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催产素诱导前列腺癌细胞迁移:涉及 Gi 偶联信号通路。

Oxytocin induces the migration of prostate cancer cells: involvement of the Gi-coupled signaling pathway.

机构信息

Center for Cancer Research and Therapeutic Development, Clark Atlanta University, Atlanta, GA 30314, USA.

出版信息

Mol Cancer Res. 2010 Aug;8(8):1164-72. doi: 10.1158/1541-7786.MCR-09-0329. Epub 2010 Jul 27.

Abstract

Expression of genes that encode oxytocin (OXT) and vasopressin (AVP) and their cognate receptors in normal and diseased prostates are only partially characterized. Reverse transcription and PCR were used to examine the expression of these genes in normal prostate epithelial and stromal cell lines, k-ras-transformed prostate epithelial cell lines, and in four prostate cancer cell lines. Secreted and cell-associated OXT peptide was measured by an enzyme immunoassay. OXT and its receptor (OXTR) were expressed in all eight prostate cell lines. Cell-associated OXT peptide was also found in all prostate epithelial cell lines except in DU145 cells. Neither AVP nor its cognate receptors (V1a receptor and V2 receptor) were expressed in any prostate cell line examined. These data point to the OXTR as the primary target of OXT and AVP, and suggest that OXT might be an autocrine/paracrine regulator in human prostate. We found that OXT induces the migration of PC3 and PC3M, but not DU145 prostate cancer cells. The effect of OXT is distinct from the epidermal growth factor (EGF)-induced migration of prostate cancer cells, in which ERK1/2 and EGF receptor kinase activities were required. When cells were pretreated with pertussis toxin, the effect of OXT, but not EGF, on cell migration was abolished. Pretreatment with the cyclic AMP analogue, 8-Br-cAMP, did not affect OXT-induced cell migration, which eliminated the nonspecific effect of pertussis toxin. We conclude that a Gi-dependent mechanism is involved in OXTR-mediated migration of prostate cancer cells, and indicates a role for OXTR in prostate cancer metastasis.

摘要

在正常和患病的前列腺中,编码催产素(OXT)和血管加压素(AVP)及其同源受体的基因的表达仅部分得到了描述。使用逆转录和 PCR 来检查这些基因在正常前列腺上皮和基质细胞系、k-ras 转化的前列腺上皮细胞系以及四种前列腺癌细胞系中的表达。通过酶免疫测定法测量分泌的和细胞相关的 OXT 肽。OXT 和其受体(OXTR)在所有八种前列腺细胞系中均有表达。细胞相关的 OXT 肽也存在于除 DU145 细胞之外的所有前列腺上皮细胞系中。在研究的任何前列腺细胞系中均未表达 AVP 或其同源受体(V1a 受体和 V2 受体)。这些数据表明 OXTR 是 OXT 和 AVP 的主要靶标,并提示 OXT 可能是人类前列腺中的自分泌/旁分泌调节剂。我们发现 OXT 诱导 PC3 和 PC3M 但不诱导 DU145 前列腺癌细胞的迁移。OXT 的作用与前列腺癌细胞的表皮生长因子(EGF)诱导的迁移不同,在这种迁移中需要 ERK1/2 和 EGF 受体激酶活性。当细胞用百日咳毒素预处理时,OXT 但不是 EGF 对细胞迁移的作用被消除。用环 AMP 类似物 8-Br-cAMP 预处理不会影响 OXT 诱导的细胞迁移,从而消除了百日咳毒素的非特异性作用。我们得出结论,Gi 依赖性机制参与了 OXTR 介导的前列腺癌细胞迁移,并表明 OXTR 在前列腺癌转移中起作用。

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