VIII 因子抗体免疫复合物以表位依赖的方式调节对 VIII 因子的体液免疫反应。

Factor VIII antibody immune complexes modulate the humoral response to factor VIII in an epitope-dependent manner.

机构信息

Department of Pediatrics, Emory University, Atlanta, GA, United States.

Aflac Cancer and Blood Disorders Center of Children's Healthcare of Atlanta, Atlanta, GA, United States.

出版信息

Front Immunol. 2023 Aug 31;14:1233356. doi: 10.3389/fimmu.2023.1233356. eCollection 2023.

DOI:10.3389/fimmu.2023.1233356

PMID:37720212

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10501482/

Abstract

INTRODUCTION

Soluble antigens complexed with immunoglobulin G (IgG) antibodies can induce robust adaptive immune responses and in animal models of disease. Factor VIII immune complexes (FVIII-ICs) have been detected in individuals with hemophilia A and severe von Willebrand disease following FVIII infusions. Yet, it is unclear if and how FVIII-ICs affect antibody development over time.

METHODS

In this study, we analyzed internalization of FVIII complexed with epitope-mapped FVIII-specific IgG monoclonal antibodies (MAbs) by murine bone marrow-derived dendritic cells (BMDCs) and antibody development in hemophilia A (FVIII) mice injected with FVIII-IC over time.

RESULTS

FVIII complexed with 2-116 (A1 domain MAb), 2-113 (A3 domain MAb), and I55 (C2 domain MAb) significantly increased FVIII uptake by BMDC but only FVIII/2-116 enhanced antibody titers in FVIII mice compared to FVIII alone. FVIII/4A4 (A2 domain MAb) showed similar FVIII uptake by BMDC to that of isolated FVIII yet significantly increased antibody titers when injected in FVIII mice. Enhanced antibody responses observed with FVIII/2-116 and FVIII/4A4 complexes were abrogated in the absence of the FVIII carrier protein von Willebrand factor.

CONCLUSION

These findings suggest that a subset of FVIII-IC modulates the humoral response to FVIII in an epitope-dependent manner, which may provide insight into the antibody response observed in some patients with hemophilia A.

摘要

简介

与免疫球蛋白 G（IgG）抗体结合的可溶性抗原可以诱导强大的适应性免疫反应，并在疾病的动物模型中发挥作用。在接受 FVIII 输注后，患有血友病 A 和严重 von Willebrand 病的个体中已经检测到因子 VIII 免疫复合物（FVIII-ICs）。然而，目前尚不清楚 FVIII-IC 是否以及如何随时间推移影响抗体的产生。

方法

在这项研究中，我们分析了 FVIII 与表位映射的 FVIII 特异性 IgG 单克隆抗体（MAb）形成复合物后被小鼠骨髓来源的树突状细胞（BMDC）内化的情况，以及随着时间的推移，FVIII 小鼠注射 FVIII-IC 后抗体的产生情况。

结果

FVIII 与 2-116（A1 结构域 MAb）、2-113（A3 结构域 MAb）和 I55（C2 结构域 MAb）形成的复合物显著增加了 FVIII 被 BMDC 的摄取，但只有 FVIII/2-116 与单独的 FVIII 相比，增强了 FVIII 小鼠中的抗体滴度。FVIII/4A4（A2 结构域 MAb）与分离的 FVIII 相比，BMDC 摄取 FVIII 的情况相似，但当在 FVIII 小鼠中注射时，显著增加了抗体滴度。FVIII/2-116 和 FVIII/4A4 复合物观察到的增强的抗体反应在缺乏 FVIII 载体蛋白 von Willebrand 因子的情况下被阻断。

结论

这些发现表明，FVIII-IC 的一部分以表位依赖性方式调节对 FVIII 的体液反应，这可能为一些血友病 A 患者中观察到的抗体反应提供一些见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9fa3/10501482/39c0b0921459/fimmu-14-1233356-g001.jpg

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VIII 因子抗体免疫复合物以表位依赖的方式调节对 VIII 因子的体液免疫反应。

Factor VIII antibody immune complexes modulate the humoral response to factor VIII in an epitope-dependent manner.

机构信息

Department of Pediatrics, Emory University, Atlanta, GA, United States.

Aflac Cancer and Blood Disorders Center of Children's Healthcare of Atlanta, Atlanta, GA, United States.