Lack of factor VIII detection in humans and dogs with an intron 22 inversion challenges hypothesis regarding inhibitor risk.

IF 5.5 2区 医学 Q1 HEMATOLOGY Journal of Thrombosis and Haemostasis Pub Date : 2024-09-02 DOI:10.1016/j.jtha.2024.08.007
Pooja Vir, Devi Gunasekera, Batsukh Dorjbal, Dennis McDaniel, Atul Agrawal, Elizabeth P Merricks, Margaret V Ragni, Cindy A Leissinger, Allen I Stering, Kenneth Lieuw, Timothy C Nichols, Kathleen P Pratt
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Abstract

Background: Almost half of severe hemophilia A (HA) cases are caused by an intron 22 inversion (Int22Inv) mutation, which truncates the 26-exon F8 messenger RNA (mRNA) after exon 22. Another F8 transcript, F8B, is initiated from within F8-intron-22. F8B mRNA consists of a short exon spliced to exons 23 to 26 and is expressed in multiple human cell types. It has been hypothesized that Int22Inv patients have self-tolerance to partial factor (F)VIII proteins expressed from these 2 transcripts. FVIII is expressed in endothelial cells, primarily in the liver and lungs. Several studies have reported FVIII expression in other cell types, although this has been controversial.

Objectives: To determine if partial FVIII proteins are expressed from intron 22-inverted and/or F8B mRNA and if FVIII is expressed in nonendothelial cells.

Methods: A panel of FVIII-specific antibodies was validated and employed to label FVIII in cells and tissues and for immunoprecipitation followed by western blots and mass spectrometry proteomics analysis.

Results: Immunofluorescent staining localized FVIII to endothelial cells in liver sections from non-HA but not HA-Int22Inv dogs. Neither FVIII nor FVIIIB was detected in human peripheral blood mononuclear cells, B cell or T cell lines, or cell lines expanded from peripheral blood mononuclear cells, whereas FVIII antigen and activity were readily detected in primary nonhemophilic liver sinusoidal endothelial cells.

Conclusion: If FVIII is expressed in nonendothelial cells or if partial FVIII proteins are expressed in HA-Int22Inv, the concentrations are below the detection limits of these sensitive assays. Our results argue against promotion of immune tolerance through expression of partial FVIII proteins in Int-22Inv patients.

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人类和狗体内未检测到 FVIII 内含子-22 倒位,这对有关抑制剂风险的假设提出了挑战。
背景:近一半的严重 A 型血友病(HA)病例是由内含子-22 倒位突变(Int22Inv)引起的,这种突变会在外显子 22 之后截断 26 外显子 F8 mRNA。另一个 F8 转录本 F8B 从 F8 内含子-22 开始。F8B mRNA 由一个短外显子剪接成 23-26 号外显子,在多种人类细胞类型中表达。据推测,Int22Inv 患者对这两种转录本表达的部分 FVIII 蛋白具有自身耐受性。FVIII 主要在肝脏和肺部的内皮细胞中表达。一些研究报告称 FVIII 在其他细胞类型中也有表达,但这一点一直存在争议:目的:确定部分 FVIII 蛋白是否由内含子 22 倒置和/或 F8B mRNA 表达,以及 FVIII 是否在非内皮细胞中表达:方法: 验证并使用一组FVIII特异性抗体标记细胞和组织中的FVIII,并进行免疫沉淀,然后进行Western印迹和质谱-蛋白质组学分析:结果:免疫荧光(IF)染色将 FVIII 定位于非 HA 而非 HA-Int22Inv 狗肝脏切片的内皮细胞。在人类 PBMCs、B 细胞系或 T 细胞系或由 PBMCs 扩增的细胞系中均未检测到 FVIII 或 FVIIIB,而在原代非血友病肝窦内皮细胞中很容易检测到 FVIII 抗原和活性:结论:如果 FVIII 在非内皮细胞中表达,或部分 FVIII 蛋白在 HA-Int22Inv 中表达,则其浓度低于这些灵敏检测方法的检测限。我们的结果表明,Int-22Inv 患者体内部分 FVIII 蛋白的表达不会促进免疫耐受。
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来源期刊
Journal of Thrombosis and Haemostasis
Journal of Thrombosis and Haemostasis 医学-外周血管病
CiteScore
24.30
自引率
3.80%
发文量
321
审稿时长
1 months
期刊介绍: The Journal of Thrombosis and Haemostasis (JTH) serves as the official journal of the International Society on Thrombosis and Haemostasis. It is dedicated to advancing science related to thrombosis, bleeding disorders, and vascular biology through the dissemination and exchange of information and ideas within the global research community. Types of Publications: The journal publishes a variety of content, including: Original research reports State-of-the-art reviews Brief reports Case reports Invited commentaries on publications in the Journal Forum articles Correspondence Announcements Scope of Contributions: Editors invite contributions from both fundamental and clinical domains. These include: Basic manuscripts on blood coagulation and fibrinolysis Studies on proteins and reactions related to thrombosis and haemostasis Research on blood platelets and their interactions with other biological systems, such as the vessel wall, blood cells, and invading organisms Clinical manuscripts covering various topics including venous thrombosis, arterial disease, hemophilia, bleeding disorders, and platelet diseases Clinical manuscripts may encompass etiology, diagnostics, prognosis, prevention, and treatment strategies.
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