Перспективы применения иммуномодулирующих препаратов и модуляторов цереблон Е3-лигазы в лечении множественной миеломы

Q4 Medicine

Klinicheskaya Onkogematologiya/Clinical Oncohematology Pub Date : 2023-06-09 DOI:10.21320/2500-2139-2023-16-3-229-241

Сергей Вячеславович Семочкин

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Abstract

In recent decades, the progress in multiple myeloma (MM) treatment has been linked to a clearer insight into the biology of this disease and practical application of new pharmaceutical classes, such as immunomodulatory drugs (IMiDs), proteasome inhibitors (PIs), and monoclonal antibodies (MABs). Modern IMiDs (lenalidomide and pomalidomide) are thalidomide derivatives which despite the similarity of chemical structure show only a relative cross-resistance. Lenalidomide is a second-generation immunomodulator with high anti-tumor activity and a favorable safety profile. In 2006, the use of lenalidomide combined with dexamethasone (Rd regimen) was approved by FDA (USA) for the treatment of relapsed/refractory MM, and 9 years later, in 2015, for newly diagnosed MM. During 2015–2019, the treatment of relapsed MM applied the newly developed regimens involving Rd combined with bortezomib (VRd), carfilzomib (KRd), ixazomib (IRd), elotuzumab (ERd), and daratumumab (DRd), the so-called triplets. Pomalidomide is a third-generation drug used in lenalidomide-refractory patients. For patients with relapsed/refractory MM who received at least two therapy lines with lenalidomide and bortezomib, regimens with 3 drugs were introduced which include pomalidomide and dexamethasone combined with elotuzumab (EPd), isatuximab (Isa-Pd), and daratumumab (DPd). In 2010, the molecular target of IMiD action was discovered, that is protein cereblon (CRBN), a component of CRBN E3 ligase enzyme complex. The insight into this mechanism provided the basis for developing a new family of thalidomide derivatives which are now called CRBN E3 ligase modulators (CELMoDs). In phase I/II trials, two drugs belonging to this group (iberdomide and mezigdomide) showed promising activity in MM refractory to three classes of antitumor drugs (IMiDs, PIs, and anti-CD38 MABs). The present review is focused on prospective studies of IMiDs and CELMoDs at different stages of MM treatment.

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免疫调制剂和e3 - ligha脑蛋白调制器治疗多发性骨髓瘤的前景

近几十年来，多发性骨髓瘤(MM)治疗的进展与对这种疾病的生物学更清晰的认识和新药物类别的实际应用有关，如免疫调节药物(IMiDs)、蛋白酶体抑制剂(pi)和单克隆抗体(mab)。现代IMiDs(来那度胺和泊马度胺)是沙利度胺衍生物，尽管化学结构相似，但仅表现出相对的交叉抗性。来那度胺是第二代免疫调节剂，具有较高的抗肿瘤活性和良好的安全性。2006年，来那度胺联合地塞米松(Rd方案)被FDA(美国)批准用于治疗复发/难治性MM, 9年后的2015年，用于治疗新诊断的MM。2015 - 2019年，复发MM的治疗采用了新开发的Rd联合硼替佐米(VRd)、卡非佐米(KRd)、伊沙唑米(IRd)、elotuzumab (ERd)和daratumumab (DRd)的方案，即所谓的三联用药。波马度胺是用于来那度胺难治性患者的第三代药物。对于接受来那度胺和硼替佐米至少两种治疗线的复发/难治性MM患者，引入3种药物的方案，包括泊马度胺和地塞米松联合艾妥珠单抗(EPd)， isatuximab (Isa-Pd)和daratumumab (DPd)。2010年，IMiD作用的分子靶点被发现，即蛋白小脑(CRBN)，是CRBN E3连接酶复合物的组成部分。对这一机制的深入了解为开发新的沙利度胺衍生物家族提供了基础，这些衍生物现在被称为CRBN E3连接酶调节剂(celmod)。在I/II期试验中，该组的两种药物(iberdomide和mezigdomide)在三种抗肿瘤药物(IMiDs, pi和抗cd38单克隆抗体)难治性MM中显示出有希望的活性。目前的综述主要集中在MM治疗不同阶段的IMiDs和celmod的前瞻性研究。

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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