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髓细胞中 l-瓜氨酸合成 l-精氨酸有助于宿主抵抗分枝杆菌的体内防御。

l-Arginine Synthesis from l-Citrulline in Myeloid Cells Drives Host Defense against Mycobacteria In Vivo.

机构信息

Department of Pediatrics, University of Cincinnati College of Medicine, Cincinnati, OH 45229.

Division of Infectious Diseases, Cincinnati Children's Hospital Medical Center, Cincinnati, OH 45229.

出版信息

J Immunol. 2019 Mar 15;202(6):1747-1754. doi: 10.4049/jimmunol.1801569. Epub 2019 Feb 1.

Abstract

Immunonutrition as a therapeutic approach is rapidly gaining interest in the fight against infection. Targeting l-arginine metabolism is intriguing, considering this amino acid is the substrate for antimicrobial NO production by macrophages. The importance of l-arginine during infection is supported by the finding that inhibiting its synthesis from its precursor l-citrulline blunts host defense. During the first few weeks following pulmonary mycobacterial infection, we found a drastic increase in l-citrulline in the lung, even though serum concentrations were unaltered. This correlated with increased gene expression of the l-citrulline-generating (i.e., iNOS) and l-citrulline-using (i.e., Ass1) enzymes in key myeloid populations. Eliminating l-arginine synthesis from l-citrulline in myeloid cells via conditional deletion of either or resulted in increased bacillus Calmette-Guérin and HR burden in the lungs compared with controls. Our data illustrate the necessity of l-citrulline metabolism for myeloid defense against mycobacterial infection and highlight the potential for host-directed therapy against mycobacterial disease targeting this nutrient and/or its metabolic pathway.

摘要

免疫营养作为一种治疗方法,在抗感染方面迅速引起关注。针对精氨酸代谢的研究很有吸引力,因为这种氨基酸是巨噬细胞产生抗菌性一氧化氮(NO)的底物。在感染期间,精氨酸的重要性得到了支持,因为发现抑制其前体 l-瓜氨酸的合成会削弱宿主防御。在肺部分枝杆菌感染后的最初几周内,我们发现肺中的 l-瓜氨酸急剧增加,尽管血清浓度没有改变。这与关键髓样细胞中 l-瓜氨酸生成(即 iNOS)和 l-瓜氨酸利用(即 Ass1)酶的基因表达增加相关。通过条件性缺失 或 从 l-瓜氨酸中消除髓样细胞中的精氨酸合成,与对照组相比,导致肺部卡介苗和 HR 负担增加。我们的数据说明了 l-瓜氨酸代谢对于髓样细胞防御分枝杆菌感染的必要性,并强调了针对分枝杆菌疾病的宿主定向治疗的潜力,该治疗方法可以针对这种营养素及其代谢途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f8f5/6401247/82de885600e8/nihms-1518112-f0001.jpg

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