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癌症预后和治疗中的免疫结构。

The immune contexture in cancer prognosis and treatment.

机构信息

Cancer, Immune Control and Escape Team, INSERM UMRS 1138, Cordeliers Research Centre.

Paris Descartes University (Paris 5), Sorbonne Paris Cité, INSERM UMRS 1138, Cordeliers Research Centre.

出版信息

Nat Rev Clin Oncol. 2017 Dec;14(12):717-734. doi: 10.1038/nrclinonc.2017.101. Epub 2017 Jul 25.


DOI:10.1038/nrclinonc.2017.101
PMID:28741618
Abstract

Immunotherapy is currently the most rapidly advancing area of clinical oncology, and provides the unprecedented opportunity to effectively treat, and even cure, several previously untreatable malignancies. A growing awareness exists of the fact that the success of chemotherapy and radiotherapy, in which the patient's disease can be stabilized well beyond discontinuation of treatment (and occasionally is cured), also relies on the induction of a durable anticancer immune response. Indeed, the local immune infiltrate undergoes dynamic changes that accompany a shift from a pre-existing immune response to a therapy-induced immune response. As a result, the immune contexture, which is determined by the density, composition, functional state and organization of the leukocyte infiltrate of the tumour, can yield information that is relevant to prognosis, prediction of a treatment response and various other pharmacodynamic parameters. Several complementary technologies can be used to explore the immune contexture of tumours, and to derive biomarkers that could enable the adaptation of individual treatment approaches for each patient, as well as monitoring a response to anticancer therapies.

摘要

免疫疗法目前是临床肿瘤学中发展最快的领域,为有效治疗甚至治愈几种以前无法治疗的恶性肿瘤提供了前所未有的机会。人们越来越意识到,化疗和放疗的成功也依赖于诱导持久的抗癌免疫反应,在这些治疗中,患者的疾病可以在治疗停止后(偶尔甚至可以治愈)得到很好的稳定。事实上,局部免疫浸润发生动态变化,伴随着从预先存在的免疫反应向治疗诱导的免疫反应的转变。因此,由肿瘤白细胞浸润的密度、组成、功能状态和组织决定的免疫结构可以提供与预后、治疗反应预测和各种其他药效学参数相关的信息。可以使用几种互补的技术来探索肿瘤的免疫结构,并从中提取出生物标志物,使我们能够根据每个患者的情况调整治疗方法,并监测对癌症治疗的反应。

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本文引用的文献

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Science. 2017-1-20

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Immune Toxicities Elicted by CTLA-4 Blockade in Cancer Patients Are Associated with Early Diversification of the T-cell Repertoire.

Cancer Res. 2017-3-15

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