首页> 外文OA文献 >Interaction between the insulin-like growth factor family and the integrin receptor family in tissue repair processes. Evidence in a rabbit ear dermal ulcer model.
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Interaction between the insulin-like growth factor family and the integrin receptor family in tissue repair processes. Evidence in a rabbit ear dermal ulcer model.

机译:胰岛素样生长因子家族和整联蛋白受体家族在组织修复过程中的相互作用。兔耳皮肤溃疡模型的证据。

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摘要

We have determined previously that IGF-I is dependent on the presence of IGF binding protein-1 (IGFBP-1) to act as a wound healing agent. We sought to determine the mechanism whereby IGFBP-1 is able to enhance IGF-I bioactivity. As IGFBP-1 binds both the alpha5beta1 integrin as well as IGF-I in vitro, we asked which of the following interactions were important: (a) the ability of IGFBP-1 to interact with an integrin receptor, and/or (b) the binding of IGF-I by IGFBP-1. We used an IGF-1 analogue (des(1-3)IGF-I) with a > 100-fold reduction in affinity for IGFBP-1 as well as an IGFBP-1 mutant (WGD-IGFBP-1) which does not associate with the alpha5beta1 integrin to selectively abrogate each of these interactions. We also tested the ability of IGFBP-2, a related binding protein which has an arginine-glycine-aspartate sequence but does not associate with integrin family members, to enhance IGF-I bioactivity. Full-thickness dermal wounds were created on rabbit ears; various combinations of native IGF-I, native IGFBP-1, native IGFBP-2, and their respective analogues/mutants were applied to each wound. Wounds were harvested 7 d later for analysis. Only native IGF-I in combination with native IGFBP-1 was effective as a wound healing agent, enhancing reepithelialization and granulation tissue deposition by 64+/-5 and 83+/-12% over controls (P = 0.008 and 0.016, respectively). The same doses of IGF-I/WGD-IGFBP-1, des(1-3)IGF-I/IGFBP-1, and IGF-I/IGFBP-2 were ineffective. We propose that IGF-I physically interacts with IGFBP-1 and that IGFBP-1 also binds to an integrin receptor, most likely the alpha5beta1 integrin. This interaction is unique to IGFBP-1 as the closely related IGFBP-2 had no effect, a finding consistent with its inability to bind to integrin receptors. Our results suggest that activation of both the IGF-I receptor and the alpha5beta1 integrin is required for IGF-I to stimulate wound healing.
机译:先前我们已经确定,IGF-I依赖于IGF结合蛋白1(IGFBP-1)的存在来充当伤口愈合剂。我们试图确定IGFBP-1能够增强IGF-1生物活性的机制。由于IGFBP-1在体外与alpha5beta1整合素和IGF-1结合,我们询问以下哪些相互作用很重要:(a)IGFBP-1与整合素受体相互作用的能力,和/或(b) IGFBP-1与IGF-1的结合。我们使用的IGF-1类似物(des(1-3)IGF-I)对IGFBP-1的亲和力降低了100倍以上,并且IGFBP-1突变体(WGD-IGFBP-1)没有关联与alpha5beta1整合素选择性地消除这些相互作用中的每一个。我们还测试了IGFBP-2(一种具有精氨酸-甘氨酸-天冬氨酸序列但不与整合素家族成员结合的相关结合蛋白)增强IGF-1生物活性的能力。在兔耳上形成了全层真皮伤口;将天然IGF-1,天然IGFBP-1,天然IGFBP-2的各种组合以及它们各自的类似物/突变体应用于每个伤口。 7天后收获伤口用于分析。只有天然IGF-I与天然IGFBP-1结合才能有效用作伤口愈合剂,与对照组相比,可使上皮再形成和肉芽组织沉积增加64 +/- 5和83 +/- 12%(分别为P = 0.008和0.016) 。相同剂量的IGF-1 / WGD-IGFBP-1,des(1-3)IGF-1 / IGFBP-1和IGF-1 / IGFBP-2无效。我们建议IGF-1与IGFBP-1进行物理相互作用,并且IGFBP-1也与整联蛋白受体结合,最有可能是α5beta1整联蛋白。这种相互作用是IGFBP-1特有的,因为紧密相关的IGFBP-2没有作用,这一发现与其不能结合整联蛋白受体相一致。我们的结果表明,IGF-I刺激伤口愈合需要激活IGF-I受体和alpha5beta1整合素。

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