating the suicidal behavior. We investigated the association between serotonin transporter polymorphisms and suicidal behavior in patients with major depressive disorder (MDD).

Methods

Serotonin transporter intron 2 VNTR polymorphism (5-HTTVNTR) and serotonin transporter linked polymorphic region polymorphism (5-HTTLPR) were analyzed in 132 depressed patients with suicidal attempt as well as in 122 normal controls. Hamilton's 17-item Depression Rating Scale (HDRS), the Risk-Rescue rating system (RRR) and the Lethality Suicide Attempt Rating Scale updated (LSARS-II) were assessed for the depressed patients.

Results

Although not statistically significant, a trend was found such that the 10/10 and 10/12 alleles of 5-HTTVNTR were more common in suicidal subjects than in control subjects. Comparing allele frequency, those with a 10 allele or 10 allele carriers were higher in suicidal subjects than in control subjects. No difference was noted in 5-HTTLPR genotypes and haplotype distribution between the suicidal subjects and control subjects. The RRR scores in subjects with the 10/10 5-HTTVNTR genotype or 10 5-HTTVNTR allele were significantly lower than those in subjects with other genotypes.

Conclusion

These results show the possibility that 10 allele of 5-HTTVNTR is related to suicidal behavior in the suicidal subjects with MDD and suggest that 12 allele of 5-HTTVNTR might be related to more lethality in the suicidal subjects with MDD.

INTRODUCTION

Across the globe, approximately one million people kill themselves every year.1 Suicide represents a serious public health problem worldwide. According to the Organization for Economic Cooperation and Development (OECD), South Korea has one of the higher rates of suicide, among OECD countries.2 Approximately 60% of all suicides occur in the context of mood disorders.3 The serotonin transporter (5-HTT) is the major determinant of serotonin inactivation following serotonin release at synapses, and it is the target for many antidepressants. Moreover, a decrease in central 5-HTT has also been observed in suicide victims with mood disorders.4 Genetic factors have been generally implicated in the etiology of suicide, although the precise mechanism and amount of genetic contribution have not yet been established.5 Therefore, the 5-HTT gene is considered to be a promising candidate to explain various psychiatric disorders, including suicidal behavior.

The serotonin transporter gene is located on chromosome 17q11.1-q12, and two polymorphisms have been reported: first, the various number of tandem repeats (VNTR) of 17 base pairs in intron 2 with three different numbers repeated (9, 10, 12)6; second, the bi-allelic insertion/deletion polymorphism in the promoter region, with the deletion (or short=S) and the insertion (or=L) alleles localized upstream from the transcription start site.7

The VNTR polymorphism on intron 2 (5-HTTVNTR) was previously thought to be functionless, however, a recent study with transgenic mice demonstrated that 5-HTTVNTR acts as a transcriptional regulator within an area of the hindbrain, and that the 12-repeat allele was better able to induce transcription than was the 10-repeat analog.8 Many studies have demonstrated associations between the 5-HTTVNTR and major depressive disorder.9,10 There are also many studies investigating the association between 5-HTTVNTR and suicide.11,12,13,14

On the other hand, S allele in serotonin transporter linked polymorphic region polymorphism (5-HTTLPR) has been reported to be associated with reduced serotonin uptake in platelets compared with L allele.15,16 An association between this polymorphism and major psychiatric disorders has been reported,17,18 whereas other studies have reported no association.19,20

In this study, we investigated the associations between the serotonin transporter gene polymorphisms (5-HTTVNTR and 5-HTTLPR) and suicide behavior of major depressive disorder patients.

METHODS

Subjects

One hundred thirty-two subjects with major depressive disorder were recruited from among patients admitted to the emergency rooms of the Korea University Medical Center Ansan Hospital following suicide attempts. Initial psychiatric interviews were conducted by psychiatrist within 1 and again 24 hours after admission to the emergency room, and the subjects were diagnosed according to DSM-IV criteria. We defined suicide attempt as self-harming behaviors with at least some intent to end one's life. Subjects were excluded if their self-injurious behaviors were determined to have no suicidal intention or ideation.

Subjects suffering from alcohol or substance dependence or who had any comorbid diagnosis including bipolar disorder, schizophrenia or dementia based on DSM-IV criteria were excluded from the study. Patients with serious or unstable medical illness were also excluded from the study. There were twenty-eight patients who were smokers who were included in the present study. All subjects were at least 18 years of age.

The control subjects consisted of randomly selected healthy individuals who visited the Korea University Ansan hospital for regular health screenings. Subjects were excluded if they had any self-reported personal, familial psychiatric history or psychotropic medication history, or if they had scores of ≥10 on the Beck Depression Inventory (BDI) or ≥40 on the State-Trait Anxiety Inventory (STAI). Finally, 122 control subjects were selected. The study protocol was approved by the Ethics Committee of Korea University, and written informed consent was obtained from all subjects. All patients and control subjects were at least 18 years of age and of Korean ethnicity.

