内源性胃间充质干细胞参与胃癌间质形成和进展。

Korean Journal of Pathology Pub Date : 2013-12-01 Epub Date: 2013-12-24 DOI:10.4132/KoreanJPathol.2013.47.6.507
Eun-Kyung Kim, Hye-Jung Kim, Young-Il Yang, Jong Tae Kim, Min-Young Choi, Chang Soo Choi, Kwang-Hee Kim, Jeong-Han Lee, Won-Hee Jang, Soon-Ho Cheong
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引用次数: 12

摘要

背景:癌相关成纤维细胞(CAFs)参与癌变和癌症进展,尽管其起源和作用尚不清楚。我们最近发现并研究了胃粘膜下间充质干细胞(GS-MSCs)在胃癌发生过程中的原位鉴定及其意义。方法:采用水凝胶支持的器官培养方法从胃粘膜下层分离GS-MSCs,并对其进行鉴定。通过免疫表型和间生多能性对分离细胞进行体外评价。研究了GS-MSCs与胃癌细胞之间的相互作用。为了确定GS-MSCs的作用,我们将胃癌细胞混合或不混合GS-MSCs构建异种移植物。结果:分离的细胞在可塑性粘附、基质细胞免疫表型和多能性方面满足MSCs的要求。我们证明了一个旁分泌环,胃癌细胞增强了GS-MSCs的迁移、增殖和分化;此外,GS-MSCs还能促进胃癌细胞的体外增殖。异种移植实验表明,GS-MSCs显著促进肿瘤生长和血管生成。整合到胃癌中的GS-MSCs不仅成为caf,而且很少成为内皮细胞,内皮细胞有助于细胞和血管癌基质的形成。结论:内源性GS-MSCs在胃癌进展中起重要作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Endogenous gastric-resident mesenchymal stem cells contribute to formation of cancer stroma and progression of gastric cancer.

Endogenous gastric-resident mesenchymal stem cells contribute to formation of cancer stroma and progression of gastric cancer.

Endogenous gastric-resident mesenchymal stem cells contribute to formation of cancer stroma and progression of gastric cancer.

Endogenous gastric-resident mesenchymal stem cells contribute to formation of cancer stroma and progression of gastric cancer.

Background: Carcinoma-associated fibroblasts (CAFs) contribute to carcinogenesis and cancer progression, although their origin and role remain unclear. We recently identified and investigated the in situ identity and implications of gastric submucosa-resident mesenchymal stem cells (GS-MSCs) in the progression of gastric carcinogenesis.

Methods: We isolated GS-MSCs from gastric submucosa using hydrogel-supported organ culture and defined their identity. Isolated cells were assessed in vitro by immunophenotype and mesengenic multipotency. Reciprocal interactions between GS-MSCs and gastric cancer cells were evaluated. To determine the role of GS-MSCs, xenografts were constructed of gastric cancer cells admixed with or without GS-MSCs.

Results: Isolated cells fulfilled MSCs requirements in regard to plastic adherence, stromal cell immunophenotype, and multipotency. We demonstrated a paracrine loop that gastric cancer cells enhanced the migration, proliferation, and differentiation of GS-MSCs; additionally, GS-MSCs promoted the proliferation of gastric cancer cell in vitro. Xenograft experiments showed that GS-MSCs significantly promoted cancer growth and angiogenesis. GS-MSCs that integrated into gastric cancer became not only CAFs but also rarely endothelial cells which contributed to the formation of cellular and vascular cancer stroma.

Conclusions: Endogenous GS-MSCs play an important role in gastric cancer progression.

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来源期刊
Korean Journal of Pathology
Korean Journal of Pathology 医学-病理学
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