Macrophage LRRK2 hyperactivity impairs autophagy and induces Paneth cell dysfunction

IF 17.6 1区 医学 Q1 IMMUNOLOGY
Shengxiang Sun, Miki Hodel, Xiang Wang, Javier De Vicente, Talin Haritunians, Anketse Debebe, Chen-Ting Hung, Changqing Ma, Atika Malique, Hoang N. Nguyen, Maayan Agam, Michael T. Maloney, Marisa S. Goo, Jillian H. Kluss, Richa Mishra, Jennifer Frein, Amanda Foster, Samuel Ballentine, Uday Pandey, Justin Kern, Shaohong Yang, Emebet Mengesha, Iyshwarya Balasubramanian, Annie Arguello, Anthony A. Estrada, Nan Gao, Inga Peter, Dermot P. B. McGovern, Anastasia G. Henry, Thaddeus S. Stappenbeck, Ta-Chiang Liu
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引用次数: 0

Abstract

LRRK2 polymorphisms (G2019S/N2081D) that increase susceptibility to Parkinson’s disease and Crohn’s disease (CD) lead to LRRK2 kinase hyperactivity and suppress autophagy. This connection suggests that LRRK2 kinase inhibition, a therapeutic strategy being explored for Parkinson’s disease, may also benefit patients with CD. Paneth cell homeostasis is tightly regulated by autophagy, and their dysfunction is a precursor to gut inflammation in CD. Here, we found that patients with CD and mice carrying hyperactive LRRK2 polymorphisms developed Paneth cell dysfunction. We also found that LRRK2 kinase can be activated in the context of interactions between genes (genetic autophagy deficiency) and the environment (cigarette smoking). Unexpectedly, lamina propria immune cells were the main intestinal cell types that express LRRK2, instead of Paneth cells as previously suggested. We showed that LRRK2-mediated pro-inflammatory cytokine release from phagocytes impaired Paneth cell function, which was rescued by LRRK2 kinase inhibition through activation of autophagy. Together, these data suggest that LRRK2 kinase inhibitors maintain Paneth cell homeostasis by restoring autophagy and may represent a therapeutic strategy for CD.
巨噬细胞 LRRK2 活性亢进会损害自噬作用并诱发潘氏细胞功能障碍
LRRK2 多态性(G2019S/N2081D)会增加帕金森病和克罗恩病(CD)的易感性,导致 LRRK2 激酶亢进并抑制自噬。这种联系表明,LRRK2 激酶抑制这种正在探索的帕金森病治疗策略也可能有益于克罗恩病患者。Paneth细胞的平衡受到自噬的严格调控,它们的功能障碍是CD患者肠道炎症的前兆。在这里,我们发现 CD 患者和携带高活性 LRRK2 多态性的小鼠会出现 Paneth 细胞功能障碍。我们还发现,LRRK2激酶可在基因(遗传性自噬缺陷)和环境(吸烟)相互作用的背景下被激活。意想不到的是,固有层免疫细胞是表达 LRRK2 的主要肠细胞类型,而不是之前认为的 Paneth 细胞。我们发现,吞噬细胞释放的 LRRK2 介导的促炎细胞因子损害了 Paneth 细胞的功能,而 LRRK2 激酶抑制剂通过激活自噬功能可挽救这种损害。这些数据共同表明,LRRK2激酶抑制剂可通过恢复自噬维持Paneth细胞的稳态,可能是CD的一种治疗策略。
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来源期刊
Science Immunology
Science Immunology Immunology and Microbiology-Immunology
CiteScore
32.90
自引率
2.00%
发文量
183
期刊介绍: Science Immunology is a peer-reviewed journal that publishes original research articles in the field of immunology. The journal encourages the submission of research findings from all areas of immunology, including studies on innate and adaptive immunity, immune cell development and differentiation, immunogenomics, systems immunology, structural immunology, antigen presentation, immunometabolism, and mucosal immunology. Additionally, the journal covers research on immune contributions to health and disease, such as host defense, inflammation, cancer immunology, autoimmunity, allergy, transplantation, and immunodeficiency. Science Immunology maintains the same high-quality standard as other journals in the Science family and aims to facilitate understanding of the immune system by showcasing innovative advances in immunology research from all organisms and model systems, including humans.
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