内含子22倒位的F8基因座允许因子VIII合成:低抑制剂风险的解释及药物基因组学的作用。
The intron-22-inverted F8 locus permits factor VIII synthesis: explanation for low inhibitor risk and a role for pharmacogenomics.
作者信息
Sauna Zuben E, Lozier Jay N, Kasper Carol K, Yanover Chen, Nichols Timothy, Howard Tom E
机构信息
Laboratory of Hemostasis, Division of Hematology Research and Review, Center for Biologics Evaluation and Research, Food and Drug Administration, Silver Spring, MD;
Hematology Section, Department of Laboratory Medicine, National Institutes of Health Clinical Center, Bethesda, MD;
出版信息
Blood. 2015 Jan 8;125(2):223-8. doi: 10.1182/blood-2013-12-530113. Epub 2014 Nov 18.
Abstract
Intron-22-inversion patients express the entire Factor VIII (FVIII)-amino-acid sequence intracellularly as 2 non-secreted polypeptides and have a positive "intracellular (I)-FVIII-CRM" status. Mutations conferring a positive I-FVIII-CRM status are associated with low inhibitor risk and are pharmacogenetically relevant because inhibitor risk may be affected by the nature of the therapeutic FVIII-protein (tFVIII), the affinity of any tFVIII-derived foreign peptide (tFVIII-fp) for any HLA class-II isomer (HLA-II) comprising individual major histocompatibility complex (MHC) repertoires, and the stability of any tFVIII-fp/HLA-II complex. We hypothesize that mutations conferring a completely or substantially negative I-FVIII-CRM status are pharmacogenetically irrelevant because inhibitor risk is high with any tFVIII and individual MHC repertoire.
摘要
内含子22倒位患者在细胞内将整个凝血因子VIII(FVIII)氨基酸序列表达为2种非分泌性多肽,并且具有阳性的“细胞内(I)-FVIII-CRM”状态。赋予阳性I-FVIII-CRM状态的突变与低抑制剂风险相关,并且在药物遗传学上具有相关性,因为抑制剂风险可能受治疗性FVIII蛋白(tFVIII)的性质、任何tFVIII衍生的外源肽(tFVIII-fp)对构成个体主要组织相容性复合体(MHC)库的任何HLA-II类异构体(HLA-II)的亲和力以及任何tFVIII-fp/HLA-II复合体的稳定性影响。我们推测,赋予完全或基本阴性I-FVIII-CRM状态的突变在药物遗传学上不相关,因为使用任何tFVIII和个体MHC库时抑制剂风险都很高。
相似文献
1
The intron-22-inverted F8 locus permits factor VIII synthesis: explanation for low inhibitor risk and a role for pharmacogenomics.内含子22倒位的F8基因座允许因子VIII合成:低抑制剂风险的解释及药物基因组学的作用。
Blood. 2015 Jan 8;125(2):223-8. doi: 10.1182/blood-2013-12-530113. Epub 2014 Nov 18.
2
Endogenous factor VIII synthesis from the intron 22-inverted F8 locus may modulate the immunogenicity of replacement therapy for hemophilia A.内源性因子 VIII 来源于内含子 22 倒置的 F8 基因座,可能调节血友病 A 替代治疗的免疫原性。
Nat Med. 2013 Oct;19(10):1318-24. doi: 10.1038/nm.3270. Epub 2013 Sep 15.
3
HLA-DRB1-factor VIII binding is a risk factor for inhibitor development in nonsevere hemophilia: a case-control study.HLA-DRB1-因子 VIII 结合是导致非重度血友病抑制剂发展的风险因素:一项病例对照研究。
Blood Adv. 2018 Jul 24;2(14):1750-1755. doi: 10.1182/bloodadvances.2018019323.
4
In silico calculated affinity of FVIII-derived peptides for HLA class II alleles predicts inhibitor development in haemophilia A patients with missense mutations in the F8 gene.基于计算机计算的 FVIII 衍生肽与 HLA Ⅱ类等位基因的亲和力可预测 F8 基因突变的血友病 A 患者产生抑制剂的情况。
Haemophilia. 2014 Mar;20(2):176-84. doi: 10.1111/hae.12276. Epub 2013 Oct 14.
5
Hemophilia A subjects with an intron-22 gene inversion mutation show CD4 T-effector responses to multiple epitopes in FVIII.患有内含子 22 基因突变的血友病 A 患者对 FVIII 中的多个表位具有 CD4 T 效应器反应。
Front Immunol. 2023 Mar 1;14:1128641. doi: 10.3389/fimmu.2023.1128641. eCollection 2023.