Clinical evaluation

Individuals in the patient groups were evaluated independently by two trained psychiatrists. Diagnoses and ratings were decided by mutual consent of the psychiatrists. The evaluations consisted of reviews of psychiatric and medical histories, current and previous medication and alcohol intake, followed by a semi-structured interview for the purpose of establishing DSM-IV criteria diagnosis. We also administered Hamilton's 17-item Depression Rating Scale.21 We evaluated the lethality of individual suicide attempts using Weisman and Worden's Risk-Rescue rating (RRR) system22 and the Lethality Suicide Attempt Rating Scale-updated (LSARS-II).23,24

According to the RRR system, lethality is expressed as the ratio of five risk and five rescue factors that are operationally defined, weighted, and scored.25 The LSARS23 is an 11-point offering an appendix listing drugs, chemicals and lethal ranges of ingestion by body weight. The LSARS-II24 includes a table of drugs and chemicals, based on current medications and recent data on the minimum lethal doses in humans.25

Blood sample collection and testing

After written informed consent was obtained, venous blood was drawn from antecubital vein of each subject.

Genotyping

Genotyping of the 5-HTTVNTR was carried out using a previously described method.9 Genomic DNA was isolated from buffy coat by a genomic DNA purification kit (Promega, Madison, WI, US). Target DNA was amplified via polymerase chain reaction with oligonucleotide primers 8224(5'-GTCAGTATCACAGGCTGCGAG) and 8223(5'-TGTTCCTA GTCTTACGCCAGTG). This primer pair amplifies across the VNTR region of intron 2 that contains the 17 bp repetitive element. PCR was performed in a final volume of 25 uL containing 50 ng of genomic DNA, 0.2 mM dNTPs, 10 pmoL of each primer, 10 mM Tris-HCl (pH 8.3), 50 mM KCl, 1.5 mM MgCl2, 0.01% gelatin and 1 unit of Taq DNA polymerase. PCR amplification consisted of 35 cycles at 95℃ (1 min), 58℃ (1 min) and 72℃ (1 min). Amplified fragments were separated on 3% agarose gels, and bands were visualized via ethidium bromide staining and ultraviolet transillumination.

For the polymerase chain reaction (PCR) analysis in 5-HTTLPR, the forward primer 50-GGC GTT GCC GCT CTG AAT TGC-30 and the reverse primer 50-GAG GGA CTG AGC TGG ACA ACC CAC-30 were employed. A 25 mL PCR analysis was performed according to a protocol previously described.16 PCR products were separated on 3% agarose gels supplemented with ethidium bromide to allow identification of the long (528 bp) and the short (484 bp) variants.

Statistical analysis

Pearson chi-square tests were performed in order to test the categorical variables (e.g., gender and diagnosis) to test for deviations from Hardy-Weinberg equilibrium. Group mean differences were ascertained using a Student's t-test or analysis of variance (ANOVA) according to the number in each group. Haplotype analysis of serotonin transporter gene polymorphism was performed. A probability value of p<0.05 was considered statistically significant. Probability values were corrected by multiplying the number of comparisons made (Bonferroni correction). All statistical analyses were performed with SPSS version 12.01 for Windows.

RESULTS

The gender distribution did not differ significantly between control subjects (63 males/59 females) and suicidal subjects (53 males/79 females; p=0.07). There was no significant difference in the age distribution between suicidal subjects and control subjects (34.9±13.3 years, mean±SD in suicidal subjects and 34.1±12.7 years in control subjects, p=0.64). Methods of suicide attempt included drug ingestion (n=53, 40.1%), wrist cutting with superficial laceration (n=15, 11.3%), wrist cutting with deep laceration (n=22, 16.7%), pesticide or agricultural chemical ingestion (n=27, 20.5%), fall down (n=6, 4.5%), hanging (n=3, 2.3%), and miscellaneous other methods (n=6, 4.5%).

Table 1 shows the distribution of 5-HTTVNTR genotypes for the two groups. We found few subjects with a 10/10 genotype in either group. The genotype distributions for the two groups were in Hardy-Weinberg equilibrium. Despite not reaching statistical significance (p=0.08), the incidence of 10/10 and 10/12 genotypes was higher in suicidal subjects than in the control subjects. Comparing allele frequency, 10 allele or 10 allele carriers were more frequently found in suicidal subjects than in control subjects. After Bonferroni correction, the statistical significance disappeared.

