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体液免疫、炎症与癌症。

Humoral immunity, inflammation and cancer.

作者信息

Tan Ting-Ting, Coussens Lisa M

机构信息

Department of Pathology, University of California, San Francisco 2340 Sutter St, San Francisco, CA 94143, USA.

出版信息

Curr Opin Immunol. 2007 Apr;19(2):209-16. doi: 10.1016/j.coi.2007.01.001. Epub 2007 Feb 2.

Abstract

Clinical and experimental data now clearly indicate that chronic inflammation significantly contributes to cancer development. Emerging out of these studies is an appreciation that persistent humoral immune responses exacerbate recruitment and activation of innate immune cells in neoplastic microenvironments where they regulate tissue remodeling, pro-angiogenic and pro-survival pathways that together potentiate cancer development. Population-based studies examining individuals with chronic inflammatory disorders have revealed that states of suppressed cellular immunity, in combination with enhanced humoral immunity and humoral immunity-associated cytokines, cooperate and effectively suppress anti-tumor immune responses while simultaneously enhancing angiogenesis and presumably overall cancer risk in afflicted tissue. In addition, studies in transgenic mouse models of de novo organ-specific cancer development have revealed that inflammation mediated by immunoglobulins and immune complexes might be functionally significant parameters of tumor promotion and progression. These recent advances support the hypothesis that enhanced states of local humoral and innate immune activation, in combination with suppressed cellular immunity and failed cytotoxic T cell anti-tumor immunity, alter cancer risk and therefore represent powerful targets for anti-cancer immunotherapeutics.

摘要

临床和实验数据现已清楚表明,慢性炎症对癌症发展有显著影响。从这些研究中逐渐认识到,持续性体液免疫反应会加剧肿瘤微环境中固有免疫细胞的募集和激活,在该环境中,这些固有免疫细胞调节组织重塑、促血管生成和促生存途径,共同促进癌症发展。对患有慢性炎症性疾病个体的基于人群的研究表明,细胞免疫抑制状态与增强的体液免疫及体液免疫相关细胞因子相结合,协同并有效抑制抗肿瘤免疫反应,同时增强血管生成,可能还会增加患病组织的总体癌症风险。此外,对原发性器官特异性癌症发展的转基因小鼠模型的研究表明,由免疫球蛋白和免疫复合物介导的炎症可能是肿瘤促进和进展的功能重要参数。这些最新进展支持这样一种假说,即局部体液和固有免疫激活增强状态,与细胞免疫抑制和细胞毒性T细胞抗肿瘤免疫功能缺失相结合,会改变癌症风险,因此是抗癌免疫治疗的有力靶点。

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