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前列腺小细胞神经内分泌癌的分子特征

Molecular characterization of prostatic small-cell neuroendocrine carcinoma.

作者信息

Clegg Nigel, Ferguson Camari, True Lawrence D, Arnold Hugh, Moorman Alec, Quinn Janna E, Vessella Robert L, Nelson Peter S

机构信息

Division of Human Biology, Fred Hutchinson Cancer Research Center, University of Washington-Seattle, 1100 Fairview Avenue North, Seattle, WA 98109-1024, USA.

出版信息

Prostate. 2003 Apr 1;55(1):55-64. doi: 10.1002/pros.10217.

Abstract

OBJECTIVES

A subset of prostate carcinomas is composed predominantly, even exclusively, of neuroendocrine (NE) cells. In this report, we sought to characterize the gene expression profile of a prostate small cell NE carcinoma by assessing the diversity and abundance of transcripts in the LuCaP 49 prostate small cell carcinoma xenograft.

METHODS

We constructed a cDNA library (PRCA3) from the LuCap 49 prostate small cell xenograft. Single pass DNA sequencing of randomly selected cDNA clones followed by sequence assembly and annotation produced a library of Expressed Sequence Tags (ESTs) representing the LuCaP 49 transcriptome. Comparative sequence analysis with ESTs derived from prostate adenocarcinoma libraries was performed using statistical algorithms designed to identify differentially expressed sequences. Putative NE cell-specific genes were further examined by Northern analysis.

RESULTS

Sequence assembly and analysis identified 1,447 distinct genes expressed in the LuCaP 49 cDNA library. These include cDNAs encoding the NE markers secretogranin (SCG2), CD24, and ENO2. Northern analysis revealed that three additional genes, ASCL1, INA, and SV2B are expressed in LuCaP 49 but not in various prostate cancer cell lines or xenografts. Fifteen genes were identified with a statistical probability (P > 0.9) of being up-regulated in LuCaP 49 small cell carcinoma relative to prostate adenocarcinoma (two primary prostate adenocarcinomas and the LNCaP prostate adenocarcinoma cell line).

CONCLUSIONS

Prostate small cell carcinoma expresses a diverse repertoire of genes that reflect characteristics of their NE cell of origin. ASCL1, INA, and SV2B are potential molecular markers for small cell NE tumors and NE cells of the prostate. This small cell NE carcinoma gene expression profile may yield insights into the development, progression, and treatment of subtypes of prostate cancer.

摘要

目的

一部分前列腺癌主要甚至完全由神经内分泌(NE)细胞构成。在本报告中,我们试图通过评估LuCaP 49前列腺小细胞癌异种移植瘤中转录本的多样性和丰度,来描绘前列腺小细胞神经内分泌癌的基因表达谱。

方法

我们从LuCap 49前列腺小细胞异种移植瘤构建了一个cDNA文库(PRCA3)。对随机选择的cDNA克隆进行单通道DNA测序,随后进行序列组装和注释,生成了一个代表LuCaP 49转录组的表达序列标签(EST)文库。使用旨在识别差异表达序列的统计算法,对来自前列腺腺癌文库的EST进行比较序列分析。通过Northern分析进一步检测推定的NE细胞特异性基因。

结果

序列组装和分析确定了在LuCaP 49 cDNA文库中表达的1447个不同基因。这些基因包括编码NE标志物分泌粒蛋白(SCG2)、CD24和烯醇化酶2(ENO2)的cDNA。Northern分析显示,另外三个基因,即无翅型MMTV整合位点家族成员1(ASCL1)、肌动蛋白结合蛋白(INA)和突触囊泡蛋白2B(SV2B)在LuCaP 49中表达,但在各种前列腺癌细胞系或异种移植瘤中不表达。相对于前列腺腺癌(两个原发性前列腺腺癌和LNCaP前列腺腺癌细胞系),在LuCaP 49小细胞癌中有15个基因被鉴定为上调,其统计学概率(P>0.9)。

结论

前列腺小细胞癌表达多种基因,反映了其起源的NE细胞的特征。ASCL1、INA和SV2B是前列腺小细胞NE肿瘤和NE细胞的潜在分子标志物。这种小细胞NE癌基因表达谱可能有助于深入了解前列腺癌亚型的发生、发展和治疗。

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