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揭开内皮抑素的奥秘。

Unraveling the mysteries of endostatin.

作者信息

Fu Yan, Tang Huadong, Huang Yujie, Song Nan, Luo Yongzhang

机构信息

National Engineering Laboratory for Anti-tumor Protein Therapeutics, Tsinghua University, Beijing, People's Republic of China.

出版信息

IUBMB Life. 2009 Jun;61(6):613-26. doi: 10.1002/iub.215.

DOI:10.1002/iub.215
PMID:19472178
Abstract

Endostatin, a 20-kDa C-terminal proteolytic fragment of collagen XVIII, is a specific endogenous angiogenesis inhibitor discovered more than a decade. The structure, stability, and mechanism of actions of endostatin have been extensively investigated during the past 12 years, among which controversial reports remain unclarified. The mysteries include the following: 1) Why controversial efficacies were observed with endostatin regarding tumor inhibition? Particularly, why does an N-terminal modified endostatin show good clinical responses in China, whereas the clinical trials of the wild type endostatin were terminated at the early stage of phase II in the USA? 2) What is the contribution of zinc-binding to the stability and biological functions of endostatin? 3) Why does insoluble endostatin shrink tumors? 4) How to ensure that endostatin is correctly refolded? 5) How does endostatin exert its biological functions? Recent progress regarding the biophysical properties, biological functions, signaling pathways, and clinical trials of endostatin are reviewed here. Surprising findings show that the integrity of the N-terminal sequence, the capability of zinc-binding, and the correct folding are three essential elements for assurance of structural stability and biological functions of endostatin. This review provides clues to understand the mysteries of endostatin and its derivatives.

摘要

内皮抑素是胶原蛋白 XVIII 的一种 20 千道尔顿的 C 末端蛋白水解片段,是十多年前发现的一种特异性内源性血管生成抑制剂。在过去 12 年中,人们对内皮抑素的结构、稳定性及作用机制进行了广泛研究,其中仍有一些有争议的报道尚未阐明。这些谜团包括:1)为何在肿瘤抑制方面内皮抑素观察到有争议的疗效?特别是,为什么 N 末端修饰的内皮抑素在中国显示出良好的临床反应,而野生型内皮抑素在美国的 II 期临床试验早期就终止了?2)锌结合对内皮抑素的稳定性和生物学功能有何贡献?3)为什么不溶性内皮抑素能使肿瘤缩小?4)如何确保内皮抑素正确复性?5)内皮抑素如何发挥其生物学功能?本文综述了内皮抑素在生物物理性质、生物学功能、信号通路及临床试验方面的最新进展。令人惊讶的发现表明,N 末端序列的完整性、锌结合能力和正确折叠是保证内皮抑素结构稳定性和生物学功能的三个关键要素。本综述为理解内皮抑素及其衍生物的奥秘提供了线索。

相似文献

1
Unraveling the mysteries of endostatin.揭开内皮抑素的奥秘。
IUBMB Life. 2009 Jun;61(6):613-26. doi: 10.1002/iub.215.
2
The N-terminal integrity is critical for the stability and biological functions of endostatin.N 端完整性对于内皮抑素的稳定性和生物学功能至关重要。
Biochemistry. 2010 Aug 3;49(30):6420-9. doi: 10.1021/bi100489x.
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Structural analysis of the N-terminal fragment of the antiangiogenic protein endostatin: a molecular dynamics study.抗血管生成蛋白内皮抑素 N 端片段的结构分析:分子动力学研究。
Proteins. 2011 Sep;79(9):2684-92. doi: 10.1002/prot.23096. Epub 2011 Jul 18.
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Generation of biologically active endostatin fragments from human collagen XVIII by distinct matrix metalloproteases.不同的基质金属蛋白酶从人胶原蛋白XVIII生成具有生物活性的内皮抑素片段。
Exp Cell Res. 2005 Jul 15;307(2):292-304. doi: 10.1016/j.yexcr.2005.03.021.
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Contributions of Zn(II)-binding to the structural stability of endostatin.锌(II)结合对内抑素结构稳定性的贡献。
FEBS Lett. 2007 Jun 26;581(16):3027-32. doi: 10.1016/j.febslet.2007.05.058. Epub 2007 May 29.
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N-terminal fragment of the anti-angiogenic human endostatin binds copper(II) with very high affinity.抗血管生成人内皮抑素的N端片段以极高的亲和力结合铜(II)。
J Inorg Biochem. 2009 Jul;103(7):940-7. doi: 10.1016/j.jinorgbio.2009.04.006. Epub 2009 Apr 23.
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Determination of the disulfide bond pattern of the endogenous and recombinant angiogenesis inhibitor endostatin by mass spectrometry.通过质谱法测定内源性和重组血管生成抑制剂内皮抑素的二硫键模式。
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Binding of endostatin to phosphatidylserine-containing membranes and formation of amyloid-like fibers.内皮抑素与含磷脂酰丝氨酸的膜结合及淀粉样纤维的形成。
Biochemistry. 2005 Mar 1;44(8):2857-63. doi: 10.1021/bi048510j.
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Antiangiogenesis in cancer therapy--endostatin and its mechanisms of action.癌症治疗中的抗血管生成——内皮抑素及其作用机制。
Exp Cell Res. 2006 Mar 10;312(5):594-607. doi: 10.1016/j.yexcr.2005.11.015. Epub 2005 Dec 22.
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Endostatin signaling and regulation of endothelial cell-matrix interactions.内皮抑素信号传导与内皮细胞-基质相互作用的调节
Adv Cancer Res. 2005;94:197-229. doi: 10.1016/S0065-230X(05)94005-0.

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