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血红素加氧酶1对抗抗原加工的调节作用及其对炎症和耐受性的影响

Modulation of antigen processing by haem-oxygenase 1. Implications on inflammation and tolerance.

作者信息

Riquelme Sebastián A, Carreño Leandro J, Espinoza Janyra A, Mackern-Oberti Juan Pablo, Alvarez-Lobos Manuel M, Riedel Claudia A, Bueno Susan M, Kalergis Alexis M

机构信息

Millennium Institute of Immunology and Immunotherapy, Departamento de Genética Molecular y Microbiología, Facultad de Ciencias Biológicas, Pontificia Universidad Católica de Chile, Santiago, Chile.

INSERM, UMR 1064, CHU Nantes, ITUN, Nantes, France.

出版信息

Immunology. 2016 Sep;149(1):1-12. doi: 10.1111/imm.12605. Epub 2016 Apr 1.

Abstract

Haem-oxygenase-1 (HO-1) is an enzyme responsible for the degradation of haem that can suppress inflammation, through the production of carbon monoxide (CO). It has been shown in several experimental models that genetic and pharmacological induction of HO-1, as well as non-toxic administration of CO, can reduce inflammatory diseases, such as endotoxic shock, type 1 diabetes and graft rejection. Recently, it was shown that the HO-1/CO system can alter the function of antigen-presenting cells (APCs) and reduce T-cell priming, which can be beneficial during immune-driven inflammatory diseases. The molecular mechanisms by which the HO-1 and CO reduce both APC- and T-cell-driven immunity are just beginning to be elucidated. In this article we discuss recent findings related to the immune regulatory capacity of HO-1 and CO at the level of recognition of pathogen-associated molecular patterns and T-cell priming by APCs. Finally, we propose a possible regulatory role for HO-1 and CO over the recently described mitochondria-dependent immunity. These concepts could contribute to the design of new therapeutic tools for inflammation-based diseases.

摘要

血红素加氧酶-1(HO-1)是一种负责降解血红素的酶,它可通过产生一氧化碳(CO)来抑制炎症。在多个实验模型中已表明,HO-1的基因诱导和药物诱导以及CO的无毒给药均可减轻炎症性疾病,如内毒素休克、1型糖尿病和移植排斥反应。最近有研究表明,HO-1/CO系统可改变抗原呈递细胞(APC)的功能并减少T细胞致敏,这在免疫驱动的炎症性疾病中可能是有益的。HO-1和CO降低APC和T细胞驱动的免疫反应的分子机制才刚刚开始被阐明。在本文中,我们讨论了与HO-1和CO在病原体相关分子模式识别以及APC引发T细胞致敏水平上的免疫调节能力相关的最新研究结果。最后,我们提出了HO-1和CO对最近描述的线粒体依赖性免疫可能具有的调节作用。这些概念可能有助于设计针对炎症性疾病的新治疗工具。

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