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神经肽Y的Y(1)介导效应在癌症中的作用:以乳腺癌为靶点

Y(1)-mediated effect of neuropeptide Y in cancer: breast carcinomas as targets.

作者信息

Reubi J C, Gugger M, Waser B, Schaer J C

机构信息

Division of Cell Biology and Experimental Cancer Research, Institute of Pathology, University of Berne, Murtenstrasse 31, CH-3010 Berne, Switzerland.

出版信息

Cancer Res. 2001 Jun 1;61(11):4636-41.

Abstract

Overexpression of selected peptide receptors in human tumors has been shown to represent clinically relevant targets for cancer diagnosis and therapy. Neuropeptide Y (NPY) is a peptide neurotransmitter mediating feeding behavior and vasoconstriction. It has never been shown to be involved in human cancer. We show here, using in vitro receptor autoradiography, a NPY receptor incidence of 85% in primary human breast carcinomas (n = 95) and of 100% in lymph node metastases of receptor-positive primaries (n = 27), predominantly as Y(1) subtype, whereas non-neoplastic human breast expressed Y(2) preferentially. Y(1) mRNA was detected in Y(1)-expressing tumors by in situ hybridization, whereas Y(2) mRNA was found in normal breast tissue. The strong predominance of Y(1) in breast carcinomas compared with Y(2) in normal breast suggests that neoplastic transformation can switch the NPY receptor expression from Y(2) to Y(1) subtype. Moreover, in Y(1)-expressing human SK-N-MC tumor cells, an NPY-induced, dose-dependent inhibition of tumor cell growth of >40% was observed, suggesting a functional role of NPY in cancer, mediated by Y(1). NPY should therefore be added to the list of small regulatory peptides related to cancer. The high incidence of Y(1) in in situ, invasive, and metastatic breast cancers allows for the possibility to target them for diagnosis and therapy with NPY analogues.

摘要

在人类肿瘤中,某些肽受体的过表达已被证明是癌症诊断和治疗的临床相关靶点。神经肽Y(NPY)是一种介导进食行为和血管收缩的肽类神经递质。从未有研究表明它与人类癌症有关。我们在此利用体外受体放射自显影技术显示,原发性人类乳腺癌(n = 95)中NPY受体的发生率为85%,受体阳性原发性肿瘤的淋巴结转移灶(n = 27)中为100%,主要为Y(1)亚型,而非肿瘤性人类乳腺组织则优先表达Y(2)。通过原位杂交在表达Y(1)的肿瘤中检测到Y(1) mRNA,而在正常乳腺组织中发现了Y(2) mRNA。与正常乳腺中的Y(2)相比,乳腺癌中Y(1)的强烈优势表明肿瘤转化可使NPY受体表达从Y(2)亚型转变为Y(1)亚型。此外,在表达Y(1)的人类SK-N-MC肿瘤细胞中,观察到NPY诱导的、剂量依赖性的肿瘤细胞生长抑制>40%,提示NPY在癌症中具有由Y(1)介导的功能作用。因此,NPY应被列入与癌症相关的小调节肽名单中。原位癌、浸润性癌和转移性乳腺癌中Y(1)的高发生率使得有可能用NPY类似物将它们作为诊断和治疗的靶点。

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