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TRPV6 等位基因不会影响前列腺癌的进展。

TRPV6 alleles do not influence prostate cancer progression.

机构信息

Institut für Experimentelle und Klinische Pharmakologie und Toxikologie, Universität des Saarlandes, Homburg/Saar, Germany.

出版信息

BMC Cancer. 2009 Oct 26;9:380. doi: 10.1186/1471-2407-9-380.

Abstract

BACKGROUND

The transient receptor potential, subfamily V, member 6 (TRPV6) is a Ca(2+) selective cation channel. Several studies have shown that TRPV6 transcripts are expressed in locally advanced prostatic adenocarcinoma, metastatic and androgen-insensitive prostatic lesions but are undetectable in healthy prostate tissue and benign prostatic hyperplasia. Two allelic variants of the human trpv6 gene have been identified which are transcribed into two independent mRNAs, TRPV6a and TRPV6b. We now asked, whether the trpv6a allele is correlated with the onset of prostate cancer, with the Gleason score and the tumour stage.

METHODS

Genomic DNA of prostate cancer patients and control individuals was isolated from resections of prostatic adenocarcinomas and salivary fluid respectively. Genotyping of SNPs of the TRPV6 gene was performed by restriction length polymorphism or by sequencing analysis. RNA used for RT-PCR was isolated from prostate tissue. Data sets were analyzed by Chi-Square test.

RESULTS

We first characterized in detail the five polymorphisms present in the protein coding exons of the trpv6 gene and show that these polymorphisms are coupled and are underlying the TRPV6a and the TRPV6b variants. Next we analysed the frequencies of the two TRPV6 alleles using genomic DNA from saliva samples of 169 healthy individuals. The homozygous TRPV6b genotype predominated with 86%, whereas no homozygous TRPV6a carriers could be identified. The International HapMap Project identified a similar frequency for an Utah based population whereas in an African population the a-genotype prevailed. The incidence of prostate cancer is several times higher in African populations than in non-African and we then investigated the TRPV6a/b frequencies in 141 samples of prostatic adenocarcinoma. The TRPV6b allele was found in 87% of the samples without correlation with Gleason score and tumour stage.

CONCLUSION

Our results show that the frequencies of trpv6 alleles in healthy control individuals and prostate cancer patients are not significantly different. Although expression of trpv6 transcripts correlates with aggressive potential of prostate cancer, the TRPV6 genotype does not correlate with the onset of prostate cancer, with the Gleason score and the tumour stage.

摘要

背景

瞬时受体电位通道,亚家族 V,成员 6(TRPV6)是一种钙离子选择性阳离子通道。几项研究表明,TRPV6 转录本在局部晚期前列腺腺癌、转移性和雄激素不敏感的前列腺病变中表达,但在健康前列腺组织和良性前列腺增生中无法检测到。已经鉴定出人类 trpv6 基因的两个等位基因变体,它们转录成两个独立的 mRNA,TRPV6a 和 TRPV6b。我们现在想知道 trpv6a 等位基因是否与前列腺癌的发生、Gleason 评分和肿瘤分期有关。

方法

分别从前列腺腺癌切除术和唾液中分离前列腺癌患者和对照个体的基因组 DNA。通过限制性长度多态性或测序分析对 TRPV6 基因的 SNP 进行基因分型。用于 RT-PCR 的 RNA 从前列腺组织中分离。通过卡方检验分析数据集。

结果

我们首先详细描述了 TRPV6 基因蛋白编码外显子中存在的五个多态性,并表明这些多态性是相互关联的,是 TRPV6a 和 TRPV6b 变体的基础。接下来,我们使用来自 169 名健康个体唾液样本的基因组 DNA 分析了两个 TRPV6 等位基因的频率。纯合 TRPV6b 基因型占主导地位,为 86%,而没有鉴定到纯合 TRPV6a 携带者。国际人类基因组单体型计划(International HapMap Project)确定了一个基于犹他州的人群的类似频率,而在非洲人群中,a 基因型占优势。非洲人群的前列腺癌发病率是非洲以外人群的数倍,我们随后在 141 个前列腺腺癌样本中研究了 TRPV6a/b 的频率。TRPV6b 等位基因在 87%的样本中发现,与 Gleason 评分和肿瘤分期无关。

结论

我们的结果表明,健康对照个体和前列腺癌患者的 trpv6 等位基因频率没有显著差异。尽管 trpv6 转录本的表达与前列腺癌的侵袭性潜力相关,但 TRPV6 基因型与前列腺癌的发生、Gleason 评分和肿瘤分期无关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b113/2774862/e20bf2d12eb9/1471-2407-9-380-1.jpg

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