The immunology of PF4 polyanion interactions.

IF 3.1 3区 医学 Q2 HEMATOLOGY Current Opinion in Hematology Pub Date : 2023-11-01 Epub Date: 2023-08-28 DOI:10.1097/MOH.0000000000000782
Anh T P Ngo, Veronica Bochenek, Kandace Gollomp
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Abstract

Purpose of review: Platelet factor 4 (PF4, CXCL4), the most abundant α-granule platelet-specific chemokine, forms tetramers with an equatorial ring of high positive charge that bind to a wide range of polyanions, after which it changes conformation to expose antigenic epitopes. Antibodies directed against PF4 not only help to clear infection but can also lead to the development of thrombotic disorders such as heparin-induced thrombocytopenia (HIT) and vaccine-induced thrombocytopenia and thrombosis (VITT). This review will outline the different mechanisms through which PF4 engagement with polyanions combats infection but also contributes to the pathogenesis of inflammatory and thrombotic disease states.

Recent findings: Recent work has shown that PF4 binding to microbial polyanions may improve outcomes in infection by enhancing leukocyte-bacterial binding, tethering pathogens to neutrophil extracellular traps (NETs), decreasing the thrombotic potential of NET DNA, and modulating viral infectivity. However, PF4 binding to nucleic acids may enhance their recognition by innate immune receptors, leading to autoinflammation. Lastly, while HIT is induced by platelet activating antibodies that bind to PF4/polyanion complexes, VITT, which occurs in a small subset of patients treated with COVID-19 adenovirus vector vaccines, is characterized by prothrombotic antibodies that bind to PF4 alone.

Summary: Investigating the complex interplay of PF4 and polyanions may provide insights relevant to the treatment of infectious disease while also improving our understanding of the pathogenesis of thrombotic disorders driven by anti-PF4/polyanion and anti-PF4 antibodies.

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PF4多阴离子相互作用的免疫学。
综述目的:血小板因子4(PF4,CXCL4)是最丰富的α-颗粒血小板特异性趋化因子,形成具有高正电荷赤道环的四聚体,与多种聚阴离子结合,然后改变构象以暴露抗原表位。针对PF4的抗体不仅有助于清除感染,还可能导致血栓性疾病的发展,如肝素诱导的血小板减少症(HIT)和疫苗诱导的血小板降低症和血栓形成症(VITT)。这篇综述将概述PF4与聚阴离子结合对抗感染的不同机制,但也有助于炎症和血栓性疾病状态的发病机制。最近的发现:最近的研究表明,PF4与微生物聚阴离子的结合可以通过增强白细胞与细菌的结合、将病原体与中性粒细胞外陷阱(NETs)结合、降低NETDNA的血栓形成潜力和调节病毒感染性来改善感染的结果。然而,PF4与核酸的结合可能会增强其被先天免疫受体的识别,从而导致自身炎症。最后,虽然HIT是由与PF4/聚阴离子复合物结合的血小板活化抗体诱导的,但发生在一小部分接受新冠肺炎腺病毒载体疫苗治疗的患者中的VITT的特征是仅与PF4结合的血栓前抗体。综述:研究PF4和聚阴离子的复杂相互作用可以提供与传染病治疗相关的见解,同时也可以提高我们对由抗PF4/聚阴离子和抗PF4抗体驱动的血栓性疾病的发病机制的理解。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
6.60
自引率
3.10%
发文量
78
审稿时长
6-12 weeks
期刊介绍: ​​​​​​​​Current Opinion in Hematology is an easy-to-digest bimonthly journal covering the most interesting and important advances in the field of hematology. Its hand-picked selection of editors ensure the highest quality selection of unbiased review articles on themes from nine key subject areas, including myeloid biology, Vascular biology, hematopoiesis and erythroid system and its diseases.
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