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Enhancing the Anticancer Efficacy of Immunotherapy through Combination with Histone Modification Inhibitors

机译:通过结合组蛋白修饰抑制剂增强免疫疗法的抗癌功效

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In the nucleus of each cell, the DNA is wrapped around histone octamers, forming the so-called “nucleosomal core particles”. The histones undergo various modifications that influence chromatin structure and function, including methylation, acetylation, ubiquitination, phosphorylation, and SUMOylation. These modifications, known as epigenetic modifications (defined as heritable molecular determinants of phenotype that are independent of the DNA sequence), result in alterations of gene expression and changes in cell behavior. Recent work has shown that epigenetic drugs targeting histone deacetylation or methylation modulate the immune response and overcome acquired resistance to immunotherapy. A number of combination therapies involving immunotherapy and epigenetic drugs, which target histone deacetylation or methylation, are currently under various clinical/pre-clinical investigations and have shown promising anticancer efficacy. These combination therapies may provide a new strategy for achieving sustained anticancer efficacy and overcoming resistance.
机译:在每个细胞的细胞核中,DNA被包裹在组蛋白八聚体周围,形成了所谓的“核小体核心颗粒”。组蛋白经历各种影响染色质结构和功能的修饰,包括甲基化,乙酰化,泛素化,磷酸化和SUMO酰化。这些修饰被称为表观遗传修饰(定义为表型的可遗传分子决定簇,独立于DNA序列),导致基因表达改变和细胞行为改变。最近的工作表明,靶向组蛋白去乙酰化或甲基化的表观遗传药物可调节免疫反应并克服对免疫疗法的后天抵抗力。针对组蛋白脱乙酰基化或甲基化的涉及免疫疗法和表观遗传学药物的多种组合疗法目前正在各种临床/临床前研究中,并且已经显示出有希望的抗癌功效。这些联合疗法可为实现持续的抗癌功效和克服耐药性提供新的策略。

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