C1q/MASP Complexes-Hybrid Complexes of Classical and Lectin Pathway Proteins Are Found in the Circulation.

IF 3.6 3区 医学 Q2 IMMUNOLOGY Journal of immunology Pub Date : 2024-10-01 DOI:10.4049/jimmunol.2400185
Anne Rosbjerg, Tereza Alica Plchová, Rafael Bayarri-Olmos, Bettina Eide Holm, Ida Sandau Pedersen, Mikkel-Ole Skjoedt, Peter Garred
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Abstract

Complement pathways, traditionally regarded as separate entities in vitro, are increasingly noted for cross-communication and bypass mechanisms. Among these, the MBL/ficolin/CL-associated serine protease (MASP)-3, a component of lectin pathway pattern recognition molecules, has shown the ability to process critical substrates such as pro-factor D and insulin growth factor binding protein-5. Given shared features between lectin pathway pattern recognition molecules and C1q from the classical pathway, we hypothesized that C1q might be a viable in vivo binding partner for the MASPs. We used microscale thermophoresis, ELISA, and immunoprecipitation assays to detect C1q/MASP complexes and functionally assessed the complexes through enzymatic cleavage assays. C1q/MASP-3 complexes were detected in human serum and correlated well with MASP-3 serum levels in healthy individuals. The binding affinity between MASP-3 and C1q in vitro was in the nanomolar range, and the interaction was calcium-dependent, as demonstrated by their dissociation in the presence of EDTA. Furthermore, most of the circulating C1q-bound MASP-3 was activated. Based on immunoprecipitation, also C1q/MASP-2 complexes appeared to be present in serum. Finally, C1q/MASP-2 and C1q/MASP-3 in vitro complexes were able to cleave C4 and pro-factor D, respectively. Our study reveals the existence of C1q/MASP complexes in the circulation of healthy individuals, and both C1q/MASP-2 and C1q/MASP-3 complexes display proteolytic activity. Hence, this study uncovers a crosstalk route between complement pathways not previously described.

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在血液循环中发现 C1q/MASP 复合物--经典蛋白和 Lectin 途径蛋白的杂交复合物。
传统上被视为体外独立实体的补体通路,其交叉交流和旁路机制日益受到关注。其中,MBL/ficolin/CL 相关丝氨酸蛋白酶(MASP)-3 是凝集素途径模式识别分子的一个组成部分,它已显示出处理关键底物(如原因子 D 和胰岛素生长因子结合蛋白-5)的能力。鉴于凝集素通路模式识别分子与经典通路中的 C1q 之间的共同特征,我们假设 C1q 可能是 MASPs 的一个可行的体内结合伙伴。我们使用微尺度热泳、酶联免疫吸附和免疫沉淀试验检测 C1q/MASP 复合物,并通过酶裂解试验对复合物进行功能评估。在人体血清中检测到了 C1q/MASP-3 复合物,并与健康人血清中的 MASP-3 水平密切相关。在体外,MASP-3 和 C1q 的结合亲和力在纳摩尔范围内,这种相互作用是钙依赖性的,在 EDTA 存在下它们的解离就证明了这一点。此外,循环中与 C1q 结合的 MASP-3 大部分被活化。根据免疫沉淀法,血清中似乎也存在 C1q/MASP-2 复合物。最后,C1q/MASP-2 和 C1q/MASP-3 体外复合物能分别裂解 C4 和原因子 D。我们的研究揭示了健康人血液循环中存在 C1q/MASP 复合物,而且 C1q/MASP-2 和 C1q/MASP-3 复合物都显示出蛋白水解活性。因此,这项研究发现了一种以前从未描述过的补体途径之间的串联途径。
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来源期刊
Journal of immunology
Journal of immunology 医学-免疫学
CiteScore
8.20
自引率
2.30%
发文量
495
审稿时长
1 months
期刊介绍: The JI publishes novel, peer-reviewed findings in all areas of experimental immunology, including innate and adaptive immunity, inflammation, host defense, clinical immunology, autoimmunity and more. Special sections include Cutting Edge articles, Brief Reviews and Pillars of Immunology. The JI is published by The American Association of Immunologists (AAI)
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