首页> 美国卫生研究院文献>Biochemical Journal >Neutrophil lysosomal dysfunctions in mutant C57 Bl/6J mice: interstrain variations in content of lysosomal elastase cathepsin G and their inhibitors.
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Neutrophil lysosomal dysfunctions in mutant C57 Bl/6J mice: interstrain variations in content of lysosomal elastase cathepsin G and their inhibitors.

机译:突变C57 Bl / 6J小鼠中的中性粒细胞溶酶体功能异常:溶酶体弹性蛋白酶组织蛋白酶G及其抑制剂含量的株间变异。

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摘要

In this paper we report the serum antiprotease screening and the biochemical and functional characteristics of neutrophils in a variety of mouse strains with different susceptibilities for developing a protease-mediated injury. C57Bl/6J mice and their mutants tight-skin and pallid have a lower serum elastase inhibitory capacity (-30, -65 and -70% respectively) than other inbred strains (i.e. NMRI and Balb/c, which both have similar values). We demonstrate that these values are a consequence of a decreased concentration of the alpha 1-protease inhibitor for elastase [PI(E)], which is the major serum inhibitor of elastase and cathepsin G. In addition, neutrophil lysosomal dysfunctions characterized by abnormally high contents of elastase and cathepsin G, or defective lysosomal secretion are observed in tight-skin and pallid mice respectively. Another C57Bl/6J mutant with lysosomal abnormalities is the beige mouse. Negligible amounts of elastase and cathepsin G, as well as defective neutrophil degranulation, have been described previously in this strain. We found, however, discrete amounts of a latent form of neutrophil elastase that undergoes a spontaneous activation by a protease-dependent mechanism. We also report that neutrophil cathepsin G in this mouse is tightly bound to lysosomal membranes, but is released in near normal quantities during exocytosis. Cytosolic elastase and cathepsin G inhibitors, which were previously reported as being specific for the beige neutrophils, have also been detected in all the examined strains. Neutrophil functions, lysosomal enzyme content and serum antiprotease screening may represent key elements in the protease-antiprotease balance and may explain the different interstrain susceptibility to developing lesions in which an elastolytic activity has been implicated.
机译:在本文中,我们报告了血清抗蛋白酶的筛选以及嗜中性白细胞的生化和功能特性,这些小鼠在发生蛋白酶介导的损伤时具有不同的敏感性。与其他近交系(即NMRI和Balb / c都具有相似的值)相比,C57Bl / 6J小鼠及其紧密皮肤和苍白球突变体的血清弹性蛋白酶抑制能力较低(分别为-30%,-65%和-70%)。我们证明这些值是弹性蛋白酶和组织蛋白酶G的主要血清抑制剂–弹性蛋白酶[PI(E)]的α1-蛋白酶抑制剂浓度降低的结果。此外,中性粒细胞溶酶体功能障碍的特征是异常高分别在紧肤和苍白的小鼠中观察到弹性蛋白酶和组织蛋白酶G的含量或溶酶体分泌缺陷。另一个具有溶酶体异常的C57Bl / 6J突变体是米色小鼠。先前已经在该菌株中描述了可忽略量的弹性蛋白酶和组织蛋白酶G,以及嗜中性粒细胞脱粒缺陷。然而,我们发现离散量的潜伏形式的嗜中性粒细胞弹性蛋白酶通过蛋白酶依赖性机制自发激活。我们还报告说,这只小鼠中的中性粒细胞组织蛋白酶G与溶酶体膜紧密结合,但在胞吐过程中以接近正常的量释放。以前据报道对米色中性粒细胞具有特异性的胞质弹性蛋白酶和组织蛋白酶G抑制剂也已在所有检测菌株中检测到。中性粒细胞功能,溶酶体酶含量和血清抗蛋白酶筛选可能代表了蛋白酶-抗蛋白酶平衡中的关键要素,并可能解释了不同的株间易感性对发展中涉及弹性蛋白酶活性的病变的敏感性。

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