An aminopeptidase regulates LPS stimulated interleukin-8 receptor on the surface of human neutrophils

被引:0
作者
Bhattacharya, C
Manna, SK
Samanta, S
Gupta, SK
Samanta, AK
机构
[1] INDIAN INST CHEM BIOL,DIV IMMUNOBIOL,CALCUTTA 700032,W BENGAL,INDIA
[2] INDIAN STAT INST,DIV BIOMETRY,CALCUTTA 700035,W BENGAL,INDIA
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中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
A large number of inflammatory diseases are mediated by interleukin-8, an inflammatory neutrophil chemotactic agent. Since the cytokine acts through a cell surface receptor, detailed knowledge about the regulation of receptor expression is very important. We found that LPS in serum became activated and triggered the expression of IL-8 receptor by more than two folds within 30 min. After that period, the receptor attained normal level within 2 hr of SA-LPS stimulation. EDTA and bestatin could block this Ca2+ level was increased till 45 min of SA-LPS stimulation downregulation of IL-8 receptor. Intracellular Ca2+ inhibited the and then the level was reduced. Addition of CaCl2 accelerated and depletion of Ca2+ downregulaion of the IL-8 receptor. The ligand could fully protect the loss of receptor from downregulation. It suggests that during SA-LPS stimulation, increase in intracellular Ca2+ level activates an aminopeptidase which presumably cleaves the N-terminal region of the receptor, critically essential for the function of IL-8. Thus the activated aminopeptidase regulates the functions of IL-8. The study is important for understanding the regulation of IL-8 receptor expression by LPS during bacterial infection.
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页码:214 / 219
页数:6
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