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Female platelets have distinct functional activity compared with male platelets: Implications in transfusion practice and treatment of trauma-induced coagulopathy

机译:与雄性血小板相比,雌性血小板具有明显的功能活性:对输血实践的影响和创伤诱导的凝血病的治疗方法

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BACKGROUND Females are hypercoagulable and have survival benefit in trauma-induced coagulopathy (TIC). The mechanism for this sex-specific hypercoagulability is unknown. Platelets and platelet function are central in providing hemostatic potential and are the largest contributor to clot strength. Ligands (adenosine diphosphate [ADP] and platelet-activating factor [PAF]) bind distinct platelet receptors to potentiate activation and aggregation. We hypothesize that female platelets have a differential response to ADP and PAF, resulting in greater aggregation and activation compared to males, and that estradiol pretreatment of male or female platelets enhances this activity. METHODS Platelets were collected from healthy volunteers: premenopausal/postmenopausal females ( 54 years) and similarly aged males. Platelet aggregometry and flow cytometry (fibrinogen binding capacity) were examined. After treatment with ADP or PAF, platelet aggregation was assessed with Chronolog and activation assessed by CD41 receptor surface expression using flow cytometry. Aggregation and activation were again assessed after platelet pretreatment with estradiol. RESULTS Healthy volunteers included 12 premenopausal and 13 postmenopausal females and 18 similarly aged males. Female platelets (combined premenopausal and postmenopausal) had increased aggregation with ADP stimulation, as compared to male platelets. Male and female platelets had differential fibrinogen receptor expression, with female platelets (combined premenopausal and postmenopausal) demonstrating robust activation with ADP versus male platelets with PAF. In the presence of estradiol incubation, male platelets' activation with PAF approximated that of females (combined premenopausal and postmenopausal) and activation with PAF was enhanced in both male and female platelets. CONCLUSION Male and female platelets have differential response to stimuli, suggesting sex-dependent signaling and cellular activation. Female platelets have both increased aggregation and activation potential, and estradiol pretreatment feminizes male platelets to approximate female platelet activation with PAF. These findings offer potential explanation for sex-based differences in hemostatic potential in TIC and question whether donor sex of transfused platelets should be considered in resuscitation. Estradiol may also serve as a novel therapeutic adjunct in TIC.
机译:背景雌性是高核酸的并且在创伤诱导的凝血病(TIC)中具有生存益处。这种性别特异性高凝的机制是未知的。血小板和血小板功能是提供止血潜力的中心,是凝块强度的最大贡献者。配体(腺苷二磷酸[ADP]和血小板活化因子[PAF])结合不同的血小板受体以增强活化和聚集。我们假设雌性血小板对ADP和PAF具有差异反应,导致与雄性相比具有更大的聚集和活化,并且雌性血小板的雌二醇预处理增强了该活性。方法从健康的志愿者收集血小板:前辈/绝经后雌性女性(54岁)和类似的男性。检查血小板聚集和流式细胞术(纤维蛋白原结合能力)。用ADP或PAF处理后,使用流式细胞术评估CD41受体表面表达评估的计时和激活进行血小板聚集。在用雌二醇血小板预处理后再次评估聚集和活化。结果健康的志愿者包括12个前肢和13名绝经后血管女性和18名同样老年男性。与雄性血小板相比,雌性血小板(联合前肢和绝经期)与ADP刺激的聚集增加。雄性和雌性血小板具有差异纤维蛋白原受体表达,雌性血小板(联合前肢和绝经期)展示了具有PAF的ADP与雄性血小板的鲁棒激活。在雌二醇孵育的存在下,用PAF的血小板激活近似于雌性血小板(联合前肢和绝经)和PAF活化的激活在雄性和雌性血小板中增强。结论男性和雌性血小板对刺激的差异反应,表明性依赖性信号传导和细胞活化。雌性血小板均具有增加的聚集和活化潜力,并且雌二醇预处理是女性血小板,以用PAF近似的雌性血小板活化。这些调查结果为性别的止血潜力差异提供了潜在的解释,并质疑转发血小板的供体性是否应考虑在复苏中。雌二醇也可作为TIC的新型治疗辅助。

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