首页> 美国卫生研究院文献>Journal of the Boston Society of Medical Sciences >The chemical mediation of delayed hypersensitivity skin reactions: III. Purification and characterization of a precursor protein for macrophage-chemotactic factor in normal guinea pig plasma.
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The chemical mediation of delayed hypersensitivity skin reactions: III. Purification and characterization of a precursor protein for macrophage-chemotactic factor in normal guinea pig plasma.

机译:迟发型超敏反应皮肤反应的化学介导:III。正常豚鼠血浆中巨噬细胞趋化因子前体蛋白的纯化和鉴定。

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摘要

A putative precursor protein for macrophage-chemotactic factor, which was extracted fro inflammatory skin sites (MCFS-1) (Kambara et al, Am J Pathol 1977, 87:359-374), was found in normal guinea pig plasma and was purified to an apparent homogeneity upon SDS-polyacrylamide gel electrophoresis with a molecular weight of 160,000. This plasma protein was different from complement components of C3 and C5 in terms of molecular weight, functional activity as complements detected by hemolytic assay, and immunologic properties. Although it exhibited the common antigenicity with MCFS-1, it did not show any chemotactic activity for macrophages, However, incubation of this plasma protein at either 4 C for 5 days or 37 C for 1-2 days could generate a chemotactic factor with a molecular weight of approximately 150,000 which was similar to that of MCFS-1. This generation of chemotactic activity was completely prevented by the presence of the serine-type protease inhibitor, phenylmethylsulfonyl fluoride. These data could be well accounted for if we assume that this plasma protein might be a precursor for the macrophage-chemotactic factor found in delayed hypersensitivity skin sites, and that a proteolytic process might be involved in the activation of this precursor.
机译:在正常的豚鼠血浆中发现一种假定的巨噬细胞趋化因子前体蛋白,该蛋白是从炎症性皮肤部位(MCFS-1)提取的(Kambara等人,Am J Pathol 1977,87:359-374)。在分子量为160,000的SDS-聚丙烯酰胺凝胶电泳时具有明显的均质性。该血浆蛋白在分子量,通过溶血测定法检测的补体的功能活性和免疫学特性方面与C3和C5的补体成分不同。尽管它具有与MCFS-1相同的抗原性,但它对巨噬细胞没有任何趋化活性,但是,将这种血浆蛋白在4 C下孵育5天或在37 C下孵育1-2天可以产生具有以下特征的趋化因子:分子量约为150,000,与MCFS-1相似。丝氨酸型蛋白酶抑制剂苯甲基磺酰氟的存在完全阻止了这种趋化活性的产生。如果我们假设这种血浆蛋白可能是在迟发型超敏反应皮肤部位发现的巨噬细胞趋化因子的前体,并且蛋白水解过程可能与该前体的活化有关,则可以很好地解释这些数据。

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