Table 1

Distributions of 5-HTTVNTR polymorphism and allele frequencies of the subjects

Table 2 shows the distribution of 5-HTTLPR genotypes for the two groups. We found few subjects with L/L genotype in either group. The genotype distributions for the two groups were in Hardy-Weinberg equilibrium. There was no significant difference in 5-HTTLPR genotype distribution between suicidal subjects and control subjects.

Table 2

Distributions of 5-HTTLPR polymorphism and allele frequencies of the subjects

Haplotype frequencies calculated from the genotypic data for both groups are presented in Table 3. No difference was noted in haplotype distribution between the suicidal subjects and control subjects.

Table 3

Estimated distribution of haplotype frequencies for 5-HTTLPR and VNTR alleles in suicide subjects with MDD and control subjects

Across all participants, HDRS, LSARS-II, RRR scores were 20.3±8.5, 4.0±2.1, 34.3±15.0 respectively. Table 4 shows the scores on three psychiatric scales according to 5-HTTVNTR genotype. There were no significant differences in the HDRS and LSARS-II according to the 5-HTTVNTR genotype. The RRR score in the subjects with 10/10 genotype of 5-HTTVNTR polymorphism was significantly lower than those in the subjects with other genotypes. The RRR score of the subjects with 10 allele was significantly lower than that of the subjects with 12 allele. After Bonferroni correction, the statistical significance sustained. The RRR score of 10 allele carriers were lower than that of 10 allele non-carriers (data not shown, p=0.028). After Bonferroni correction, the statistical significance disappeared.

Table 4

Clinical characteristics according to the serotonin transporter gene polymorphism (5-HTTVNTR) in suicidal subjects with major depressive disorder

There were no significant differences in the HDRS, LSARS-II, RRR scores according to the 5-HTTLPR polymorphism (Table 5).

Table 5

Clinical characteristics according to the serotonin transporter gene polymorphism (5-HTTLPR) in suicidal subjects with major depressive disorder

DISCUSSION

The aim of the present study was to identify the role of a serotonin transporter polymorphism on suicide behavior in major depressive disorder.

In this study, we found less number of the subjects with 10/10 than that of the subjects with other genotypes in control subjects and suicidal subjects, which is similar to rates found in other Asian populations.13 In this study, we demonstrated that the presence of the 10 allele was more frequent in suicidal subjects than in control subjects. In line with the present study, an earlier study found a significant association between suicide completion and the presence of at least one copy of the 5-HTTVNTR 10 allele.12 Further investigation regarding the frequencies of concurrence of tryptophan hydroxylase (TPH) and 5-HTTVNTR containing "lower activity" alleles (C/C and 10/10, respectively) revealed higher frequencies of lower activity in 5-HTT and TPH genotype combinations in suicidal victims than in control subjects.26 In a study performed in a Chinese population, however, no association was demonstrated between the 5-HTTVNTR polymorphism and suicidal history in mood disorder patients.27 It is difficult to conclude the association between the 5-HTTVNTR polymorphism and suicidal attempts was due to major depressive dis-order, because that study was performed with participants with bipolar disorder or major depressive disorder who had an attempted suicide.

For 5-HTTLPR genotype, we could not find higher frequency of the genotype with lower activity in suicide subjects. A meta-analysis including many psychiatric disorders revealed significant association between 5-HTTLPR polymorphism and suicide.28,29 In line with the present study including only major depressive disorder, however, there are many negative association studies between 5-HTTLPR and suicidal behavior in the patients with each specific psychiatric disorder.30,31

In the present study, no difference was noted in haplotype distribution between the suicidal subjects and control subjects. Similary, it was reported no statistically significant differences between serotonin transporter genotypes of controls and suicide victims.14 On the Contrary, It was reported a trend towards an increase of 5-HTTLPR allele L and 5-HTTVNTR allele 10 in Croatian suicide victims.6 Across all studies investigating links between haplotype and rate of suicide completion, however, there does appear to be a trend such that haplotypes that include 10 allele of 5-HTTVNTR are more frequently found in suicide victims. Regarding suicide attempts, it was found that the L10 haplotype in Russian females was associated with suicidal behavior, although the association was not significant after Bonferroni correction.11 With respect to patients of Asian ethnicity, neither the 5-HTTVNTR and 5-HTTLPR, nor the haplotype frequencies of these genes was shown to be significantly different between inpatients with suicidal attempt of different psychiatric disorders and controls in a Chinese population.13

Decreased levels of platelet 5-HTT have been observed in depressive patients.32 Furthermore, the impulsivity that often leads to suicide was significantly correlated with low 5-HTT in suicidal attempters.33 Because the 10-repeat allele displayed lower transcriptional activity than the 12-repeat allele,8,34 it is possible that the 10-repeat allele could be a contributing factor for suicide. If so, this would support findings in the present study. Contrary to previous in vitro data, Bah and colleagues35 assessed the availability of serotonin 5-HTT in male suicide attempters with single photon emission computed tomography and found that the 12-repeat allele was related to low 5-HTT availability in whole brain. However, they reported that the abnormality in suicidal depression was localized to parts of the prefrontal cortex.36 Further studies with a larger number of subjects are needed in order to verify the 5-HTT contribution to activity in a specific brain region.

