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Carbohydrate-independent recognition of collagens by the macrophage mannose receptor.

机译:Carbohydrate-independent识别空泡巨噬细胞的甘露糖受体。

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摘要

Mannose receptor (MR) is the best characterised member of a family of four endocytic molecules that share a common domain structure; a cysteine-rich (CR) domain, a fibronectin-type II (FNII) domain and tandemly arranged C-type lectin-like domains (CTLD, eight in the case of MR). Two distinct lectin activities have been described for MR. The CR domain recognises sulphated carbohydrates while the CTLD mediate binding to mannose, fucose or N-acetylglucosamine. FNII domains are known to be important for collagen binding and this has been studied in the context of two members of the MR family, Endo180 and the phospholipase A2 receptor. Here, we have investigated whether the broad and effective lectin activity mediated by the CR domain and CTLD of MR is favoured to the detriment of FNII-mediated interaction(s). We show that MR is able to bind and internalise collagen in a carbohydrate-independent manner and that MR deficient macrophages have a marked defect in collagen IV and gelatin internalisation. These data have major implications at the molecular level as there are now three distinct ligand-binding sites described for MR. Furthermore our findings extend the range of endogenous ligands recognised by MR, a molecule firmly placed at the interface between homeostasis and immunity.
机译:甘露糖受体(MR)是最好的特征一个四口之家的成员内吞作用的分子共享一个共同的域结构;fibronectin-type II cysteine-rich (CR)域(FNII)域和衔接着这种安排lectin-like域(CTLD八的情况先生)。描述CR域先生承认硫酸化的碳水化合物而CTLD调解绑定到甘露糖、植物种子或N-acetylglucosamine。对胶原蛋白绑定和这很重要研究中两个成员家庭,Endo180和磷脂酶A2受体。广泛和有效的活动由外源凝集素先生的CR域和CTLD的青睐不利于FNII-mediated交互(s)。表明先生能够绑定和吸收胶原蛋白carbohydrate-independent的方式先生巨噬细胞有明显不足缺陷在第四胶原蛋白和明胶掩饰。有在分子水平上的影响现在三个不同的配体结合网站描述此外先生我们的发现扩展范围内源性配体被先生承认的分子牢固地放置在之间的接口体内平衡和免疫力。

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