Carfilzomib-Induced Thrombotic Microangiopathy—Two Case Reports

IF 1.5 Q4 ONCOLOGY Cancer reports Pub Date : 2024-10-10 DOI:10.1002/cnr2.2163

Irene Attucci, Sofia Pilerci, Maria Messeri, Ludovica Pengue, Giulia Tomasino, Leonardo Caroti, Alessandro M. Vannucchi, Elisabetta Antonioli

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Abstract

Background

Thrombotic microangiopathy (TMA) is a pathological syndrome characterized by a combination of three key features: microangiopathic hemolytic anemia (MAHA), thrombocytopenia, and organ damage, primarily affecting the kidneys. There are several drugs known to have a definite or probable causal association with TMA, and carfilzomib, a second-generation irreversible proteasome inhibitor (PI), approved for the treatment of multiple myeloma (MM), is one of them. In the medical literature, there have been a growing number of reports describing this serious adverse event occurring in MM patients. The precise mechanisms underlying the development of PI-induced TMA are not yet fully understood. Significant improvements in both renal and hematological aspects have been documented following the administration of eculizumab.

Recent Findings

In this report, we present two cases of MM patients who developed TMA while undergoing carfilzomib therapy. These cases were successfully treated at the Haematology Unit, Careggi Hospital in Florence. In our cases as well, the introduction of eculizumab resulted in rapid enhancements in renal function and platelet count, ultimately leading to the discontinuation of hemodialysis after 4 and 2 weeks, respectively.

Discussion and Conclusion

We assessed 91 patients who received carfilzomib-based therapies at our Haematology Department, during which we identified two cases of DITMA (2.2% incidence). Additionally, we conducted a literature review and discovered a total of 75 documented cases of carfilzomib-induced TMA. Our experience aligns with the cases reported in literature: this adverse event can manifest at any point during treatment, regardless of the specific drug combinations used alongside carfilzomib. The initial and most crucial step in its management involves discontinuing carfilzomib therapy; therefore, recognizing TMA in a timely manner is of utmost importance. Eculizumab could play a role in improving and expediting the resolution of this potentially fatal adverse event, but further studies are needed.

In a MM patient receiving carfilzomib, presenting with anemia, thrombocytopenia, and impaired renal function, a carfilzomib-induced TMA should be suspected in order to discontinue the causative agent.

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卡非佐米诱发血栓性微血管病--两例报告

背景：血栓性微血管病（TMA）是一种病理综合征，具有三个主要特征：微血管病性溶血性贫血（MAHA）、血小板减少症和器官损伤（主要影响肾脏）。目前已知有几种药物与 TMA 有明确或可能的因果关系，已被批准用于治疗多发性骨髓瘤（MM）的第二代不可逆蛋白酶体抑制剂（PI）卡非佐米（carfilzomib）就是其中之一。在医学文献中，越来越多的报告描述了发生在 MM 患者身上的这种严重不良事件。PI诱发TMA的确切机制尚未完全明了。最近的研究结果表明，使用依库珠单抗后，肾脏和血液学方面均有明显改善：在本报告中，我们介绍了两例在接受卡非佐米治疗期间出现 TMA 的 MM 患者。佛罗伦萨卡雷吉医院血液科成功治疗了这两例患者。在我们的病例中，使用依库珠单抗后，肾功能和血小板计数迅速增加，最终分别在 4 周和 2 周后停止了血液透析：我们对血液科接受卡非佐米治疗的 91 名患者进行了评估，发现了两例 DITMA 病例（发生率为 2.2%）。此外，我们还进行了文献综述，发现共有 75 例卡非佐米诱发 TMA 的记录病例。我们的经验与文献报道的病例一致：无论卡非佐米同时使用哪种特定的药物组合，这种不良事件都可能在治疗过程中的任何阶段出现。治疗的第一步也是最关键的一步是停止卡非佐米治疗；因此，及时发现 TMA 至关重要。Eculizumab 可在改善和加速解决这一潜在致命不良事件方面发挥作用，但仍需进一步研究。接受卡非佐米治疗的 MM 患者出现贫血、血小板减少和肾功能受损时，应怀疑是卡非佐米引起的 TMA，以便停用致病药物。

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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