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补体治疗性因子H-IgG蛋白作为莱姆疏螺旋体感染的暴露前预防措施。

Complement therapeutic Factor H-IgG proteins as pre-exposure prophylaxes against Lyme borreliae infections.

作者信息

McKaig Connor W, Malfetano Jill, Tran Y, Yang Xiuli, Pal Utpal, Wycoff Keith, Lin Yi-Pin

机构信息

Department of Infectious Disease and Global Health, Cummings School of Veterinary Medicine, Tufts University, North Grafton, MA, USA.

Division of Infectious Diseases, Wadsworth Center, NYSDOH, Albany, NY, USA.

出版信息

bioRxiv. 2024 Sep 26:2024.09.26.615144. doi: 10.1101/2024.09.26.615144.

Abstract

Lyme disease (LD) is the most common vector-borne disease in the northern hemisphere and is caused by the bacteria sensu lato (also known as Lyme borreliae) with no effective prevention available. Lyme borreliae evade complement killing, a critical arm of host immune defense, by producing outer surface proteins that bind to a host complement inhibitor, factor H (FH). These outer surface proteins include CspA and CspZ, which bind to the 6 and 7 short consensus repeats of FH (SCR(6-7)), and the OspE family of proteins (OspE), which bind to the 19 and 20 SCR (SCR19-20). In this study, we produced two chimeric proteins, FH-Fc, containing the Fc region of immunoglobulin G (Fc) with SCR(6-7) or SCR(19-20). We found that both FH-Fc constructs killed in the presence of complement and reduced bacterial colonization and LD-associated joint inflammation . While SCR(6-7)-Fc displayed Lyme borreliae species-specific bacterial killing, SCR(19-20)-Fc versatilely eradicated all tested bacterial species/strains. This correlated with SCR(6-7)-Fc binding to select variants of CspA and CspZ, but SCR(19-20)-Fc binding to all tested OspE variants. Overall, we demonstrated the concept of using FH-Fc constructs to kill Lyme borreliae and defined underlying mechanisms, highlighting the potential of FH-Fc as a pre-exposure prophylaxis against LD infection.

摘要

莱姆病(LD)是北半球最常见的媒介传播疾病,由疏螺旋体属细菌(也称为莱姆疏螺旋体)引起,目前尚无有效的预防方法。莱姆疏螺旋体通过产生与宿主补体抑制剂H因子(FH)结合的外表面蛋白,逃避补体杀伤这一宿主免疫防御的关键环节。这些外表面蛋白包括与FH的6和7个短共识重复序列(SCR(6-7))结合的CspA和CspZ,以及与19和20个SCR(SCR19-20)结合的OspE蛋白家族(OspE)。在本研究中,我们制备了两种嵌合蛋白FH-Fc,分别包含免疫球蛋白G(Fc)的Fc区域与SCR(6-7)或SCR(19-20)。我们发现,两种FH-Fc构建体在补体存在的情况下均能杀伤细菌,并减少细菌定植和与LD相关的关节炎症。虽然SCR(6-7)-Fc表现出对莱姆疏螺旋体物种特异性的细菌杀伤作用,但SCR(19-20)-Fc能广泛根除所有测试的细菌物种/菌株。这与SCR(6-7)-Fc结合特定的CspA和CspZ变体,但SCR(19-20)-Fc结合所有测试的OspE变体相关。总体而言,我们证明了使用FH-Fc构建体杀伤莱姆疏螺旋体的概念,并确定了潜在机制,突出了FH-Fc作为预防LD感染的暴露前预防措施的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8ddf/11463399/2df62ce1bb74/nihpp-2024.09.26.615144v1-f0001.jpg

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