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Molecular interaction between natural IgG and ficolin – mechanistic insights on adaptive-innate immune crosstalk

机译:天然IgG和Ficolin之间的分子相互作用-适应性先天免疫串扰的机理研究

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摘要

Recently, we found that natural IgG (nIgG; a non-specific immunoglobulin of adaptive immunity) is not quiescent, but plays a crucial role in immediate immune defense by collaborating with ficolin (an innate immune protein). However, how the nIgG and ficolin interplay and what factors control the complex formation during infection is unknown. Here, we found that mild acidosis and hypocalcaemia induced by infection- inflammation condition increased the nIgG:ficolin complex formation. Hydrogen-deuterium exchange mass spectrometry delineated the binding interfaces to the CH2–CH3 region of nIgG Fc and P-subdomain of ficolin FBG domain. Infection condition exposes novel binding sites. Site-directed mutagenesis and surface plasmon resonance analyses of peptides, derived from nIgG and ficolin, defined the interacting residues between the proteins. These results provide mechanistic insights on the interaction between two molecules representing the adaptive and innate immune pathways, prompting potential development of immunomodulatory/prophylactic peptides tunable to prevailing infection conditions.
机译:最近,我们发现天然IgG(nIgG;适应性免疫的非特异性免疫球蛋白)不是静止的,而是通过与Ficolin(一种先天免疫蛋白)的协同作用在立即免疫防御中起关键作用。但是,尚不清楚nIgG和纤维胶蛋白如何相互作用以及在感染过程中哪些因素控制复合物的形成。在这里,我们发现由感染-炎症引起的轻度酸中毒和低血钙症增加了nIgG:ficolin复合物的形成。氢-氘交换质谱法描绘了结合界面与nIgG Fc的CH2-CH3区和Ficolin FBG结构域的P-亚结构域。感染条件暴露出新的结合位点。来源于nIgG和纤维胶凝蛋白的多肽的定点诱变和表面等离子体共振分析确定了蛋白质之间的相互作用残基。这些结果为代表适应性免疫途径和先天性免疫途径的两个分子之间的相互作用提供了机械学见解,从而促进了可调节至主要感染条件的免疫调节/预防肽的潜在发展。

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