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Tspan8 和 Tspan8/CD151 双基因敲除小鼠中白细胞迁移、血管生成、伤口修复和转移的扭曲表明 Tspan8 和 CD51 具有互补的活性。

Distorted leukocyte migration, angiogenesis, wound repair and metastasis in Tspan8 and Tspan8/CD151 double knockout mice indicate complementary activities of Tspan8 and CD51.

机构信息

Tumor Cell Biology, University Hospital of Surgery, Heidelberg, Germany.

Pancreas Section, University Hospital of Surgery, Heidelberg, Germany.

出版信息

Biochim Biophys Acta Mol Cell Res. 2018 Feb;1865(2):379-391. doi: 10.1016/j.bbamcr.2017.11.007. Epub 2017 Nov 11.

DOI:10.1016/j.bbamcr.2017.11.007
PMID:29138006
Abstract

The tetraspanin Tspan8 supports via associated integrins and proteases tumor progression and angiogenesis. To shed light on its activities in non-transformed cells, we generated a Tspan8 knockout (ko) mouse, comparing leukocyte migration, angiogenesis, wound healing and tumor growth with wild type, CD151ko and Tspan8/CD151ko (dbko) mice. CD151ko mice were included as CD151 activities resemble that of Tspan8, and dbko mice to exclude mutual substitution. Tspan8ko and dbko mice show no pathological phenotype. However, delayed type hypersensitivity reactions are mitigated in Tspan8ko mice, angiogenesis is severely impaired in Tspan8ko, CD151ko and dbko mice, with Tspan8 mostly affecting lymphangiogenesis. Distinct contributions of CD151 and Tspan8 to skin wound healing rely on preferentially CD151 anchoring basal keratinocytes and Tspan8 promoting motility. Proliferation of wounded skin keratinocytes is not affected. Metastasis formation of a melanoma and a Tspan8-expressing pancreatic cancer line was impaired in Tspan8ko and dbko mice, pointing towards a contribution of host Tspan8 to tumor progression. In line with the importance of tetraspanins in exosome-mediated intercellular communication, defects became mitigated by Tspan8/CD151-competent serum exosomes, which offers a most promising therapeutic option for chronic wounds and arteriosclerosis.

摘要

四跨膜蛋白 Tspan8 通过与其相关的整合素和蛋白酶支持肿瘤进展和血管生成。为了阐明其在非转化细胞中的活性,我们生成了 Tspan8 敲除(ko)小鼠,将白细胞迁移、血管生成、伤口愈合和肿瘤生长与野生型、CD151ko 和 Tspan8/CD151ko(dbko)小鼠进行了比较。包括 CD151ko 小鼠是因为 CD151 的活性类似于 Tspan8,而 dbko 小鼠则排除了相互替代。Tspan8ko 和 dbko 小鼠没有表现出病理性表型。然而,Tspan8ko 小鼠的迟发型超敏反应减轻,Tspan8ko、CD151ko 和 dbko 小鼠的血管生成严重受损,Tspan8 主要影响淋巴管生成。CD151 和 Tspan8 对皮肤伤口愈合的不同贡献依赖于 CD151 优先锚定基底层角质形成细胞和 Tspan8 促进迁移。受伤皮肤角质形成细胞的增殖不受影响。黑色素瘤和表达 Tspan8 的胰腺癌系的转移形成在 Tspan8ko 和 dbko 小鼠中受损,这表明宿主 Tspan8 对肿瘤进展有贡献。与四跨膜蛋白在细胞外体介导的细胞间通讯中的重要性一致,Tspan8/CD151 有功能的血清外体减轻了缺陷,这为慢性伤口和动脉硬化提供了最有前途的治疗选择。

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