In the present study, LSARS-II scores did not differ with both serotonin transporter polymorphisms. In 5-HTTVNTR, however, RRR scores in the subjects with the 10/10 genotype or 10 carriers were lower than those in the subjects with other genotypes, indicating that there were fewer fatal attempts in 10/10 or 10 carriers. In contrast, other studies suggest the prevalence of 10 carriers was higher in completed suicides, therefore it is difficult to obtain a clear conclusion regarding the effect of 5-HTTVNTR on the lethality of suicide.

Some potential limitations of the present study should be noted. First, the distribution of 5-HTTVNTR in Korean is different from among Caucasians. The ratio of the 10/12 allele in control subjects in the present study was 0.09/0.91, whereas the frequency of the 12 allele in general Caucasian population is 0.54-0.66.37 Furthermore, the 9 allele was absent in the Korean population. The ratio of the S/L allele among our subjects was approximately 0.76/0.24, while the corresponding figure for Caucasians is 0.43/0.57. As such, due to such ethnic differences in the distribution of the genotype, the results of this study are not necessarily applicable to other ethnicities. Second, the methods of suicide attempt were not controlled, although there is no statistical difference in the prevalence of fatality in suicidal attempts. Third, there was not a depressed group without a suicidal attempt to stand as an additional control group, and the total number of subjects was small. Fourth, controls were not clinically evaluated and the scale for stress or personality trait was not given to these subjects.

Notwithstanding of these limitations, this study is an important first step in examining the potential association between serotonin transporter gene polymorphisms and suicide behavior of major depressive disorder patients in a Korean population. Finally, identification of other polymorphisms which are related to 5-HTT activity or serotonin would be useful in identifying the role of the 5-HTT gene in the pathogenesis of suicidal behavior.

Acknowledgments

This study was supported by a grant of the Korean Health Technology R&D Project, Ministry of Health & Welfare, Republic of Korea (A120051).

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Table 1

Distributions of 5-HTTVNTR polymorphism and allele frequencies of the subjects

Table 1

Genotypes: χ2=5.12, df=2, p=0.08(pcorr=0.16); alleles: χ2=4.29, df=1, p=0.04 (pcorr=0.08); allele carriers: χ2=4.93, df=1, p=0.026 (pcorr=0.052). 10+: 10 carrier, 10-:10 non-carrier. *Hardy-Weinberg equilibrium test for suicidal group: χ2=2.969, df=1, p=0.08, Hardy-Weinberg equilibrium test for control group: χ2=2.668, df=1, p=0.10. pcorr: p-value after Bonferroni correction, MDD: major depressive disorder

Table 2

Distributions of 5-HTTLPR polymorphism and allele frequencies of the subjects

Table 2

Genotypes: χ2=0.65, df=2, p=0.72; alleles: χ2=0.001, df=1, p=0.98. *Hardy-Weinberg equilibrium test for suicidal group: χ2=0.50, df=1, p=0.48, Hardy-Weinberg equilibrium test for control group: χ2=0.20, df=1, p=0.66. MDD: major depressive disorder

Table 3

Estimated distribution of haplotype frequencies for 5-HTTLPR and VNTR alleles in suicide subjects with MDD and control subjects

Table 3

*χ2=4.70, df=3, p=0.20. MDD: major depressive disorder, VNTR: various number of tandem repeats

Table 4

Clinical characteristics according to the serotonin transporter gene polymorphism (5-HTTVNTR) in suicidal subjects with major depressive disorder

Table 4

*Kruskal-Wallis test. HDRS: Hamilton's 17-item Depression Rating Scale, LSARS-II: the Lethality Suicide Attempt Rating Scale-updated, RRR: Risk-Rescue rating (RRR) system, pcorr: p-value after Bonferroni correction

Table 5

Clinical characteristics according to the serotonin transporter gene polymorphism (5-HTTLPR) in suicidal subjects with major depressive disorder

Table 5

*Kruskal-Wallis test. HDRS: Hamilton's 17-item Depression Rating Scale, LSARS-II: the Lethality Suicide Attempt Rating Scale-updated, RRR: Risk-Rescue rating (RRR) system