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抗磷脂综合征中血栓形成、妊娠并发症或死亡的风险

Risk of Thrombosis, Pregnancy Morbidity or Death in Antiphospholipid Syndrome.

作者信息

Killian Martin, van Mens Thijs E

机构信息

CIRI - Centre International de Recherche en Infectiologie, Team GIMAP, Université de Lyon, Université Jean Monnet, Université Claude Bernard Lyon 1, Inserm, U1111, CNRS, UMR530, Saint-Étienne, France.

Internal Medicine Department, Saint-Etienne University Hospital, Saint-Étienne, France.

出版信息

Front Cardiovasc Med. 2022 Mar 1;9:852777. doi: 10.3389/fcvm.2022.852777. eCollection 2022.

Abstract

The antiphospholipid syndrome is an autoimmune disease characterized by thrombosis and pregnancy morbidity. The manifestations are caused by antibodies targeting cell membrane phospholipids and/or associated proteins. The triggers leading to these antibodies' production are unknown but recent work suggests cross-reactivity between the autoantigens and peptides produced by the intestinal microbiome. Work on how the autoantibodies could cause clinical manifestations implicates different mechanisms. Binding to surface proteins of different cell types can induce intracellular signaling leading to cell activation and tissue factor expression. Complement activation and neutrophil extracellular-traps are also involved, and recent evidence implicates endothelial protein C receptor-lysobisphosphatidic acid complex. Pregnancy is a high-risk situation for antiphospholipid syndrome patients due to the increased risk of thrombosis and obstetric complications. Epidemiological and clinical research on APS is hampered by heterogeneity in populations, testing and treatment strategies. About one in 10 to one in fifty APS pregnancies is complicated by thrombosis, despite treatment. Pregnant patients with prior thrombosis are prescribed therapeutic dose heparins and low dose aspirin. Without prior thrombosis a prophylactic dose is used. The most frequent obstetrical manifestation is recurrent early pregnancy loss. The association of APS antibodies with late pregnancy loss is stronger, however. Prevention of recurrence is achieved with aspirin and prophylactic dose heparin, although the evidence is of low certainty. The third obstetrical classifying manifestation comprises preterm delivery due to placenta-mediated complications and is treated in subsequent pregnancies with aspirin with or without prophylactic dose heparin, again based on low quality evidence. New therapies are under investigation.

摘要

抗磷脂综合征是一种自身免疫性疾病,其特征为血栓形成和妊娠并发症。这些表现是由靶向细胞膜磷脂和/或相关蛋白的抗体引起的。导致这些抗体产生的触发因素尚不清楚,但最近的研究表明,自身抗原与肠道微生物群产生的肽之间存在交叉反应。关于自身抗体如何导致临床表现涉及不同的机制。与不同细胞类型的表面蛋白结合可诱导细胞内信号传导,导致细胞活化和组织因子表达。补体激活和中性粒细胞胞外陷阱也参与其中,最近的证据表明内皮蛋白C受体 - 溶血双磷脂酸复合物也与之有关。由于血栓形成和产科并发症的风险增加,妊娠对抗磷脂综合征患者来说是一种高风险情况。抗磷脂综合征的流行病学和临床研究受到人群、检测和治疗策略异质性的阻碍。尽管进行了治疗,但每10至50例抗磷脂综合征妊娠中仍有1例并发血栓形成。有血栓形成史的孕妇会被处方治疗剂量的肝素和低剂量阿司匹林。没有血栓形成史则使用预防剂量。最常见的产科表现是反复早期妊娠丢失。然而,抗磷脂综合征抗体与晚期妊娠丢失的关联更强。阿司匹林和预防剂量的肝素可预防复发,尽管证据的确定性较低。第三种产科分类表现包括因胎盘介导的并发症导致的早产,在后续妊娠中根据低质量证据使用阿司匹林加或不加预防剂量的肝素进行治疗。新的治疗方法正在研究中。

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