完善免疫性血栓性血小板减少性紫癜的治疗标准。

IF 1.1 Q4 ONCOLOGY Clinical Advances in Hematology & Oncology Pub Date : 2024-10-01
Jeffrey Laurence
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引用次数: 0

摘要

急性免疫性血栓性血小板减少性紫癜(iTTP)是一种医疗急症。在出现任何血栓性微血管病(TMA)的情况下,应抽血测量 ADAMTS13 活性和抑制剂水平,并在获得 ADAMTS13 结果之前评估 TTP 风险。这包括使用 PLASMIC 和 French 评分。然后开始进行血浆置换(PE)。一旦确诊为 iTTP,ADAMTS13 低于 10%,且存在抑制剂,则应针对 iTTP 病理生理学的各个方面采取干预措施:通过持续 PE 补充 ADAMTS13;用糖皮质激素和利妥昔单抗抑制抗 ADAMTS13 自身抗体;用卡普珠单抗抑制血栓形成过程--血小板/冯-威廉因子(VWF)微血栓的失控形成。后者是对现有治疗标准的补充,以国际血栓与止血学会指南为基础,强调跟踪 ADAMTS13 的活性。在一项关键的随机对照试验 HERCULES 中,使用卡普拉珠单抗可减少 iTTP 复发次数、减少 PE 并缩短住院时间。在高度怀疑有 iTTP 的情况下,临床医生应考虑在收到 ADAMTS13 结果之前使用卡普珠单抗,因为在确认 TMA 后 3 天内开始使用卡普珠单抗可获得最大益处。在 HERCULES 中,卡普拉珠单抗组有 11% 的患者发生了严重出血事件,而安慰剂组仅有 1%,但所有出血事件都得到了缓解,其中大部分无需干预。用卡普拉珠单抗快速预防 VWF 多聚体/血小板形成是否能抑制此类长期后遗症,以及卡普拉珠单抗是否能取代 PE 作为初始治疗,这些问题都在研究之中。
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Refining the standard of care in immune thrombotic thrombocytopenic purpura.

Acute immune thrombotic thrombocytopenic purpura (iTTP) is a medical emergency. In the setting of any thrombotic microangiopathy (TMA), blood should be drawn to measure ADAMTS13 activity and inhibitor levels, and an assessment should be made of TTP risk before receiving ADAMTS13 results. This can include the use of PLASMIC and French scores. Plasma exchange (PE) is then initiated. Upon confirmation of iTTP, with ADAMTS13 less than 10% in the presence of an inhibitor, interventions targeting all facets of iTTP pathophysiology should be instituted: replenishing ADAMTS13 via continued PE; suppressing anti-ADAMTS13 autoantibodies with glucocorticoids and rituximab; and inhibiting the thrombotic process-uncontrolled formation of platelet/Von Willebrand factor (VWF) microthrombi-with caplacizumab. The latter, an addition to existing standards of care, is based on International Society on Thrombosis and Haemostasis guidelines and emphasizes tracking of ADAMTS13 activity. In HERCULES, a pivotal randomized controlled trial, caplacizumab use resulted in fewer recurrent iTTP episodes, decreased PE, and shortened hospital stay. In settings of high suspicion for iTTP, clinicians should consider the administration of caplacizumab before receiving ADAMTS13 results because the greatest benefits of caplacizumab accrued starting it within 3 days of TMA recognition. In HERCULES, serious bleeding events occurred among 11% of those in the caplacizumab group vs 1% in the placebo group, but all resolved, most without intervention. iTTP survivors receiving PE and immunosuppression alone are at a heightened risk for stroke, other cardiovascular disorders, neurocognitive impairment, and kidney disease. Whether rapid prevention of VWF multimer/platelet formation with caplacizumab can suppress such long-term sequelae, and whether caplacizumab can replace PE in initial therapy, are under investigation.

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来源期刊
CiteScore
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期刊介绍: Clinical Advances in Hematology & Oncology (CAH&O) is a monthly peer-reviewed journal reaching more than 27,000 hematology and oncology clinicians. CAH&O provides editorial content encompassing a wide array of topics relevant and useful to the fields of oncology and hematology, both separately and together. Content is directed by the strong input of today’s top thought leaders in hematology & oncology, including feature-length review articles, monthly columns consisting of engaging interviews with experts on current issues in solid tumor oncology, hematologic malignancies, hematologic disorders, drug development, and clinical case studies with expert commentary. CAH&O also publishes industry-supported meeting highlights, clinical roundtable monographs, and clinical review supplements.
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