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前列腺内分泌-旁分泌(神经内分泌)调节系统与前列腺癌中的神经内分泌分化:综述及基础研究的未来方向

The prostatic endocrine-paracrine (neuroendocrine) regulatory system and neuroendocrine differentiation in prostatic carcinoma: a review and future directions in basic research.

作者信息

Di Sant'Agnese P A, Cockett A T

机构信息

Department of Pathology and Laboratory Medicine, University of Rochester Medical Center, New York 14642.

出版信息

J Urol. 1994 Nov;152(5 Pt 2):1927-31. doi: 10.1016/s0022-5347(17)32417-5.

Abstract

Endocrine-paracrine (neuroendocrine, amine precursor uptake and decarboxylation [APUD]) cells of the prostato-urethral region are serotonin and peptide containing regulatory cells, which are part of a dispersed neuroendocrine regulatory system also known as the APUD system. These cells most likely regulate growth and differentiation, as well as the secretory functions of the prostate. Prostatic carcinoma exhibits neuroendocrine differentiation in 3 forms: 1) small cell neuroendocrine carcinoma, 2) carcinoid-like tumors and 3) conventional prostatic adenocarcinoma with focal neuroendocrine differentiation. Small cell carcinoma and carcinoid-like tumors are rather rare (1 to 2% of all prostatic malignancies) and generally pursue an aggressive course. Focal neuroendocrine differentiation in adenocarcinoma is extensive in 10% of the cases and may be present in virtually all adenocarcinomas to a minor degree. There are conflicting studies on the prognostic significance of focal neuroendocrine differentiation in prostatic carcinoma, although several suggest a poor prognosis. The finding that serum neuroendocrine markers predict initial insensitivity to or the development of resistance to hormonal suppression therapy, coupled with the recent observation that androgen receptor is not expressed in neoplastic neuroendocrine cells suggests that neuroendocrine differentiation directly results in resistance to hormonal manipulation therapy. Neuroendocrine differentiation in prostatic carcinoma raises the possibility of innovative modes of treatment. Future directions of research should concentrate on the quantitative analysis of serotonin and various peptides in prostatic malignancy, since high levels of constitutive secretion may not be appreciated by immunocytochemistry, as well as analysis of tumors for receptors to neuroendocrine products, which are necessary for these products to have a functional role. Finally, specific subtypes of neoplastic cells with neuroendocrine differentiation based on serotonin and peptide profiles should be analyzed.

摘要

前列腺尿道区域的内分泌旁分泌(神经内分泌、胺前体摄取及脱羧[APUD])细胞是含5-羟色胺和肽的调节细胞,它们是分散的神经内分泌调节系统(也称为APUD系统)的一部分。这些细胞很可能调节前列腺的生长、分化以及分泌功能。前列腺癌呈现3种神经内分泌分化形式:1)小细胞神经内分泌癌,2)类癌样肿瘤,3)具有局灶性神经内分泌分化的传统前列腺腺癌。小细胞癌和类癌样肿瘤相当罕见(占所有前列腺恶性肿瘤的1%至2%),且通常病程进展迅速。腺癌中的局灶性神经内分泌分化在10%的病例中很广泛,实际上在所有腺癌中都可能有轻微程度的存在。关于前列腺癌局灶性神经内分泌分化的预后意义存在相互矛盾的研究,不过有几项研究提示预后不良。血清神经内分泌标志物可预测对激素抑制治疗初始无反应或产生耐药性这一发现,再加上最近观察到肿瘤性神经内分泌细胞中不表达雄激素受体,提示神经内分泌分化直接导致对激素操纵治疗产生耐药性。前列腺癌中的神经内分泌分化增加了创新治疗模式的可能性。未来的研究方向应集中于对前列腺恶性肿瘤中5-羟色胺和各种肽进行定量分析,因为免疫细胞化学可能无法检测到高水平的组成性分泌,同时还要分析肿瘤中神经内分泌产物的受体,这些产物发挥功能作用需要这些受体。最后,应分析基于5-羟色胺和肽谱的具有神经内分泌分化的肿瘤细胞的特定亚型。

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