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人类中性粒细胞对凝血酶的反应:两种新型受体的证据。

The response to thrombin of human neutrophils: evidence for two novel receptors.

作者信息

Jenkins A L, Howells G L, Scott E, Le Bonniec B F, Curtis M A, Stone S R

机构信息

Department of Haematology, University of Cambridge, UK.

出版信息

J Cell Sci. 1995 Sep;108 ( Pt 9):3059-66. doi: 10.1242/jcs.108.9.3059.

Abstract

Human alpha-thrombin was a chemoattractant for human neutrophils yielding a maximal response of similar magnitude to that observed with formyl-Met-Leu-Phe. The observed chemotaxis was not due to stimulation of the proteolytically activated thrombin receptor since: (1) this receptor was not detected by flow cytometry; (2) the inactive thrombin mutant Ser195-->Ala elicited a chemotactic response indistinguishable from that caused by wild-type thrombin; (3) antibodies to the cleavage site of the proteolytically activated receptor did not affect thrombin-induced chemotaxis; (4) a thrombin receptor activating peptide (TRAP) failed to stimulate chemotaxis. These data indicate the existence of a thrombin receptor for neutrophil chemotaxis which is not activated by proteolysis. In addition, although wild-type and ser195-->Ala thrombin did not cause an increase in intracellular Ca2+, a Ca2+ response to TRAP was observed with neutrophils from some donors. The TRAP-induced increase in Ca2+ was reproducible, dose dependent and specific. The use of alanine-substituted peptides demonstrated that the Ca2+ response was due to TRAP stimulation of a receptor other than the proteolytically activated thrombin receptor. Thus, it is necessary to re-evaluate the assumption made in previous studies that responses to TRAP are mediated by the proteolytically activated thrombin receptor.

摘要

人α-凝血酶是人类中性粒细胞的趋化因子,其产生的最大反应幅度与甲酰甲硫氨酰亮氨酰苯丙氨酸所观察到的相似。观察到的趋化作用并非由于蛋白水解激活的凝血酶受体的刺激,原因如下:(1) 通过流式细胞术未检测到该受体;(2) 无活性的凝血酶突变体Ser195→Ala引发的趋化反应与野生型凝血酶引起的趋化反应无法区分;(3) 针对蛋白水解激活受体切割位点的抗体不影响凝血酶诱导的趋化作用;(4) 凝血酶受体激活肽(TRAP)未能刺激趋化作用。这些数据表明存在一种用于中性粒细胞趋化的凝血酶受体,其不会被蛋白水解激活。此外,尽管野生型和Ser195→Ala凝血酶不会导致细胞内Ca2+增加,但在一些供体的中性粒细胞中观察到了对TRAP的Ca2+反应。TRAP诱导的Ca2+增加是可重复的、剂量依赖性的且具有特异性。使用丙氨酸取代的肽表明,Ca2+反应是由于TRAP刺激了除蛋白水解激活的凝血酶受体之外的另一种受体。因此,有必要重新评估先前研究中所做的假设,即对TRAP的反应是由蛋白水解激活的凝血酶受体介导的。

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