Variant:
rs1799732 at chr11:113346252 in DRD2 (VIP)

Alleles (on + chromosomal strand): - > G
Alternate Names:: DRD2: -141C Ins/Del, g.16908668_16908669insG, g.4749_4750insC

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Clinical Annotations

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Variant Annotations

PharmGKB variant annotations provide information about variant-drug pairs based on individual PubMed publications. Each annotation represents information from a single paper and the goal is to report the information that the author states, not an interpretation of the paper. The PMID for supporting PubMed publications is found in the "Evidence" field.

Information presented, including study size, allele frequencies and statistics is taken directly from the publication. However, if the author does not correct p-values in cases of multiple hypotheses, curators may apply a Bonferroni correction. Curators attempt to report study size based on the actual number of participants used for the calculation of the association statistics, so the number may vary slightly from what is reported in the abstract of the paper. OMB Race Category information is derived from the paper and mapped to standardized categories. Category definitions may be found by clicking on the "OMB Race Category" link.

There are 15 annotations for this variant. Register or sign in to see them.

There are 12 disease-related annotations for this variant. Register or sign in to see them.

VIP Variant in DRD2

The -141C Ins/Del polymorphism of DRD2 has been reported to influence the outcome of both antipsychotic [Article:20194480] and addiction treatments [Articles:11920858, 16123753]. The -141C Ins/Del (rs1799732) polymorphism is located in the promoter region of the DRD2 gene and is found at an allele frequency of about 22% of the Japanese population. This allele is less common among Chinese and Caucasian populations (9%) [Article:9713903]. Allele frequencies are known for a number of different populations, and of these, the deletion polymorphism is the most common allele in only the Yoruban sample set see The ALlele FREquency Database.

A number of studies have shown that the -141C Ins/Del polymorphism of DRD2 appears to have a role in determining the response to antipsychotic drugs in schizophrenic patients, in which the Ins allele is associated with favorable treatment outcome (see Table1). But there are also contrary results reporting no association (Table1). A recent meta-analysis examined the relationship of DRD2 genetic variation and clinical response to antipsychotic treatment (risperidone, olanzapine, chlorpromazine, clozapine, and aripiprazole) [Article:20194480]. This analysis included six studies, which met the inclusion criteria for reported results on the -141C Ins/Del polymorphism, with a total sample size of 687 patients [Article:20194480]. The authors showed that the group of Del allele carrier was significantly associated with poorer antipsychotic drug response relative to the Ins/Ins genotype [Article:20194480]. The -141C Ins/Del variant has also been investigated in the context of substance addiction and treatments. Li and colleagues found a positive association between nasal inhaled but not injected heroin use and the -141C Ins/Del DRD2 polymorphism in Chinese subjects [Article:11920858]. Lerman et al. suggest that the -141C Ins/Del polymorphism may influence whether bupropion or nicotine replacement therapy (NRT) would be more effective for tobacco dependence treatment [Article:16123753]. The authors found that bupropion was more effective for patients who were homozygous for the Ins allele, whereas NRT appeared to be more helpful for patients who were homozygous for the Del allele [Article:16123753].

Note: The DRD2 gene is found on the minus chromosomal strand. Please note that for standardization, the PharmGKB presents all allele base pairs on the positive chromosomal strand, therefore the alleles within our variant annotations will differ (in a complementary manner) from those in this VIP summary that are given on the minus strand as reported in the literature.

Table: Effect of the -141C Ins/Del polymorphism on antipsychotics response in schizophrenic patients based on studies investigating association between DRD2 variants and response to antipsychotic drugs.

