SIGN-R1, a C-type lectin, enhances apoptotic cell clearance through the complement deposition pathway by interacting with C1q in the spleen

被引:0
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作者
M G Prabagar
Y Do
S Ryu
J-Y Park
H-J Choi
W-S Choi
T J Yun
J Moon
I-S Choi
K Ko
K Ko
C Young Shin
C Cheong
Y-S Kang
机构
[1] SMART Institute of Advanced Biomedical Science,Department of Biomedical Science and Technology
[2] Institute of Functional Genomics,Department of Cardiothoracic Surgery
[3] Konkuk University,Department of Microbiology and Immunology
[4] 1 Hwayang-dong,Department of Infectious Diseases
[5] Gwangjin-gu,Department of Medicine
[6] School of Nano-Bioscience and Chemical Engineering,Department of Stem Cell Biology
[7] Ulsan National Institute of Science and Technology,Department of Pharmacology
[8] #100 Banyeon-ri,undefined
[9] Eonyang-eup,undefined
[10] Ulju-gun,undefined
[11] Weill Cornell Medical College of Cornell University,undefined
[12] Laboratory Animal Center,undefined
[13] Daegu-Gyeongbuk Medical Innovation Foundation (DGMIF),undefined
[14] 2387 Dalgubeol-daero,undefined
[15] Suseong-gu,undefined
[16] Institut de Recherches Cliniques de Montréal (IRCM),undefined
[17] 110 avenue des Pins Ouest,undefined
[18] University of Montreal,undefined
[19] College of Veterinary Medicine,undefined
[20] Konkuk University,undefined
[21] 1 Hwayang-dong,undefined
[22] Gwangjin-gu,undefined
[23] Medical Research Institute,undefined
[24] College of Medicine,undefined
[25] Chung-Ang University,undefined
[26] School of Medicine,undefined
[27] SMART Institute of Advanced Biomedical Science,undefined
[28] Konkuk University,undefined
[29] 1 Hwayang-dong,undefined
[30] Gwangjin-gu,undefined
[31] School of Medicine,undefined
[32] SMART Institute of Advanced Biomedical Science,undefined
[33] Konkuk University,undefined
[34] 1 Hwayang-dong,undefined
[35] Gwangjin-gu,undefined
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SIGN-R1; splenic marginal zone macrophages; complements; apoptotic cells; autoimmune disease;
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摘要
Complements, such as C1q and C3, and macrophages in the splenic marginal zone (MZMs) play pivotal roles in the efficient uptake and processing of circulating apoptotic cells. SIGN-R1, a C-type lectin that is highly expressed in a subpopulation of MZMs, regulates the complement fixation pathway by interacting with C1q, to fight blood-borne Streptococcus pneumoniae. Therefore, we examined whether the SIGN-R1-mediated classical complement pathway plays a role in apoptotic cell clearance and immune tolerance. SIGN-R1 first-bound apoptotic cells and this binding was significantly enhanced in the presence of C1q. SIGN-R1–C1q complex then immediately mediated C3 deposition on circulating apoptotic cells in the MZ, leading to the efficient clearance of them. SIGN-R1-mediated C3 deposition was completely abolished in the spleen of SIGN-R1 knockout (KO) mice. Given that SIGN-R1 is not expressed in the liver, we were struck by the finding that C3-deposited apoptotic cells were still found in the liver of wild-type mice, and dramatically reduced in the SIGN-R1 KO liver. In particular, SIGN-R1 deficiency caused delayed clearance of apoptotic cells and aberrant secretion of cytokines, such as TNF-α, IL-6, and TGF-β in the spleen as well as in the liver. In addition, anti-double- and single-stranded DNA antibody level was significantly increased in SIGN-R1-depleted mice compared with control mice. These findings suggest a novel mechanism of apoptotic cell clearance which is initiated by SIGN-R1 in the MZ and identify an integrated role of SIGN-R1 in the systemic clearance of apoptotic cells, linking the recognition of apoptotic cells, the opsonization of complements, and the induction of immune tolerance.
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页码:535 / 545
页数:10
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