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胃泌素释放肽受体(GRPR)的免疫组化分析及其在人前列腺癌中雌激素受体βcx 的可能调节作用。

Immunohistochemical analysis of gastrin-releasing peptide receptor (GRPR) and possible regulation by estrogen receptor βcx in human prostate carcinoma.

机构信息

Department of Pathology, Tohoku University Graduate School of Medicine, Sendai, Japan.

出版信息

Neoplasma. 2012;59(2):224-32. doi: 10.4149/neo_2012_029.

DOI:10.4149/neo_2012_029
PMID:22248281
Abstract

Gastrin-releasing peptide (GRP) belongs to the family of bombesin-like peptides. GRP was demonstrated to stimulate the proliferation and invasiveness of androgen-independent prostate carcinoma. GRP mediates its action through the membrane-bound receptor, GRP receptor (GRPR), which is characterized by a high-affinity binding for both GRP and bombesin. In human prostate cancer tissue, GRPR mRNA was reported to be detectable in more than 90% but its immunolocalizaition has not been reported. Therefore, in this study we immunolocalized GRPR in 51 human prostate cancer cases and correlated the findings with several clinicopathological parameters in order to better understand the function and regulation of GRPR in human prostate cancer. GRPR was immnolocalized in carcinoma cells and their values were significantly associated with Gleason score and immunoreactivity of estrogen receptor βcx (ERβcx) that is one of splicing variants of ligand dependent transcription factor, ERβ, and considered to be prognostic factor of prostate cancer patients. The amounts of GRPR and ERβcx mRNA in three prostate cancer cell lines PC-3, DU-145 and LNCaP evaluated by quantitative RT-PCR (qPCR) analysis were also significantly correlated. In addition, we established stable transformants of prostate carcinoma cell line PC-3 introduced with ERβcx, and confirmed that GRPR mRNA was induced in ERβcx over-expressing PC-3 cells by qPCR analysis. These results also suggest that ERβcx contributes to prostate cancer development possibly through mediating GRPR expression in carcinoma cells.

摘要

胃泌素释放肽(GRP)属于铃蟾肽样肽家族。已经证明 GRP 可刺激雄激素非依赖性前列腺癌的增殖和侵袭性。GRP 通过其膜结合受体,GRP 受体(GRPR)发挥作用,GRPR 对 GRP 和铃蟾肽均具有高亲和力。在人类前列腺癌组织中,已报道 GRPR mRNA 在超过 90%的病例中可检测到,但尚未报道其免疫定位。因此,在这项研究中,我们在 51 例人类前列腺癌病例中免疫定位了 GRPR,并将发现与几种临床病理参数相关联,以便更好地了解 GRPR 在人类前列腺癌中的功能和调节。GRPR 免疫定位于癌细胞中,其值与 Gleason 评分和雌激素受体 βcx(ERβcx)的免疫反应性显著相关,ERβcx 是配体依赖性转录因子 ERβ 的剪接变体之一,被认为是前列腺癌患者的预后因素。通过定量 RT-PCR(qPCR)分析评估的三种前列腺癌细胞系 PC-3、DU-145 和 LNCaP 中的 GRPR 和 ERβcx mRNA 含量也呈显著相关性。此外,我们建立了前列腺癌细胞系 PC-3 的稳定转化体,引入了 ERβcx,并通过 qPCR 分析证实了 ERβcx 过表达 PC-3 细胞中 GRPR mRNA 的诱导。这些结果还表明,ERβcx 可能通过介导癌细胞中 GRPR 的表达而促进前列腺癌的发展。

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