快速化疗诱导的急性内皮祖细胞动员:抗血管生成药物作为化疗增敏剂的意义。
Rapid chemotherapy-induced acute endothelial progenitor cell mobilization: implications for antiangiogenic drugs as chemosensitizing agents.
作者信息
Shaked Yuval, Henke Erik, Roodhart Jeanine M L, Mancuso Patrizia, Langenberg Marlies H G, Colleoni Marco, Daenen Laura G, Man Shan, Xu Ping, Emmenegger Urban, Tang Terence, Zhu Zhenping, Witte Larry, Strieter Robert M, Bertolini Francesco, Voest Emile E, Benezra Robert, Kerbel Robert S
机构信息
Molecular and Cellular Biology, Sunnybrook Health Sciences Centre, University of Toronto, Toronto, ON M4N 3M5, Canada.
出版信息
Cancer Cell. 2008 Sep 9;14(3):263-73. doi: 10.1016/j.ccr.2008.08.001.
Abstract
Several hypotheses have been proposed to explain how antiangiogenic drugs enhance the treatment efficacy of cytotoxic chemotherapy, including impairing the ability of chemotherapy-responsive tumors to regrow after therapy. With respect to the latter, we show that certain chemotherapy drugs, e.g., paclitaxel, can rapidly induce proangiogenic bone marrow-derived circulating endothelial progenitor (CEP) mobilization and subsequent tumor homing, whereas others, e.g., gemcitabine, do not. Acute CEP mobilization was mediated, at least in part, by systemic induction of SDF-1alpha and could be prevented by various procedures such as treatment with anti-VEGFR2 blocking antibodies or paclitaxel treatment in CEP-deficient Id mutant mice, both of which resulted in enhanced antitumor effects mediated by paclitaxel, but not by gemcitabine.
摘要
已经提出了几种假说来解释抗血管生成药物如何提高细胞毒性化疗的治疗效果,包括损害化疗反应性肿瘤在治疗后重新生长的能力。关于后者,我们发现某些化疗药物,如紫杉醇,可迅速诱导骨髓来源的促血管生成循环内皮祖细胞(CEP)动员及随后的肿瘤归巢,而其他药物,如吉西他滨,则不会。急性CEP动员至少部分是由SDF-1α的全身诱导介导的,并且可以通过各种方法预防,例如用抗VEGFR2阻断抗体治疗或在CEP缺陷的Id突变小鼠中进行紫杉醇治疗,这两种方法均导致紫杉醇介导的抗肿瘤作用增强,但吉西他滨则不然。
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本文引用的文献
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Tumor angiogenesis.肿瘤血管生成
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Multiple circulating proangiogenic factors induced by sunitinib malate are tumor-independent and correlate with antitumor efficacy.苹果酸舒尼替尼诱导的多种循环促血管生成因子与肿瘤无关,并与抗肿瘤疗效相关。
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Tumor refractoriness to anti-VEGF treatment is mediated by CD11b+Gr1+ myeloid cells.肿瘤对抗VEGF治疗的难治性是由CD11b+Gr1+髓样细胞介导的。
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