Michelson A D, Furman M I, Goldschmidt-Clermont P, Mascelli M A, Hendrix C, Coleman L, Hamlington J, Barnard M R, Kickler T, Christie D J, Kundu S, Bray P F
Departments of Medicine and Pathology, Johns Hopkins University School of Medicine, Baltimore, MD 21205, USA.
Circulation. 2000 Mar 7;101(9):1013-8. doi: 10.1161/01.cir.101.9.1013.
Both inherited predisposition and platelet hyperreactivity have been associated with ischemic coronary events, but mechanisms that support genetic differences among platelets from different subjects are generally lacking. Associations between the platelet Pl(A2) polymorphism of GP IIIa and coronary syndromes raise the question as to whether this inherited variation may contribute to platelet hyperreactivity.
In this study, we characterized functional parameters in platelets from healthy donors with the Pl(A) (HPA-1) polymorphism, a Leu (Pl(A1)) to Pro (Pl(A2)) substitution at position 33 of the GP IIIa subunit of the platelet GP IIb/IIIa receptor (integrin alpha(IIb)beta(3)). We studied 56 normal donors (20 Pl(A1,A1), 20 Pl(A1,A2), and 16 Pl(A2,A2)). Compared with Pl(A1,A1) platelets, Pl(A2)-positive platelets showed a gene dosage effect for significantly greater surface-expressed P-selectin, GP IIb/IIIa-bound fibrinogen, and activated GP IIb/IIIa in response to low-dose ADP. Surface expression of GP IIb/IIIa was similar in resting platelets of all 3 genotypes but was significantly greater on Pl(A2,A2) platelets after ADP stimulation (P=0.003 versus Pl(A1,A1); P=0.03 versus Pl(A1,A2)). Pl(A1,A2) platelets were more sensitive to inhibition of aggregation by pharmacologically relevant concentrations of aspirin and abciximab.
Pl(A2)-positive platelets displayed a lower threshold for activation, and platelets heterozygous for Pl(A) alleles showed increased sensitivity to 2 antiplatelet drugs. These in vitro platelet studies may have relevance for in vivo thrombotic conditions.
遗传易感性和血小板高反应性均与缺血性冠状动脉事件相关,但不同个体血小板间遗传差异的支持机制通常尚不明确。血小板糖蛋白IIIa的Pl(A2)多态性与冠状动脉综合征之间的关联引发了这样一个问题,即这种遗传变异是否可能导致血小板高反应性。
在本研究中,我们对具有Pl(A)(HPA-1)多态性(血小板糖蛋白IIb/IIIa受体(整合素α(IIb)β(3))的糖蛋白IIIa亚基第33位氨基酸由亮氨酸(Pl(A1))替换为脯氨酸(Pl(A2)))的健康供者血小板的功能参数进行了表征。我们研究了56名正常供者(20名Pl(A1,A1)、20名Pl(A1,A2)和16名Pl(A2,A2))。与Pl(A1,A1)血小板相比,Pl(A2)阳性血小板在低剂量ADP刺激下,表面表达的P-选择素、与糖蛋白IIb/IIIa结合的纤维蛋白原以及活化的糖蛋白IIb/IIIa呈现基因剂量效应,显著增加。所有3种基因型静息血小板中糖蛋白IIb/IIIa的表面表达相似,但在ADP刺激后,Pl(A2,A2)血小板上的表达显著更高(与Pl(A1,A1)相比,P = 0·003;与Pl(A1,A2)相比,P = 0·03)。Pl(A1,A2)血小板对药理学相关浓度的阿司匹林和阿昔单抗抑制聚集更为敏感。
Pl(A2)阳性血小板表现出较低的激活阈值,Pl(A)等位基因杂合的血小板对两种抗血小板药物的敏感性增加。这些体外血小板研究可能与体内血栓形成情况相关。
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