the mesolimbic and striatal-frontal systems (Sadock,
2008; Katzung, 2018).
4 DRD2 GENE POLYMORPHISM
The two single nucleotide polymorphisms (SNPs) of
the DRD2 gene, Taq1A and -141C Ins/Del
polymorphisms, may be linked to schizophrenia
susceptibility. Several studies have explored the link
between Taq1A polymorphisms and the risk of
developing schizophrenia. However, the outcomes of
these reports are conflicting. Some studies have
shown that the Taq1A polymorphism increases the
risk of developing schizophrenia. Similarly, the -
141C Ins/Del (rs1799732) polymorphism was
deemed to be related to the risk of schizophrenia as
well. However, these findings are inconsistent.
Several similar case-control studies were
conducted to determine the potential role of the
DRD2 gene polymorphisms in the incidence of
schizophrenia. For example, Arinami et al. (1997)
identified a positive correlation for -141C Ins/Del
with susceptibility for schizophrenia. The results of
studies reported by Betcheva et al. (2009) in the
Bulgarian community are consistent with the positive
correlations observed in different Caucasian
populations between the C957T (rs6277)
polymorphism and schizophrenia.
Two variants of G allele, which coincides with
the C allele in both the database and the literature for
the single nucleotide polymorphism, was defined as a
risk allele. After an initial study by Lawford et al.
(2005), which recorded a relationship between rs6277
and schizophrenia in an Australian (Caucasian)
population, three other studies documented markedly
higher frequencies of C alleles and C/C genes in
schizophrenic patients of European origin (natural
populations of Finland, Spain, and Russia). However,
case-control studies using Indian subjects did not
confirm a positive correlation with schizophrenia.
(Kukreti et al., 2006).
Moreover, the findings of two meta-analyses
using data from five studies or a Caucasian
population revealed a relationship between the C
allele and the C/C genotype with a combined odd
ratio of 1.42 (95% confidence interval (CI): 1.26-
1.61) and 1.45 (95% CI: 1.21–1.73), and the OR
estimates for the genotype were 1%. Since all positive
associations are found in European ancestral
populations, the effects of ancestry must be
understood and the genetic effects of this variant
should be tested across populations with different
ancestral descent (Betcheva et al., 2009).
5 CONCLUSIONS
Various studies suggest that Taq1A, -141C Ins/Del,
and C957T polymorphisms in the DRD2 gene play a
major role in the incidence of schizophrenia. They
can affect the pathophysiology and the degree of
severity of clinical symptoms experienced by
patients. Therefore, further studies on the
polymorphisms of the DRD2 gene at Taq1A, -141C
Ins/Del, and C957T are necessary.
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