Subjects (population)	Antipsychotic drug	Treatment Duration	Response measurement	Genotyped DRD2 polymorphisms	-141C Ins/Del effect	Reference
151 schizophrenics 95 controls (Caucasian)	clozapine	-	GAS	-141C Ins/Del	No association	[Article:991813]
170 schizophrenics; 121 controls (Japanese)	antipsychotic drugs not specified	-	PANSS	-141C Ins/Del	No association	[Article:9858029]
49 schizophrenic inpatients (Japanese)	bromperidol or nemonapride	3 weeks	BPRS	-141C Ins/Del	Ins allele associated with greater improvement (only for anxiety-depression symptoms)	[Article:11505224]
73 schizophrenic patients (Japanese)	risperidone	8 weeks	PANSS	-141C Ins/Del; Taq1A	Ins-A2/Del-A1 diplotype associated with better response	[Article:14610521]
135 schizophrenic inpatients (Chinese)	chlorpromazine	8 weeks	BPRS	Del -	genotype associated with higher degree of improvement	[Article:15694263]
DSM-III-R or DSM-IV schizophrenics (183 Caucasian; 49 African-American)	clozapine	6 months	BPRS	-141C Ins/Del; Taq1A; Taq1B; and rs1125394	no association	[Article:15830237]
61 first-episode schizophrenia patients (41% African American; 28% Caucasian; 18% Hispanic; 5% Asian; 8% other)	olanzapine or risperidone	16 weeks	CGIIS	-141C Ins/Del; A-241G	-141C Del allele showed significantly longer time to respond relative to Ins/Ins homozygotes	[Article:16513877]
125 schizophrenia patients (Chinese)	risperidone	8 weeks	BPRS	-141C Ins/Del; Taq1B; rs1076562; Taq1A	no association	[Article:17105675]
128 schizophrenic inpatients (Han Chinese)	aripiprazole	4 weeks	PANSS	-141C Ins/Del; Taq1A; C957T; Ser311Cys	no significant effect	[Article:18926547]

BPRS: Brief Psychiatric Rating Scale; CGIIS: Clinical Global Impression Improvement Scale; GAS: Global Assessment Scale; PANSS: Positive and Negative Symptom Scale;
-141C Ins/Del (rs1799732); Taq1A (rs1800497); Taq1B (rs1079597); -241A>G (rs1799978); 957C>T (rs6277); Ser311Cys (rs1801028)

Key Publications:	Article:11505224 Article:11920858 Article:15694263 Article:16045195 Article:16123753 Article:9713903
Drugs / Other Molecules	Drug (5) Bromperidol ¹ bupropion ² chlorpromazine ³ heroin ⁴ nemonapride ⁵
Diseases	Schizophrenia ⁶ ⁷ Tobacco Use Disorder ⁸

Appendix

DRD2: \-141C Ins/Del

Genomic Variant & GenBank ID:	16833244 G>A on NT_033899.7
mRNA Variant & GenBank ID:	There are no changes to the DRD2 mRNA, but this variation causes a change in the ANKK1 mRNA
Protein Variant & GenBank ID:	There are no changes to the DRD2 protein, but this variation causes a nonsynonymous change in ANKK1.
dbSNP rs#:	[rs1800497]
GoldenPath Position:	chr11:112776038 (hg18)

Related Drugs Related Diseases

Connected Drugs

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Evidence	Drug
CA VA	aripiprazole
CA VA VIP	Bromperidol
VA VIP	bupropion
CA VA VIP	chlorpromazine
CA VA	clozapine
VIP	heroin
CA VA VIP	nemonapride
VA	nicotine
CA VA	olanzapine
CA VA	risperidone

Connected Drug Classes

Evidence	Drug Class
Clinical Annotation, Variant Annotation CA VA	antipsychotics

Connected Diseases

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Evidence	Disease
VA	Alcoholism
CA VA VIP	Schizophrenia
VIP	Tobacco Use Disorder

