Proteolytic exposure of a cryptic site within collagen type IV is required for angiogenesis and tumor growth in vivo

Jingsong Xu; Dorothy Rodriguez; Eric Petitclerc; Jenny J. Kim; Masanori Hangai; S. Moon Yuen; George E. Davis; Peter C. Brooks

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Proteolytic exposure of a cryptic site within collagen type IV is required for angiogenesis and tumor growth in vivo

机译：体内血管生成和肿瘤生长需要蛋白水解性暴露IV型胶原内的隐性位点

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Evidence is provided that proteolytic cleavage of collagen type IV results in the exposure of a functionally important cryptic site hidden within its triple helical structure. Exposure of this cryptic site was associated with angiogenic, but not quiescent, blood vessels and was required for angiogenesis in vivo. Exposure of the HUIV26 epitope was associated with a loss of α1β1 integrin binding and the gain of αvβ3 binding. A monoclonal antibody (HUIV26) directed to this site disrupts integrin-dependent endothelial cell interactions and potently inhibits angiogenesis and tumor growth. Together, these studies suggest a novel mechanism by which proteolysis contributes to angiogenesis by exposing hidden regulatory elements within matrix-immobilized collagen type IV.

机译：提供的证据表明，IV型胶原蛋白的蛋白水解裂解导致隐藏在其三重螺旋结构内的功能重要的隐秘位点暴露。该隐蔽位点的暴露与血管生成有关，但与静态血管无关，并且是体内血管生成所必需的。 HUIV26表位的暴露与α1β1整联蛋白结合的丧失和αvβ3结合的获得有关。针对该位点的单克隆抗体（HUIV26）破坏整合素依赖性内皮细胞相互作用，并有效抑制血管生成和肿瘤生长。总之，这些研究提出了一种新的机制，通过这种机制，蛋白水解作用通过暴露固定在基质固定的IV型胶原蛋白中的隐藏调节因子来促进血管生成。

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《Journal of cell biology》 |2001年第5期|共11页
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Jingsong Xu; Dorothy Rodriguez; Eric Petitclerc; Jenny J. Kim; Masanori Hangai; S. Moon Yuen; George E. Davis; Peter C. Brooks;
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1. Ionizing radiation modulates the exposure of the HUIV26 cryptic epitope within collagen type IV during angiogenesis. [J] . Brooks PC, Roth JM, Lymberis SC, International Journal of Radiation Oncology, Biology, Physics . 2002,第4期

机译：电离辐射调节血管生成过程中IV型胶原中HUIV26隐性表位的暴露。
2. Type IV collagen alpha6 chain-derived noncollagenous domain 1 (alpha6(IV)NC1) inhibits angiogenesis and tumor growth. [J] . Mundel TM, Yliniemi AM, Maeshima Y, International Journal of Cancer =: Journal International du Cancer . 2008,第8期

机译：IV型胶原蛋白alpha6链衍生的非胶原结构域1（alpha6（IV）NC1）抑制血管生成和肿瘤生长。
3. Modulation of collagen gene expression by cytokines: stimulatory effect of transforming growth factor-beta1, with divergent effects of epidermal growth factor and tumor necrosis factor-alpha on collagen type I and collagen type IV. [J] . Grande JP, Melder DC, Zinsmeister AR The Journal of laboratory and clinical medicine . 1997,第5期

机译：细胞因子对胶原蛋白基因表达的调节：转化生长因子-β1的刺激作用，表皮生长因子和肿瘤坏死因子-α对I型和IV型胶原的发散作用。
4. Human urine-derived stem cells expressing vascular endothelial growth factor within collagen type Ⅰ gels promote muscle and nerve regeneration in vivo [C] . Guihua Liu, Shaofeng Wu, Shantaram Bharadwaj, World biomaterials congress . 2012

机译：Ⅰ型胶原凝胶中表达血管内皮生长因子的人尿干细胞在体内促进肌肉和神经再生
5. Regulation of angiogenesis and tumor growth by the pro-inflammatory cryptic RGDKGE containing collagen epitope. [D] . Ames, Jacquelyn Joan. 2015

机译：通过含有胶原蛋白抗原决定簇的促炎性隐秘RGDKGE调节血管生成和肿瘤生长。
6. Proteolytic exposure of a cryptic site within collagen type IV is required for angiogenesis and tumor growth in vivo [O] . Jingsong Xu, Dorothy Rodriguez, Eric Petitclerc, 2001

机译：体内血管生成和肿瘤生长需要蛋白水解性暴露IV型胶原内的隐性位点
7. Proteolytic exposure of a cryptic site within collagen type IV is required for angiogenesis and tumor growth in vivo [O] . Xu, Jingsong, Rodriguez, Dorothy, Petitclerc, Eric, 2001

机译：体内血管生成和肿瘤生长需要蛋白水解性暴露IV型胶原内的隐性位点
8. Can Labeled Human CD 34+ Lymphocytes be Used to Identify Sites of Angiogenesis Within Growing Tumors [R] . Brooks, S. P. 2002

机译：标记的人CD 34+淋巴细胞可用于识别生长肿瘤内血管生成的位点

Proteolytic exposure of a cryptic site within collagen type IV is required for angiogenesis and tumor growth in vivo

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