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Primary refractory and early-relapsed Hodgkin's lymphoma: strategies for therapeutic targeting based on the tumour microenvironment

机译:原发性难治性和早发性霍奇金淋巴瘤:基于肿瘤微环境的靶向治疗策略

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摘要

Classical Hodgkin's lymphoma (cHL), a distinct disease entity with characteristic clinical and pathological features, accounts for approximately 10% of all malignant lymphomas. cHL can be considered a prototype model for how the tumour microenvironment influences cancer pathogenesis. Cellular components of the cHL microenvironment express molecules involved in cancer cell growth and survival, such as CD30L or CD40L. Moreover, several signal transduction pathways that are critical for the proliferation and survival of neoplastic Hodgkin Reed-Sternberg (HRS) cells, including NF-B, JAK-STAT, PI3K-AkT and ERK, are deregulated in cHL. Although most patients can be cured with modern treatment strategies, approximately a quarter experience either primary or secondary chemorefractoriness or disease relapse, thus requiring novel treatments. Preclinical and clinical evidence has elucidated a complex crosstalk between malignant HRS cells and the reactive cells of the microenvironment, which suggests that novel therapeutic approaches capable of targeting HRS cells along with reactive cells might overcome chemorefractoriness. In the near future, these novel therapies will also be tested in chemosensitive patients, to reduce the long-term toxicity of chemo-radiotherapy. Copyright (c) 2015 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd.
机译:古典霍奇金淋巴瘤(cHL)是具有特征性临床和病理特征的独特疾病实体,约占所有恶性淋巴瘤的10%。 cHL可被视为肿瘤微环境如何影响癌症发病机制的原型模型。 cHL微环境的细胞成分表达参与癌细胞生长和存活的分子,例如CD30L或CD40L。此外,在cHL中,对于肿瘤性霍奇金·里德-斯特恩伯格(HRS)细胞的增殖和存活至关重要的几种信号转导途径,包括NF-B,JAK-STAT,PI3K-AkT和ERK,都被解除了调控。尽管大多数患者可以通过现代治疗方法治愈,但大约四分之一的患者经历了原发性或继发性化学性难治性或疾病复发,因此需要新颖的治疗方法。临床前和临床证据阐明了恶性HRS细胞与微环境的反应性细胞之间的复杂串扰,这表明能够将HRS细胞与反应性细胞一起靶向的新型治疗方法可能克服了化学断裂性。在不久的将来,这些新疗法还将在化学敏感性患者中进行测试,以减少化学放射疗法的长期毒性。版权所有(c)2015英国和爱尔兰病理学会。由John Wiley&Sons,Ltd.出版

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