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In vivo tracking of platelets: circulating degranulated platelets rapidly lose surface P-selectin but continue to circulate and function.

机译：体内追踪血小板：循环的脱颗粒血小板迅速失去表面P-选择蛋白，但继续循环并发挥作用。

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To examine the hypothesis that surface P-selectin-positive (degranulated) platelets are rapidly cleared from the circulation, we developed novel methods for tracking of platelets and measurement of platelet function in vivo. Washed platelets prepared from nonhuman primates (baboons) were labeled with PKH2 (a lipophilic fluorescent dye), thrombin-activated, washed, and reinfused into the same baboons. Three-color whole blood flow cytometry was used to simultaneously (i) identify platelets with a mAb directed against glycoprotein (GP)IIb-IIIa (integrin alpha 11b beta 3), (ii) distinguish infused platelets by their PKH2 fluorescence, and (iii) analyze platelet function with mAbs. Two hours after infusion of autologous thrombin-activated platelets (P-selectin-positive, PKH2-labeled), 95 +/- 1% (mean +/- SEM, n = 5) of the circulating PKH2-labeled platelets had become P-selectin-negative. Compared with platelets not activated with thrombin preinfusion, the recovery of these circulating PKH2-labeled, P-selectin-negative platelets was similar 24 h after infusion and only slightly less 48 h after infusion. The loss of platelet surface P-selectin was fully accounted for by a 67.1 +/- 16.7 ng/ml increase in the plasma concentration of soluble P-selectin. The circulating PKH2-labeled, P-selectin-negative platelets were still able to function in vivo, as determined by their (i) participation in platelet aggregates emerging from a bleeding time wound, (ii) binding to Dacron in an arteriovenous shunt, (iii) binding of mAb PAC1 (directed against the fibrinogen binding site on GPIIb-IIIa), and (iv) generation of procoagulant platelet-derived microparticles. In summary, (i) circulating degranulated platelets rapidly lose surface P-selectin to the plasma pool, but continue to circulate and function; and (ii) we have developed novel three-color whole blood flow cytometric methods for tracking of platelets and measurement of platelet function in vivo.

机译：为了检查表面P-选择蛋白阳性（脱粒的）血小板迅速从循环中清除的假说，我们开发了在体内追踪血小板和测量血小板功能的新方法。用PKH2（亲脂性荧光染料）标记从非人类灵长类动物（狒狒）制备的洗涤血小板，进行凝血酶活化，洗涤并重新注入相同的狒狒中。三色全血流式细胞仪用于同时（i）鉴定具有针对糖蛋白（GP）IIb-IIIa（整联蛋白alpha 11b beta 3）的mAb的血小板，（ii）通过其PKH2荧光区分注入的血小板，和（iii））使用mAb分析血小板功能。输注自体凝血酶激活的血小板（P-选择蛋白阳性，PKH2标记）后两小时，循环PKH2标记的血小板中95 +/- 1％（平均值+/- SEM，n = 5）变为P-选择素阴性。与未通过凝血酶预输注激活的血小板相比，这些循环的PKH2标记的P-选择素阴性血小板的恢复在输注后24小时相似，而在输注后48小时仅稍少。血小板表面P-选择素的损失完全由可溶性P-选择素的血浆浓度增加67.1 +/- 16.7 ng / ml造成。循环的PKH2标记的P-选择素阴性血小板仍然能够在体内发挥作用，这取决于它们（i）参与从出血时间伤口中流出的血小板聚集体，（ii）在动静脉分流器中与达可隆结合，（ iii）mAb PAC1的结合（针对GPIIb-IIIa上的纤维蛋白原结合位点），以及（iv）促血小板源性微粒的产生。总之，（i）循环的脱颗粒血小板迅速使表面P-选择蛋白流失到血浆库中，但继续循环并发挥作用；（ii）我们开发了新颖的三色全血流式细胞术，用于体内跟踪血小板和测量血小板功能。

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Michelson, A D; Barnard, M R; Hechtman, H B; MacGregor, H; Connolly, R J; Loscalzo, J; Valeri, C R;
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年度 1996
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1. In vivo tracking of platelets: Circulating degranulated platelets rapidly lose surface P-selectin but continue to circulate and function [J] . Alan D. Michelson, Marc R. Barnard, Herbert B. Hechtman Proceedings of the National Academy of Sciences of the United States of America . 1996,第21期

机译：体内追踪血小板：循环的脱颗粒血小板迅速丧失表面P-选择蛋白，但继续循环并发挥作用
2. Circulating monocyte-platelet aggregates are a more sensitive marker of in vivo platelet activation than platelet surface P-selectin: studies in baboons, human coronary intervention, and human acute myocardial infarction. [J] . Michelson AD, Barnard MR, Krueger LA, Circulation: An Official Journal of the American Heart Association . 2001,第13期

机译：循环单核细胞-血小板聚集体比血小板表面P-选择素是体内血小板活化更敏感的标志物：狒狒，人类冠状动脉介入和人类急性心肌梗死的研究。
3. Circulating monocyte-platelet aggregates are a more sensitive marker of in vivo platelet activation than platelet surface P-selectin: studies in baboons, human coronary intervention, and human acute myocardial infarction. [J] . Michelson AD, Barnard MR, Krueger LA, Circulation: An Official Journal of the American Heart Association . 2001,第13期

机译：循环单核细胞-血小板聚集体比血小板表面P-选择素是体内血小板活化更敏感的标志物：狒狒，人类冠状动脉介入和人类急性心肌梗死的研究。
4. Detection of circulating platelet microaggregates and surface microthrombi during continuous flow LVAD: evidence for shear-induced platelet activation [C] . Linneweber, J., Chow, . 2002

机译：LVAD连续流动过程中循环血小板微聚集体和表面微血栓的检测：剪切诱导的血小板活化的证据
5. Elevated circulating aldosterone and platelet activity in overweight/obese young adults: Roles in vascular remodeling and cardiometabolic health. [D] . Cooper, Jennifer N. 2012

机译：超重/肥胖年轻人中循环醛固酮和血小板活性的升高：在血管重塑和心脏代谢健康中的作用。
6. In vivo tracking of platelets: circulating degranulated platelets rapidly lose surface P-selectin but continue to circulate and function. [O] . A D Michelson, M R Barnard, H B Hechtman, 1996

机译：体内追踪血小板：循环的脱颗粒血小板迅速失去表面P-选择蛋白但继续循环并发挥作用。
7. In vivo tracking of platelets: circulating degranulated platelets rapidly lose surface P-selectin but continue to circulate and function [O] . Michelson, Alan D., Barnard, Marc R., Hechtman, Herbert B., 1996

机译：体内跟踪血小板：循环脱颗粒血小板迅速失去表面p-选择素但继续循环和功能
8. In Vivo Tracking of Platelets: Circulating Degranulated Platelets Rapidly Lose Surface P-Selectin but Continue to Circulate and Function [R] . Michelson, A. D. , Barnard, M. R. , Hechtman, H. B. , 1995

机译：血小板的体内追踪：循环脱颗粒血小板迅速失去表面p-选择素但继续循环和功能

In vivo tracking of platelets: circulating degranulated platelets rapidly lose surface P-selectin but continue to circulate and function.

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