Effects of functional genetic polymorphisms in the<i>CYP19A1</i>gene on prostate cancer risk and survival

Kanda, Sohei; Tsuchiya, Norihiko; Narita, Shintaro; Inoue, Takamitsu; Huang, Mingguo; Chiba, Shuji; Akihama, Susumu; Saito, Mitsuru; Numakura, Kazuyuki; Satoh, Shigeru; Saito, Seiichi; Οhyama, Chikara; Arai, Yoichi; Ogawa, Osamu; Habuchi, Tomonori

doi:10.1002/ijc.28952

Cited by 33 publications

(24 citation statements)

References 31 publications

(64 reference statements)

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“…Although it is unclear if decreased L‐plastin expression is defined by genetic factors or is the result of other pathways, it is interesting to note that the homozygous genotype of SNP −1,687 (T/T), which reduced the promoter activity of L‐plastin in prostate cancer cells, was related to an improved prognosis for prostate cancer patients. Previous studies on SNP‐related prostate cancer susceptibility and prognosis indicated that CYP19A1 polymorphisms influence prostate cancer risk and survival by modifying promoter activity, with subsequent effects on the sex hormone environments . In the present study, we demonstrated that SNP −1,687 (T/T) occurred more frequently in the healthy individuals than in the prostate cancer patients compared with the (C/C) and (C/T) genotypes.…”

Section: Discussionsupporting

confidence: 58%

An NKX3.1 binding site polymorphism in the l-plastin promoter leads to differential gene expression in human prostate cancer

et al. 2015

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The L-plastin gene is involved in the invasion and metastasis of prostate cancer. However, the molecular mechanisms underlying L-plastin transcription are unclear. We hypothesize that the occurrence of polymorphic genetic variations in the L-plastin promoter might affect an individual's susceptibility to prostate cancer. In this study, we identified a single nucleotide polymorphism (SNP) at position 21,687 in the L-plastin promoter by genotype sequencing. The SNP 21,687 showed different transcriptional activity in the luciferase assay in vitro. The TRANSFAC software was applied to predict the multiple cis-elements, and luciferase assay was used to further identify the L-plastin regulatory region. We performed EMSAs, supershift assays and ChIP-qPCR demonstrated that the transcriptional suppressor NKX3.1 binds to the SNP site of the L-plastin promoter. SNP 21,687 (T/T) led to an increase in the affinity of NKX3.1 for L-plastin promoter, resulted in lower levels of L-plastin RNA and protein expression. Furthermore, we collected and sequenced samples from 640 individuals (372 prostate cancer patients and 268 healthy controls) from 2000 to 2013. The results showed that SNP 21,687 (T/T) occurred more frequently in the healthy individuals than that in the prostate cancer patients compared to SNP 21,687 (C/C). Similarly, SNP 21,687 (T/T) genotype occurred more frequently compared to SNP 21,687 (C/C) genotype in the patients with low and moderately differentiated tumors. In conclusion, SNP 21,687, located in the NKX3.1 binding site within the L-plastin promoter, might reduce the expression of L-plastin and potentially decrease the tumorigenesis and progression of prostate cancer. This SNP could be a potential prognostic factor for prostate cancer.

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Section: Discussionsupporting

confidence: 58%

An NKX3.1 binding site polymorphism in the l-plastin promoter leads to differential gene expression in human prostate cancer

et al. 2015

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“…CYP19A1 encodes an enzyme that catalyzes the conversion of androgens to estrogens. Recent studies have suggested that functional genetic polymorphisms in the CYP19A1 gene may modify serum and/or intratumoral sex hormone levels and therefore influence prostate cancer risk and survival (Latil et al 2001, Suzuki et al 2003, Tsuchiya et al 2006, Kanda et al 2015. The androgen transporter gene SLCO2B1 also has a polymorphism that has been associated with prostate cancer risk and outcome (Yang et al 2011).…”

Section: Ar In Prostate Cancer Initiationmentioning

confidence: 99%

Androgens and androgen receptor signaling in prostate tumorigenesis

Zhou¹,

Bolton²,

Jones³

2014

Journal of Molecular Endocrinology

165

112

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Androgens and androgen receptor (AR) signaling are necessary for prostate development and homeostasis. AR signaling also drives the growth of nearly all prostate cancer cells. The role of androgens and AR signaling has been well characterized in metastatic prostate cancer, where it has been shown that prostate cancer cells are exquisitely adept at maintaining functional AR signaling to drive cancer growth. As androgens and AR signaling are so intimately involved in prostate development and the proliferation of advanced prostate cancer, it stands to reason that androgens and AR are also involved in prostate cancer initiation and the early stages of cancer growth, yet little is known of this process. In this review, we summarize the current state of knowledge concerning the role of androgens and AR signaling in prostate tissue, from development to metastatic, castration-resistant prostate cancer, and use that information to suggest potential roles for androgens and AR in prostate cancer initiation.

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“…A case-control study researched the relationship between SNPs in cytochrome P450 family 19 subfamily A member 1 (CYP19A1) and metastatic PCa. They found that patients with the minor variant rs4775936 had decreased chances for survival and verified their discovery in two commonly studied metastatic PCa cell lines, DU145 and PC3 [29]. rs2228013 in NKX3.1 could increase the metastasis in younger PCa patients [30].…”

Section: Discussionmentioning

confidence: 83%

Functional analysis implicating the SNP rs61552325 in ERBB2 as an effector for androgen-insensitive prostate cancer cell invasion

Xin

Chen

et al. 2017

Oncotarget

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BackgroundAs one of the most common cancers in men, the pathogenesis of prostate cancer has been widely researched. Aberrant activation of the erb-b2 receptor tyrosine kinase 2 (ERBB2) has been found to play a critical role in metastatic prostate cancer. In our previous study, we demonstrated that rs61552325 (Pro1140Ala) located in ERBB2 is strongly correlated to prostate cancer. Therefore, we initially studied the effect of rs61552325 on androgen-independent prostate cancer cell metastasis.ResultsBioinformatic results demonstrated that the mutant Pro1140Ala likely decrease the stability of the ERBB2 protein and its interactions. The mean migration rate after 6 h for PC3 minor variant cells which carried the G allele was 1.28-fold higher than major variant PC3 cells that carried the C allele (P = 0.016). The mean invasion rate of DU145 putative minor variant cells was 0.40 reducer than negative control cells (P = 5.9E-04).Methodsrs61552325 major variant (C allele) and minor variant (G allele) were produced by site directed mutagenesis and transfected into DU145 and PC3 cells. A wound healing assay was performed to compare migration abilities between alleles. After knocking down endogenous ERBB2 and then expressing the rs61552325 minor variant, invasion abilities were evaluated with a transwell assay using DU145 and PC3 cells.ConclusionsOur data showed that the rs61552325 major variant decreases PC3 cell migration and its minor variant depresses DU145 cell invasion, suggesting that rs61552325 is likely an important change during prostate cancer invasion.

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Effects of functional genetic polymorphisms in theCYP19A1gene on prostate cancer risk and survival

Cited by 33 publications

References 31 publications

An NKX3.1 binding site polymorphism in the l-plastin promoter leads to differential gene expression in human prostate cancer

An NKX3.1 binding site polymorphism in the l-plastin promoter leads to differential gene expression in human prostate cancer

Androgens and androgen receptor signaling in prostate tumorigenesis

Functional analysis implicating the SNP rs61552325 in ERBB2 as an effector for androgen-insensitive prostate cancer cell invasion

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