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正常人与免疫性血小板减少症患者之间以及年轻血小板与衰老血小板之间血小板α-颗粒释放的差异。

Differences in platelet alpha-granule release between normals and immune thrombocytopenic patients and between young and old platelets.

作者信息

Rinder H M, Tracey J B, Recht M, DeCastro L, Rinder C S, McHugh C, Smith B R

机构信息

Department of Laboratory Medicine, Yale University School of Medicine, New Haven, CT 06520-8035, USA.

出版信息

Thromb Haemost. 1998 Sep;80(3):457-62.

PMID:9759627
Abstract

The risk of serious bleeding in patients with immune thrombocytopenic purpura (ITP) appears to be less than in comparably thrombocytopenic patients with megakaryocytic hypoplasia. It has been proposed that this difference is due to enhanced hemostatic activity of young platelets, which are increased in the circulation during ITP. We examined alpha-granule release in reticulated platelets (RP), which are thought to be the youngest circulating platelets, and in older non-reticulated platelets (non-RP) in normal human controls and ITP patients. Normal controls had a mean RP of 7%, compared with 42% in ITP patients. The mean concentration of thrombin receptor agonist peptide (TRAP) causing 50% of control RP to express CD62P (EC50) was 0.82+/-0.08 microM (SEM), significantly higher than the TRAP CD62P EC50 for RP in ITP, 0.57+/-0.06 microM (p = 0.04). Similarly, the TRAP EC50 for non-RP in controls, 0.84+/-0.09 microM, was significantly higher than in ITP, 0.56+/-0.07 microM (p = 0.03), suggesting that all platelets in ITP have an enhanced alpha-granule threshold response to TRAP compared with controls, while RP and older platelets within each patient group have similar threshold sensitivities to TRAP. By contrast, high-dose TRAP caused RP to express twice as much mean and total CD62P as non-RP in both ITP patients and controls (p <0.05 for both comparisons). We conclude that compared with controls, all platelets in ITP are primed to undergo alpha-granule release to TRAP, while in both ITP and controls, the newly circulating, reticulated platelets have the potential to contribute greater amounts of CD62P surface ligand compared with older platelets (non-RP) after stimulation. Both the increased RP% and enhanced platelet response to agonist in ITP may contribute to maintenance of hemostasis despite thrombocytopenia.

摘要

免疫性血小板减少性紫癜(ITP)患者发生严重出血的风险似乎低于血小板生成减少性巨核细胞发育不全的血小板减少患者。有人提出,这种差异是由于年轻血小板的止血活性增强,而在ITP期间循环中的年轻血小板数量增加。我们检测了网织血小板(RP)(被认为是循环中最年轻的血小板)和正常人类对照及ITP患者中较老的非网织血小板(非RP)的α-颗粒释放情况。正常对照的平均RP为7%,而ITP患者为42%。使50%的对照RP表达CD62P的凝血酶受体激动肽(TRAP)的平均浓度(EC50)为0.82±0.08微摩尔/升(SEM),显著高于ITP中RP的TRAP CD62P EC50,即0.57±0.06微摩尔/升(p = 0.04)。同样,对照中非RP的TRAP EC50为0.84±0.09微摩尔/升,显著高于ITP中的0.56±0.07微摩尔/升(p = 0.03),这表明与对照相比,ITP中的所有血小板对TRAP的α-颗粒阈值反应增强,而每个患者组内的RP和较老的血小板对TRAP具有相似的阈值敏感性。相比之下,高剂量TRAP使ITP患者和对照中的RP表达的平均和总CD62P是非RP的两倍(两个比较的p均<0.05)。我们得出结论,与对照相比,ITP中的所有血小板都易于对TRAP发生α-颗粒释放,而在ITP和对照中,新循环的网织血小板在受到刺激后与较老的血小板(非RP)相比,有潜力贡献更多量的CD62P表面配体。ITP中增加的RP%和血小板对激动剂增强的反应可能有助于在血小板减少的情况下维持止血。

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