Elial cell line [19]. Elevated expression of survivin was also observed in RCC tissues compared with adjacent normal tissues [19,32]. RCC patients with high survivin levels had a significantly shorter overall survival time than those with low levels [33,34]. In other words, decreased miR-27a levels might reduce the incidence of RCC through suppressing the expression of survivn indirectly. That was why we focus on the pre-miR-27a polymorphism in RCC patients. In this study, there were more hypertension patients and diabetics among the cases than among the controls, indicating that there was potential Methionine enkephalin custom synthesis association between the two factors and RCC. We also found that rs895819 had multiplicative interactions with hypertension. It has been reported that certain types of renal tumors and cancer treatment could cause hypertension [35,36] and a history of diabetes has been linked to renal cell cancer risk inseveral cohort studies [37], but its role independent of those of obesity and hypertension has not been demonstrated conclusively. Besides, our results indicated that the individuals with G allele have a reduced RCC risk in non-smokers. Cigarette smoking is the most consistently established causal risk factor for RCC, accounting for approximately 20 of cases of RCC [38]. Compared to never smokers, risk increased about 50 in male and 20 in female smokers [39]. Furthermore, after stratification for RCC clinical stage, it appeared that rs895819 GG genotype had a decreased risk of RCC with localized clinical stage. Thus, it was plausible that the variation was 57773-65-6 involved in the lower stage RCCs. However, this hypothesis needs to be confirmed in further studies. As to the association between genotypes and overall survival of RCC, there was no significant result. The reason for this discrepancy may be that the mortality rate of our survival analysis is low due to our short follow-up time and the biological mechanisms that underlie the incidence of RCC may be different from those underlying prognosis, and even if the miR-27a polymorphism is involved in the etiology of RCC, that does not necessarily mean that it affects the outcome. When interpreting our results, several limitations should be concerned. Firstly, our case-control study was a hospital-based study and it could not provide a good representation of overall populations. Nevertheless, the G allele frequency in our controls was similar to that in the HapMap database. Besides, the genotype distributions of the polymorphism in our controls conformed to HWE. Thus, the selection bias was unlikely to be substantial. Secondly, our sample size was relatively small. However, we had 83 power to detect a minimal OR of 0.68 with an exposure frequency of 30 under the current sample size. Thirdly, we did not perform the gene-environment interaction analysis due to lack of the detailed information of environment factors, such as occupational exposures, diet, and physical activities. However, our study also had several strengths. Firstly, it was the first study to investigate the association between pre-miR-27a rs895819 polymorphism and susceptibility to RCC. Secondly, we matched cases and controls by age and sex, 1313429 and we obtained the results by adjustment of age, sex, smoking, drinking status, hypertension, and diabetes, which could reduce the influence of confounding factors. In conclusion, our results provided the first insight into the contribution of pre-miR-27a rs895819 polymorphism to the risk of R.Elial cell line [19]. Elevated expression of survivin was also observed in RCC tissues compared with adjacent normal tissues [19,32]. RCC patients with high survivin levels had a significantly shorter overall survival time than those with low levels [33,34]. In other words, decreased miR-27a levels might reduce the incidence of RCC through suppressing the expression of survivn indirectly. That was why we focus on the pre-miR-27a polymorphism in RCC patients. In this study, there were more hypertension patients and diabetics among the cases than among the controls, indicating that there was potential association between the two factors and RCC. We also found that rs895819 had multiplicative interactions with hypertension. It has been reported that certain types of renal tumors and cancer treatment could cause hypertension [35,36] and a history of diabetes has been linked to renal cell cancer risk inseveral cohort studies [37], but its role independent of those of obesity and hypertension has not been demonstrated conclusively. Besides, our results indicated that the individuals with G allele have a reduced RCC risk in non-smokers. Cigarette smoking is the most consistently established causal risk factor for RCC, accounting for approximately 20 of cases of RCC [38]. Compared to never smokers, risk increased about 50 in male and 20 in female smokers [39]. Furthermore, after stratification for RCC clinical stage, it appeared that rs895819 GG genotype had a decreased risk of RCC with localized clinical stage. Thus, it was plausible that the variation was involved in the lower stage RCCs. However, this hypothesis needs to be confirmed in further studies. As to the association between genotypes and overall survival of RCC, there was no significant result. The reason for this discrepancy may be that the mortality rate of our survival analysis is low due to our short follow-up time and the biological mechanisms that underlie the incidence of RCC may be different from those underlying prognosis, and even if the miR-27a polymorphism is involved in the etiology of RCC, that does not necessarily mean that it affects the outcome. When interpreting our results, several limitations should be concerned. Firstly, our case-control study was a hospital-based study and it could not provide a good representation of overall populations. Nevertheless, the G allele frequency in our controls was similar to that in the HapMap database. Besides, the genotype distributions of the polymorphism in our controls conformed to HWE. Thus, the selection bias was unlikely to be substantial. Secondly, our sample size was relatively small. However, we had 83 power to detect a minimal OR of 0.68 with an exposure frequency of 30 under the current sample size. Thirdly, we did not perform the gene-environment interaction analysis due to lack of the detailed information of environment factors, such as occupational exposures, diet, and physical activities. However, our study also had several strengths. Firstly, it was the first study to investigate the association between pre-miR-27a rs895819 polymorphism and susceptibility to RCC. Secondly, we matched cases and controls by age and sex, 1313429 and we obtained the results by adjustment of age, sex, smoking, drinking status, hypertension, and diabetes, which could reduce the influence of confounding factors. In conclusion, our results provided the first insight into the contribution of pre-miR-27a rs895819 polymorphism to the risk of R.