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LNCaP 图谱:与体内进展为去势抵抗性前列腺癌相关的基因表达。

LNCaP Atlas: gene expression associated with in vivo progression to castration-recurrent prostate cancer.

机构信息

Genome Sciences Centre, British Columbia Cancer Agency, Vancouver, British Columbia, Canada.

出版信息

BMC Med Genomics. 2010 Sep 24;3:43. doi: 10.1186/1755-8794-3-43.

Abstract

BACKGROUND

There is no cure for castration-recurrent prostate cancer (CRPC) and the mechanisms underlying this stage of the disease are unknown.

METHODS

We analyzed the transcriptome of human LNCaP prostate cancer cells as they progress to CRPC in vivo using replicate LongSAGE libraries. We refer to these libraries as the LNCaP atlas and compared these gene expression profiles with current suggested models of CRPC.

RESULTS

Three million tags were sequenced using in vivo samples at various stages of hormonal progression to reveal 96 novel genes differentially expressed in CRPC. Thirty-one genes encode proteins that are either secreted or are located at the plasma membrane, 21 genes changed levels of expression in response to androgen, and 8 genes have enriched expression in the prostate. Expression of 26, 6, 12, and 15 genes have previously been linked to prostate cancer, Gleason grade, progression, and metastasis, respectively. Expression profiles of genes in CRPC support a role for the transcriptional activity of the androgen receptor (CCNH, CUEDC2, FLNA, PSMA7), steroid synthesis and metabolism (DHCR24, DHRS7, ELOVL5, HSD17B4, OPRK1), neuroendocrine (ENO2, MAOA, OPRK1, S100A10, TRPM8), and proliferation (GAS5, GNB2L1, MT-ND3, NKX3-1, PCGEM1, PTGFR, STEAP1, TMEM30A), but neither supported nor discounted a role for cell survival genes.

CONCLUSIONS

The in vivo gene expression atlas for LNCaP was sequenced and support a role for the androgen receptor in CRPC.

摘要

背景

去势抵抗性前列腺癌(CRPC)无法治愈,且该疾病阶段的发病机制尚不清楚。

方法

我们使用复制的 LongSAGE 文库分析了人 LNCaP 前列腺癌细胞在体内向 CRPC 进展过程中的转录组。我们将这些文库称为 LNCaP 图谱,并将这些基因表达谱与目前提出的 CRPC 模型进行比较。

结果

使用体内样本在激素进展的各个阶段对 300 万个标签进行测序,以揭示 96 个在 CRPC 中差异表达的新基因。31 个基因编码的蛋白质要么是分泌蛋白,要么位于质膜上,21 个基因对雄激素的反应改变了表达水平,8 个基因在前列腺中富集表达。26、6、12 和 15 个基因的表达与前列腺癌、Gleason 分级、进展和转移分别相关。CRPC 中基因的表达谱支持雄激素受体(CCNH、CUEDC2、FLNA、PSMA7)、类固醇合成和代谢(DHCR24、DHRS7、ELOVL5、HSD17B4、OPRK1)、神经内分泌(ENO2、MAOA、OPRK1、S100A10、TRPM8)和增殖(GAS5、GNB2L1、MT-ND3、NKX3-1、PCGEM1、PTGFR、STEAP1、TMEM30A)的转录活性,但既不支持也不排除细胞存活基因的作用。

结论

对 LNCaP 的体内基因表达图谱进行了测序,支持雄激素受体在 CRPC 中的作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d5cf/2956710/4b4d4930fa9b/1755-8794-3-43-1.jpg

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