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白血病中的重排:分子方面和治疗前景。

Rearrangements in Leukemias: Molecular Aspects and Therapeutic Perspectives.

机构信息

Department of Translational Hematology & Oncology Research, Taussig Cancer Institute, Cleveland Clinic, Cleveland, OH 44114, USA.

Department of Biomedicine and Prevention, Tor Vergata University of Rome, 00133 Rome, Italy.

出版信息

Int J Mol Sci. 2024 Aug 20;25(16):9023. doi: 10.3390/ijms25169023.

Abstract

(alias: mixed-lineage leukemia []) gene mapping on chromosome 11q23 encodes the lysine-specific histone N-methyltransferase 2A and promotes transcription by inducing an open chromatin conformation. Numerous genomic breakpoints within the gene have been reported in young children and adults with hematologic disorders and are present in up to 10% of acute leukemias. These rearrangements describe distinct features and worse prognosis depending on the fusion partner, characterized by chemotherapy resistance and high rates of relapse, with a progression-free survival of 30-40% and overall survival below 25%. Less intensive regimens are used in pediatric patients, while new combination therapies and targeted immunotherapeutic agents are being explored in adults. Beneficial therapeutic effects, and even cure, can be reached with hematopoietic stem cell transplantation, mainly in young children with dismal molecular lesions; however, delayed related toxicities represent a concern. Herein, we summarize the translocation partner genes and partial tandem duplications of the gene, their molecular impact, clinical aspects, and novel targeted therapies.

摘要

(别名:混合谱系白血病[])基因定位于染色体 11q23,编码赖氨酸特异性组蛋白 N-甲基转移酶 2A,并通过诱导开放染色质构象促进转录。在患有血液系统疾病的幼儿和成人中,已报道了该基因内的许多基因组断裂点,并且在高达 10%的急性白血病中存在。这些重排根据融合伙伴具有不同的特征和更差的预后,表现为化疗耐药和高复发率,无进展生存率为 30-40%,总生存率低于 25%。在儿科患者中使用了不太密集的方案,而新的联合治疗和靶向免疫治疗药物正在成人中进行探索。造血干细胞移植可以达到有益的治疗效果,甚至治愈,主要适用于分子病变不良的幼儿;然而,延迟的相关毒性是一个问题。在此,我们总结了 基因的易位伙伴基因和部分串联重复,及其分子影响、临床方面和新的靶向治疗。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3b06/11354696/7afcb3d06b5a/ijms-25-09023-g001.jpg

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