6
FVIII Immunogenicity-Bioinformatic Approaches to Evaluate Inhibitor Risk in Non-severe Hemophilia A.FVIII 免疫原性-生物信息学方法评估非重度血友病 A 抑制剂风险。
Front Immunol. 2020 Jul 28;11:1498. doi: 10.3389/fimmu.2020.01498. eCollection 2020.
7
CD4+ T-cell clones specific for wild-type factor VIII: a molecular mechanism responsible for a higher incidence of inhibitor formation in mild/moderate hemophilia A.针对野生型凝血因子VIII的CD4 + T细胞克隆:轻度/中度A型血友病中抑制剂形成发生率较高的分子机制。
Blood. 2003 Feb 15;101(4):1351-8. doi: 10.1182/blood-2002-05-1369. Epub 2002 Oct 17.
8
Analysis of F8 inversions as risk factors for FVIII inhibitor development in Indian severe haemophilia A patients.印度重度甲型血友病患者中F8倒位作为FVIII抑制剂形成风险因素的分析
Blood Cells Mol Dis. 2014 Sep;53(3):161-3. doi: 10.1016/j.bcmd.2014.04.007. Epub 2014 May 11.
9
Prediction of factor VIII inhibitor development in the SIPPET cohort by mutational analysis and factor VIII antigen measurement.通过突变分析和因子 VIII 抗原测量预测 SIPPET 队列中因子 VIII 抑制剂的发展。
J Thromb Haemost. 2018 Apr;16(4):778-790. doi: 10.1111/jth.13961. Epub 2018 Mar 23.
10
A large-scale computational study of inhibitor risk in non-severe haemophilia A.一项关于非重度血友病 A 抑制剂风险的大规模计算研究。
Br J Haematol. 2015 Feb;168(3):413-20. doi: 10.1111/bjh.13131. Epub 2014 Sep 22.
引用本文的文献
1
A scan of pleiotropic immune mediated disease genes identifies novel determinants of baseline FVIII inhibitor status in hemophilia A.对多效性免疫介导疾病基因的扫描确定了甲型血友病中基线FVIII抑制物状态的新决定因素。
Genes Immun. 2025 Apr 22. doi: 10.1038/s41435-025-00325-7.
2
A Scan of Pleiotropic Immune Mediated Disease Genes Identifies Novel Determinants of Baseline FVIII Inhibitor Status in Hemophilia-A.对多效性免疫介导疾病基因的扫描揭示了血友病A中基线FVIII抑制剂状态的新决定因素。
Res Sq. 2023 Oct 18:rs.3.rs-3371095. doi: 10.21203/rs.3.rs-3371095/v1.
3
Hemophilia A subjects with an intron-22 gene inversion mutation show CD4 T-effector responses to multiple epitopes in FVIII.患有内含子 22 基因突变的血友病 A 患者对 FVIII 中的多个表位具有 CD4 T 效应器反应。
Front Immunol. 2023 Mar 1;14:1128641. doi: 10.3389/fimmu.2023.1128641. eCollection 2023.
4
F9 mutations causing deletions beyond the serine protease domain confer higher risk for inhibitor development in hemophilia B.导致丝氨酸蛋白酶结构域以外缺失的F9突变会增加B型血友病患者产生抑制剂的风险。
Blood. 2023 Feb 9;141(6):677-680. doi: 10.1182/blood.2022017871.
5
Genome-Wide Association Study and Gene-Based Analysis of Participants With Hemophilia A and Inhibitors in the My Life, Our Future Research Repository.全基因组关联研究以及对参与“我的生活,我们的未来”血友病A和抑制物研究库的患者进行基因分析。
Front Med (Lausanne). 2022 Jun 23;9:903838. doi: 10.3389/fmed.2022.903838. eCollection 2022.
6
Mechanistic Insights into Factor VIII Immune Tolerance Induction via Prenatal Cell Therapy in Hemophilia A.对血友病A中通过产前细胞疗法诱导凝血因子VIII免疫耐受的机制性见解。
Curr Stem Cell Rep. 2019 Dec;5(4):145-161. doi: 10.1007/s40778-019-00165-y. Epub 2019 Nov 20.
