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Schizophrenia is a psychiatric syndrome that affects approximately 1 % of the world population and is among the top 10 reasons for disability. In this case-control study, we investigated the association between 15 insertion/deletion (Indel) polymorphisms and schizophrenia risk using pooled samples. In the present case-control study, 361 individuals with schizophrenia and 360 healthy individuals were included in the study. We examined the insertion/deletion polymorphisms in
Schizophrenia is a common severe mental illness. Twin and other studies have consistently shown that there is a large genetic component to schizophrenia, with heritability estimated at around 80 %. Genome-wide association studies showed that multiple common variants, each with small effect, are associated with schizophrenia. More than 100 loci are significantly associated with schizophrenia (McCutcheon et al., 2020[
Both single nucleotide polymorphisms (SNPs) and Insertion/deletions (Indels) generally are abundant in human genomes. Although, Indels discovery efforts have lagged significantly behind SNPs discovery efforts, numerous Indels have been identified. Many of Indels have been identified within known genes and they might be located in the promoters and exons of genes, where gene function would be expected to be influenced the greatest (Mills et al., 2006[
In the present case-control study, 361 individuals with schizophrenia (267 males, 94 females; mean age ± SD = 41.5 ± 13.0 years) and 360 healthy individuals (267 males, 93 females; mean age ± SD = 39.8 ± 11.2 years) were included in the study, as reported previously (Taghipour et al., 2019[
Using the Epi Info software (version 7.2.2.6), assuming a statistical power of 0.80, α=0.05, case/control ratio equal to 1.0, 20 % frequency of the Del alleles for Indel polymorphisms, and OR=1.50, a minimum of 270 patients and 270 controls would be needed to identify a real difference in allelic frequency between the schizophrenia patient and healthy control groups. It should be noted that here 361 schizophrenia and 360 controls were included in the present case-control study.
Considering that the use of pooled samples for estimation of allelic frequencies is simple, inexpensive and fast method, this method was used in the present study to compare allelic frequencies of 15 Indels polymorphisms between the schizophrenia patients and control group. Genomic DNA was extracted from blood samples by boiling method (Newton, 1995[
The pooled DNA samples and DNA of a heterozygous individual (as a calibrator sample) were used for PCR. The specific forward and reverse primers for PCR were shown in the Supplementary information. After PCR, on gel electrophoresis, two bands were observed for the Ins and Del alleles. The intensity of the Ins and Del bands in pooled samples and heterozygote sample, was measured and the allelic frequencies in pooled samples were estimated using the method described previously (Saadat et al., 2019[
The ORs (odds ratios) and the 95 % confidence intervals (95 % CIs) indicate the association between polymorphisms and schizophrenia. In statistical comparisons, the Ins alleles were used as reference alleles (OR=1.0). Data was analyzed by SPSS software version 25. The logistic regression was used and the statistical significance level was set at a p-value of 0.05.
Data on allelic frequencies of the studied Indel genetic polymorphisms in schizophrenia patients and control group were summarized in Table 1
However, it should be noted that significant differences were not observed in the other insertion/deletion polymorphisms studied in this research (Table 1
In this study, we used a simple, fast, inexpensive, and accurate method for estimating the allelic frequency of 15 insertion/deletion polymorphisms in pooled samples so that we could examine more genes in the appropriate sample size in a short time.
The TPA Alu+/Alu- is a functional polymorphism and might play a role in the protein secretion rate or protein primary structure (Jern et al., 1999[
In addition, the human chromosome segment 6p21.1-p22.3 has a significantly higher number of susceptible loci, including the HLA, suggesting that components of the immune system are associated with the risk of schizophrenia (Saadat, 2013[
Finally, we should mention major limitations of the present study. By comparing the allelic frequency between schizophrenia and control groups using pooled samples, we cannot compare genotypes of the cases and controls with each other and investigate the effects of environmental factors and genotypes simultaneously. Also, it is impossible to study the potential interactive effects of associate genes. As mentioned earlier, the use of pooled sample method is accompanied by a reduction in costs and time, and the researcher can simply examine a larger number of genetic polymorphisms.
In summary, the HLA-G 14bp Indel and tPA Alu Indel polymorphisms were associated with schizophrenia. Future case-control genetic association studies are needed to conclude that these polymorphisms are risk factors for schizophrenia.
Ethical approval was obtained from Shiraz University Ethics Research Committee.
The authors declare no conflicts of interest.
Authors are indebted to the participants for their close cooperation.