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Role of the microenvironment across histological subtypes of NHL

机译:微环境在NHL组织学亚型中的作用

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摘要

Recent progress in next-generation sequencing strategies has revealed the genetic landscape of B-cell non-Hodgkin lymphoma, but the tumor microenvironment is increasingly recognized as crucial to sustaining malignant B-cell survival and growth, subclonal evolution, and drug resistance. The tumor niche is made up of a dynamic and organized network of strongly heterogeneous immune and stromal cell subsets characterized by specific phenotypic, transcriptomic, and functional features. Nonmalignant cell recruitment and plasticity are dictated by lymphoma B cells, which convert their surrounding microenvironment into a supportive niche. In addition, they are also influenced by the crosstalk between the various components of this niche. In agreement with this, the B-cell lymphoma subtype is a key determinant of the organization of the tumor niche, but genetic alteration patterns, tumor localization, stage of the disease, and treatment strategy may also modulate its composition and activity. Moreover, the complex set of bidirectional interactions between B cells and their microenvironment has been proposed as a promising therapeutic target with the aim of reinforcing antitumor immunity and/or of abbrogating the lymphoma-promoting signals delivered by the tumor niche.
机译:下一代测序策略的最新进展已经揭示了B细胞非霍奇金淋巴瘤的遗传格局,但人们日益认识到肿瘤微环境对于维持恶性B细胞存活和生长,亚克隆进化以及耐药性至关重要。肿瘤位是由动态和有组织的网络组成的,网络由高度异质的免疫和基质细胞亚群组成,其特征是特定的表型,转录组和功能特征。非恶性细胞募集和可塑性是由淋巴瘤B细胞决定的,后者将其周围的微环境转化为支持位。此外,它们还受到该细分市场各个组件之间的串扰的影响。与此相符的是,B细胞淋巴瘤亚型是决定肿瘤生态位的关键因素,但是遗传改变模式,肿瘤定位,疾病阶段和治疗策略也可能会调节其组成和活性。此外,已经提出了B细胞与其微环境之间复杂的双向相互作用的集合作为有希望的治疗靶标,目的是增强抗肿瘤免疫力和/或减轻由肿瘤位点传递的促进淋巴瘤的信号。

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