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KISS1 过表达抑制异种移植小鼠模型中胰腺腺癌的转移。

KISS1 over-expression suppresses metastasis of pancreatic adenocarcinoma in a xenograft mouse model.

机构信息

Department of Radiation Oncology, University of Alabama at Birmingham, 35294-2182, USA.

出版信息

Clin Exp Metastasis. 2010 Dec;27(8):591-600. doi: 10.1007/s10585-010-9349-5. Epub 2010 Sep 16.

Abstract

Identifying molecular targets for treatment of pancreatic cancer metastasis is critical due to the high frequency of dissemination prior to diagnosis of this lethal disease. Because the KISS1 metastasis suppressor is expressed at reduced levels in advanced pancreatic cancer, we hypothesized that re-expression of KISS1 would reduce metastases. Highly metastatic S2VP10 cells expressing luciferase (S2VP10L) were transfected with a FLAG-tagged version of KISS1 (KFM), KFMΔSS (with deleted secretion signal sequence), or pcDNA3 control plasmid (CP) and expression was confirmed by RTQ-PCR. SCID mice were implanted orthotopically with S2VP10L cells or transfectants and tumor growth and metastases were monitored using bioluminescence imaging. Mice with S2VP10L-KISS1 tumors developed fewer liver (98%) and lung (99%) metastases than S2VP10L. Unexpectedly, mice with S2VP10L-KFMΔSS tumors also had reduced liver and lung metastases, but had more metastases than mice with S2VP10L-KISS. KISS1 protein was found in the cytoplasm of both KFMΔSS and KISS1-expressing orthotopic tumors by immunohistochemistry. Metastases were not found in lungs of mice with S2VP10L-KISS1 tumors; whereas, KFMΔSS lung sections had regions of concentrated KISS1 staining, suggesting that secretion of KISS1 is needed to reduce metastasis significantly. These data suggest induction of KISS1 expression has potential as an adjuvant treatment for pancreatic cancer.

摘要

由于在这种致命疾病诊断之前,播散的发生率很高,因此确定用于治疗胰腺癌转移的分子靶标至关重要。由于 Kiss1 转移抑制因子在晚期胰腺癌中的表达水平降低,我们假设重新表达 Kiss1 将减少转移。高转移性 S2VP10 细胞表达荧光素酶(S2VP10L),用 FLAG 标记的 Kiss1 版本(KFM)、具有缺失的分泌信号序列的 KFMΔSS(KFMΔSS)或 pcDNA3 对照质粒(CP)转染,并通过 RTQ-PCR 确认表达。将 S2VP10L 细胞或转染细胞原位植入 SCID 小鼠中,并使用生物发光成像监测肿瘤生长和转移。与 S2VP10L 相比,携带 S2VP10L-KISS1 肿瘤的小鼠肝脏(98%)和肺部(99%)转移减少。出乎意料的是,携带 S2VP10L-KFMΔSS 肿瘤的小鼠也有减少的肝脏和肺部转移,但比携带 S2VP10L-KISS 的小鼠有更多的转移。免疫组织化学发现,KFMΔSS 和表达 Kiss1 的原位肿瘤的细胞质中都存在 Kiss1 蛋白。在 S2VP10L-KISS1 肿瘤小鼠的肺部未发现转移;然而,KFMΔSS 肺切片有 Kiss1 染色集中的区域,表明 Kiss1 的分泌是显著减少转移所必需的。这些数据表明,诱导 Kiss1 表达具有作为胰腺癌辅助治疗的潜力。

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