Bayer A S, Sullam P M, Ramos M, Li C, Cheung A L, Yeaman M R
Division of Adult Infectious Diseases, Harbor-UCLA Medical Center, Torrance 90509, USA.
Infect Immun. 1995 Sep;63(9):3634-41. doi: 10.1128/iai.63.9.3634-3641.1995.
Platelet aggregation by bacteria is felt to play an important role in the pathogenesis of infective endocarditis. However, the mechanisms involved in bacterium-induced platelet aggregation are not well-defined. In the present study, we examined the mechanisms by which Staphylococcus aureus causes rabbit platelet aggregation in vitro. In normal plasma, the kinetics of S. aureus-induced platelet aggregation were rapid and biphasic. The onset and magnitude of aggregation phase 1 varied with the bacterium-platelet ratio, with maximal aggregation observed at a ratio of 5:1. The onset of aggregation phase 2 was delayed in the presence of apyrase (an ADP hydrolase), suggesting that this later aggregation phase may be triggered by secreted ADP. The onset of aggregation phase 2 was delayed in the presence of prostaglandin I2-treated platelets, and this phase was absent when paraformaldehyde-fixed platelets were used, implicating platelet activation in this process. Platelet aggregation phase 2 was dependent on S. aureus viability and an intact bacterial cell wall, and it was mitigated by antibody directed against staphylococcal clumping factor (a fibrinogen-binding protein) and by the cyclooxygenase inhibitor indomethacin. Similarly, aggregation phase 2 was either delayed or absent in three distinct transposon-induced S. aureus mutants with reduced capacities to bind fibrinogen in vitro. In addition, a synthetic pentadecapeptide, corresponding to the staphylococcal binding domain in the C terminus of the fibrinogen delta-chain, blocked aggregation phase 2. However, phase 2 of aggregation was not inhibited by two synthetic peptides (alone or in combination) analogous to the two principal fibrinogen-binding domains on the platelet glycoprotein (GP) IIb/IIIa integrin receptor: (i) a recognition site on the IIIa molecule for the Arg-Gly-Asp (RGD) sequence of the fibrinogen alpha-chain and (ii) a recognition site on the IIb molecule for a dodecapeptide sequence of the fibrinogen delta-chain. This differs from ADP-induced platelet aggregation, which relies on an intact platelet GP IIb/IIIa receptor with an accessible RGD sequence and dodecapeptide recognition site for fibrinogen. Furthermore, a monoclonal antibody directed against the RGD recognition site on rabbit platelet GP IIb/IIIa receptors failed to inhibit rabbit platelet aggregation by S. aureus. Collectively, these data suggest that S. aureus-induced platelet aggregation requires bacterial binding to fibrinogen but is not principally dependent upon the two major fibrinogen-binding domains on the platelet GP IIb/IIIa integrin receptor, the RGD and dodecapeptide recognition sites.
细菌诱导的血小板聚集被认为在感染性心内膜炎的发病机制中起重要作用。然而,细菌诱导血小板聚集的机制尚未明确。在本研究中,我们检测了金黄色葡萄球菌在体外引起兔血小板聚集的机制。在正常血浆中,金黄色葡萄球菌诱导的血小板聚集动力学快速且呈双相性。聚集第一阶段的起始和程度随细菌与血小板的比例而变化,在比例为5:1时观察到最大聚集。在存在腺苷三磷酸双磷酸酶(一种ADP水解酶)的情况下,聚集第二阶段的起始延迟,这表明该后期聚集阶段可能由分泌的ADP触发。在用前列腺素I2处理的血小板存在时,聚集第二阶段的起始延迟,而当使用多聚甲醛固定的血小板时,该阶段不存在,这表明血小板活化参与了这一过程。血小板聚集第二阶段依赖于金黄色葡萄球菌的活力和完整的细菌细胞壁,并且可被针对葡萄球菌聚集因子(一种纤维蛋白原结合蛋白)的抗体和环氧化酶抑制剂吲哚美辛所减轻。同样,在三种不同的转座子诱导的体外结合纤维蛋白原能力降低的金黄色葡萄球菌突变体中,聚集第二阶段要么延迟要么不存在。此外,一种与纤维蛋白原δ链C末端的葡萄球菌结合结构域相对应的合成十五肽可阻断聚集第二阶段。然而,聚集的第二阶段未被两种类似于血小板糖蛋白(GP)IIb/IIIa整合素受体上两个主要纤维蛋白原结合结构域的合成肽(单独或联合使用)所抑制:(i)IIIa分子上针对纤维蛋白原α链的精氨酸 - 甘氨酸 - 天冬氨酸(RGD)序列的识别位点,以及(ii)IIb分子上针对纤维蛋白原δ链十二肽序列的识别位点。这与ADP诱导的血小板聚集不同,后者依赖于具有可及的RGD序列和纤维蛋白原十二肽识别位点的完整血小板GP IIb/IIIa受体。此外,一种针对兔血小板GP IIb/IIIa受体上RGD识别位点的单克隆抗体未能抑制金黄色葡萄球菌诱导的兔血小板聚集。总体而言,这些数据表明金黄色葡萄球菌诱导的血小板聚集需要细菌与纤维蛋白原结合,但主要不依赖于血小板GP IIb/IIIa整合素受体上的两个主要纤维蛋白原结合结构域,即RGD和十二肽识别位点。