Publications related to rs1799732 at chr11:113346252: 16

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VA	Sexual dysfunction in male schizophrenia: influence of antipsychotic drugs, prolactin and polymorphisms of the dopamine D2 receptor genes. Pharmacogenomics. 2011. Zhang Xiang Rong, et al. [Article:21749219@PubMed]
VA	DRD2 promoter region variation predicts antipsychotic-induced weight gain in first episode schizophrenia. Pharmacogenetics and genomics. 2010. Lencz Todd, et al. [Article:20664489@PubMed]
CA VA	D2 receptor genetic variation and clinical response to antipsychotic drug treatment: a meta-analysis. The American journal of psychiatry. 2010. Zhang Jian-Ping, et al. [Article:20194480@PubMed]
CA VA	Effects of DRD2/ANKK1 gene variations and clinical factors on aripiprazole efficacy in schizophrenic patients. Journal of psychiatric research. 2009. Shen Yu-Chih, et al. [Article:18926547@PubMed]
VA	Association of the dopamine D2 receptor gene with alcohol dependence: haplotypes and subgroups of alcoholics as key factors for understanding receptor function. Pharmacogenetics and genomics. 2009. Kraschewski Adrian, et al. [Article:19603545@PubMed]
CA VA	The relationship between the therapeutic response to risperidone and the dopamine D2 receptor polymorphism in Chinese schizophrenia patients. The international journal of neuropsychopharmacology / official scientific journal of the Collegium Internationale Neuropsychopharmacologicum (CINP). 2007. Xing Qinghe, et al. [Article:17105675@PubMed]
VA VIP	Role of functional genetic variation in the dopamine D2 receptor (DRD2) in response to bupropion and nicotine replacement therapy for tobacco dependence: results of two randomized clinical trials. Neuropsychopharmacology : official publication of the American College of Neuropsychopharmacology. 2006. Lerman Caryn, et al. [Article:16123753@PubMed]
CA VA	DRD2 promoter region variation as a predictor of sustained response to antipsychotic medication in first-episode schizophrenia patients. The American journal of psychiatry. 2006. Lencz Todd, et al. [Article:16513877@PubMed]
CA VA VIP	Response to chlorpromazine treatment may be associated with polymorphisms of the DRD2 gene in Chinese schizophrenic patients. Neuroscience letters. 2005. Wu Shengnan, et al. [Article:15694263@PubMed]
VIP	[Clinical pharmacogenetics in the treatment of schizophrenia]. Nihon shinkei seishin yakurigaku zasshi = Japanese journal of psychopharmacology. 2005. Saito Manabu, et al. [Article:16045195@PubMed]
CA VA	Association study of 12 polymorphisms spanning the dopamine D(2) receptor gene and clozapine treatment response in two treatment refractory/intolerant populations. Psychopharmacology. 2005. Hwang Rudi, et al. [Article:15830237@PubMed]
VIP	Allelic association analysis of the dopamine D2, D3, 5-HT2A, and GABA(A)gamma2 receptors and serotonin transporter genes with heroin abuse in Chinese subjects. American journal of medical genetics. 2002. Li Tao, et al. [Article:11920858@PubMed]
CA VA VIP	The -141C Ins/Del polymorphism in the dopamine D2 receptor gene promoter region is associated with anxiolytic and antidepressive effects during treatment with dopamine antagonists in schizophrenic patients. Pharmacogenetics. 2001. Suzuki A, et al. [Article:11505224@PubMed]
CA VA	Lack of association between a polymorphism in the promoter region of the dopamine-2 receptor gene and clozapine response. Pharmacogenetics. 1998. Arranz M J, et al. [Article:9918131@PubMed]
CA VA	Functional polymorphism of -141C Ins/Del in the dopamine D2 receptor gene promoter and schizophrenia. Psychiatry research. 1998. Ohara K, et al. [Article:9858029@PubMed]
VIP	Case-control, haplotype relative risk and transmission disequilibrium analysis of a dopamine D2 receptor functional promoter polymorphism in schizophrenia. Schizophrenia research. 1998. Li T, et al. [Article:9713903@PubMed]

Cross-References

UCSC Golden Path:: chr11:113346252
dbSNP:: rs1799732
ALFRED:: SI000135J

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