Venetoclax:急性髓系白血病和骨髓增生异常综合征新治疗时代的新伙伴。

Jean El-Cheikh, Ghassan Bidaoui, Mustafa Saleh, Nour Moukalled, Iman Abou Dalle, Ali Bazarbachi
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引用次数: 5

摘要

背景:急性髓系白血病(AML)和骨髓增生异常综合征(MDS)是两种密切相关的血癌,常见于老年人。AML是成人急性白血病中最常见的类型,MDS的特点是血细胞生成无效,骨髓和血液异常。两者均可耐药,往往是由于细胞凋亡过程中的功能障碍,这是机体细胞死亡的自然机制。Venetoclax是一种选择性靶向BCL-2蛋白的口服药物,有望通过降低细胞凋亡阈值来提高某些血液系统恶性肿瘤的治疗敏感性。本综述旨在评价venetoclax治疗AML和MDS的有效性,以及对该药物的潜在耐药机制。方法:利用PUBMED进行文献检索,获取所有使用venetoclax治疗这两种疾病的相关研究文章。检索MeSH词条“急性髓系白血病”、“骨髓增生异常综合征”和“venetoclax”。此外,还访问了Clinicaltrials.gov,以确保纳入所有正在进行的临床试验。结果:尽管Venetoclax作为单药治疗AML的效果一般,但基于Venetoclax的联合治疗?主要是低甲基化药物还是低剂量阿糖胞苷?取得了显著的积极效果。以维托克拉西为基础联合HMA(主要是阿扎胞苷)治疗不适合高危MDS也取得了乐观的结果。各种药物已被批准的突变鉴定促使了对venetoclax联合试验的积极研究。结论:基于venetoclax的联合治疗在不适合强化化疗的AML患者中可诱导快速反应并提高总生存率。这些疗法在高风险MDS患者的I期试验中也取得了积极的初步结果。对venetoclax的耐药性和药物相关毒性是需要克服的两个主要障碍,以获得该疗法的全部益处。
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Venetoclax: A New Partner in the Novel Treatment Era for Acute Myeloid Leukemia and Myelodysplastic Syndrome.

Background: Acute Myeloid Leukemia (AML) and Myelodysplastic Syndrome (MDS) are two closely related blood cancers that are more frequent in older adults. AML is the most common type of adult acute leukemia, and MDS is characterized by ineffective blood cell production and abnormalities in the bone marrow and blood. Both can be resistant to treatment, often due to dysfunction in the process of apoptosis, the body's natural mechanism for cell death. Venetoclax, an orally-administered medication that selectively targets the BCL-2 protein, has shown promise in enhancing treatment sensitivity in some hematological malignancies by reducing the apoptotic threshold. This review aims to evaluate the effectiveness of venetoclax in treating AML and MDS, as well as potential mechanisms of resistance to the medication.

Methods: A literature search was conducted utilizing PUBMED to capture all relevant research articles on the use of venetoclax as a therapy for both diseases. The MeSH terms "acute myeloid leukemia", "myelodysplastic syndrome" and "venetoclax" were searched. Furthermore, Clinicaltrials.gov was accessed to ensure the inclusion of all ongoing clinical trials.

Results: Although Venetoclax showed modest results as a single-agent therapy in AML, venetoclax-based combination therapies? mainly with hypomethylating agents or low-dose cytarabine? yielded significantly positive results. Preliminary results oN the use of venetoclax-based combination therapy with HMA, mainly azacitidine, in unfit high-risk MDS also yielded optimistic results. Identification of mutations for which various drugs have been approved has spurred active investigation of venetoclax in combination trials.

Conclusion: Venetoclax-based combination therapies have been shown to induce rapid responses and increase overall survival in AML patients unfit for intensive chemotherapy. These therapies are also yielding positive preliminary results in high-risk MDS patients in phase I trials. Resistance to venetoclax and drug-related toxicity are two main obstacles that need to be overcome to reap the full benefits of this therapy.

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