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杆菌肽揭示了多种硫醇异构酶在血小板功能中的作用。

Bacitracin reveals a role for multiple thiol isomerases in platelet function.

作者信息

Robinson Aisling, O'Neill Sarah, Kiernan Aoife, O'Donoghue Niaobh, Moran Niamh

机构信息

Department of Clinical Pharmacology, Royal College of Surgeons in Ireland, Dublin 2, Ireland.

出版信息

Br J Haematol. 2006 Feb;132(3):339-48. doi: 10.1111/j.1365-2141.2005.05878.x.

Abstract

The platelet-specific integrin alphaIIb beta3 has endogenous thiol isomerase activity associated with the CXXC motifs within the beta subunit. Using a highly purified form of bacitracin, a thiol isomerase inhibitor, we now provide further evidence of the functional significance of this enzymatic activity in integrin activation. In addition, we demonstrate a role for multiple thiol isomerases in platelet function. This bacitracin prevented platelet aggregation to thrombin and collagen, and directly inhibited alphaIIb beta3 activation, as detected by PAC-1 binding. In parallel, bacitracin inhibited the endogenous thiol isomerase activity of purified alphaIIb beta3 with a 50% inhibitory concentration of 15.5 micromol/l. In order to determine whether the effects of bacitracin are solely mediated by inhibition of integrin enzymatic activity, we examined integrin-independent indices of platelet activation. We found bacitracin inhibited both platelet secretion (CD62P and CD63) and thromboxane (TxA2) production, with complete inhibition at different concentrations. Thus, we demonstrated a role for multiple thiol isomerases in platelet function. Taken together, these studies support a role for the endogenous integrin thiol isomerase activity in activation of alphaIIb beta3 and highlight the novel regulation of platelet function by other, as yet undefined thiol isomerases.

摘要

血小板特异性整合素αIIbβ3具有与β亚基内CXXC基序相关的内源性硫醇异构酶活性。我们使用一种硫醇异构酶抑制剂——高度纯化形式的杆菌肽,进一步证明了这种酶活性在整合素激活中的功能重要性。此外,我们还证明了多种硫醇异构酶在血小板功能中的作用。这种杆菌肽可防止血小板对凝血酶和胶原蛋白的聚集,并直接抑制αIIbβ3的激活,这可通过PAC-1结合检测到。同时,杆菌肽以15.5微摩尔/升的50%抑制浓度抑制纯化的αIIbβ3的内源性硫醇异构酶活性。为了确定杆菌肽的作用是否仅由整合素酶活性的抑制介导,我们检查了血小板激活的整合素非依赖性指标。我们发现杆菌肽抑制血小板分泌(CD62P和CD63)和血栓素(TxA2)的产生,在不同浓度下均完全抑制。因此,我们证明了多种硫醇异构酶在血小板功能中的作用。综上所述,这些研究支持内源性整合素硫醇异构酶活性在αIIbβ3激活中的作用,并突出了其他尚未明确的硫醇异构酶对血小板功能的新调节作用。

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