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血小板反应蛋白-1在转基因小鼠中选择性抑制早期致癌作用和血管生成,但不抑制肿瘤淋巴管生成和淋巴转移。

Thrombospondin-1 selectively inhibits early-stage carcinogenesis and angiogenesis but not tumor lymphangiogenesis and lymphatic metastasis in transgenic mice.

作者信息

Hawighorst Thomas, Oura Hajimu, Streit Michael, Janes Lauren, Nguyen Lynh, Brown Lawrence F, Oliver Guillermo, Jackson David G, Detmar Michael

机构信息

Cutaneous Biology Research Center and Department of Dermatology, Massachusetts General Hospital and Harvard Medical School, Charlestown 02129, USA.

出版信息

Oncogene. 2002 Nov 14;21(52):7945-56. doi: 10.1038/sj.onc.1205956.

Abstract

The roles played by the endogenous angiogenesis inhibitor thrombospondin-1 (TSP-1) in the early stages of multi-step carcinogenesis and in the control of hematogenous versus lymphatic metastasis are unknown. To investigate these issues we compared tumor development in normal mice and in transgenic mice with targeted overexpression of TSP-1 in the epidermis following a standard two-step chemical skin carcinogenesis regimen. Overexpression of TSP-1 resulted in delayed and reduced development of premalignant epithelial hyperplasias, but did not inhibit the malignant conversion to squamous cell carcinomas. TSP-1 overexpression also suppressed tumor angiogenesis and distant organ metastasis, but failed to inhibit tumor-associated lymphangiogenesis or lymphatic tumor spread to regional lymph nodes. Concomitant with these results, we found that the endothelial TSP-1 receptor CD36 was mostly absent from cutaneous lymphatic vessels. Our findings indicate the potential use of TSP-1 for the prevention of premalignant stages of tumorigenesis and are likely to have implications for the further development of anti-angiogenic cancer therapies.

摘要

内源性血管生成抑制剂血小板反应蛋白-1(TSP-1)在多步骤致癌作用早期以及在控制血行转移与淋巴转移方面所起的作用尚不清楚。为了研究这些问题,我们在标准的两步化学皮肤致癌方案后,比较了正常小鼠和表皮靶向过表达TSP-1的转基因小鼠中的肿瘤发展情况。TSP-1的过表达导致癌前上皮增生的发展延迟且程度减轻,但并未抑制向鳞状细胞癌的恶性转化。TSP-1的过表达还抑制了肿瘤血管生成和远处器官转移,但未能抑制肿瘤相关的淋巴管生成或肿瘤向区域淋巴结的淋巴转移。与这些结果一致,我们发现内皮TSP-1受体CD36在皮肤淋巴管中大多不存在。我们的研究结果表明TSP-1在预防肿瘤发生的癌前阶段具有潜在用途,并且可能对抗血管生成癌症治疗的进一步发展产生影响。

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