7
Safety and efficacy of turoctocog alfa in the prevention and treatment of bleeds in previously untreated paediatric patients with severe haemophilia A: Results from the guardian 4 multinational clinical trial.泰它西普在预防和治疗未曾治疗过的重度 A 型血友病儿童患者出血的安全性和疗效:来自 guardian 4 项多国临床试验的结果。
Haemophilia. 2020 Jan;26(1):64-72. doi: 10.1111/hae.13883. Epub 2019 Dec 9.
8
Innovative Approaches for Immune Tolerance to Factor VIII in the Treatment of Hemophilia A.血友病A治疗中对凝血因子VIII免疫耐受的创新方法。
Front Immunol. 2017 Nov 24;8:1604. doi: 10.3389/fimmu.2017.01604. eCollection 2017.
9
In situ genetic correction of F8 intron 22 inversion in hemophilia A patient-specific iPSCs.对血友病 A 患者特异性诱导多能干细胞中 F8 内含子 22 倒位进行原位基因校正。
Sci Rep. 2016 Jan 8;6:18865. doi: 10.1038/srep18865.
本文引用的文献
1
Apoptotic cell clearance: basic biology and therapeutic potential.细胞凋亡清除:基础生物学与治疗潜能。
Nat Rev Immunol. 2014 Mar;14(3):166-80. doi: 10.1038/nri3607. Epub 2014 Jan 31.
2
Building better drugs: developing and regulating engineered therapeutic proteins.研发更好的药物:开发和监管工程治疗性蛋白。
Trends Pharmacol Sci. 2013 Oct;34(10):534-48. doi: 10.1016/j.tips.2013.08.005. Epub 2013 Sep 20.
3
Endogenous factor VIII synthesis from the intron 22-inverted F8 locus may modulate the immunogenicity of replacement therapy for hemophilia A.内源性因子 VIII 来源于内含子 22 倒置的 F8 基因座,可能调节血友病 A 替代治疗的免疫原性。
Nat Med. 2013 Oct;19(10):1318-24. doi: 10.1038/nm.3270. Epub 2013 Sep 15.
4
Factor VIII gene (F8) mutation and risk of inhibitor development in nonsevere hemophilia A.VIII 因子基因(F8)突变与非重度血友病 A 抑制剂发展风险。
Blood. 2013 Sep 12;122(11):1954-62. doi: 10.1182/blood-2013-02-483263. Epub 2013 Aug 7.
5
NetMHCIIpan-3.0, a common pan-specific MHC class II prediction method including all three human MHC class II isotypes, HLA-DR, HLA-DP and HLA-DQ.NetMHCIIpan-3.0 是一种常见的 pan-specific MHC 类 II 预测方法,包括所有三种人类 MHC 类 II 同种异型,HLA-DR、HLA-DP 和 HLA-DQ。
Immunogenetics. 2013 Oct;65(10):711-24. doi: 10.1007/s00251-013-0720-y. Epub 2013 Jul 31.
6
Polymorphisms in the F8 gene and MHC-II variants as risk factors for the development of inhibitory anti-factor VIII antibodies during the treatment of hemophilia a: a computational assessment.F8 基因多态性和 MHC-II 变体作为血友病 A 治疗过程中抑制性抗因子 VIII 抗体产生的风险因素:计算评估。
PLoS Comput Biol. 2013;9(5):e1003066. doi: 10.1371/journal.pcbi.1003066. Epub 2013 May 16.
7
F8 haplotype and inhibitor risk: results from the Hemophilia Inhibitor Genetics Study (HIGS) Combined Cohort.F8 单倍型与抑制剂风险:来自血友病抑制剂遗传学研究(HIGS)联合队列的结果。
Haemophilia. 2013 Jan;19(1):113-8. doi: 10.1111/hae.12004. Epub 2012 Sep 7.
8
Cross-presentation by dendritic cells.树突状细胞的交叉呈递。
Nat Rev Immunol. 2012 Jul 13;12(8):557-69. doi: 10.1038/nri3254.
9
F8 gene mutation type and inhibitor development in patients with severe hemophilia A: systematic review and meta-analysis.F8 基因突变类型和严重血友病 A 患者抑制剂的开发:系统评价和荟萃分析。
Blood. 2012 Mar 22;119(12):2922-34. doi: 10.1182/blood-2011-09-379453. Epub 2012 Jan 26.
10
Plasma derivatives: new products and new approaches.血浆衍生物:新产品与新方法。
Biologicals. 2012 May;40(3):191-5. doi: 10.1016/j.biologicals.2011.11.003. Epub 2012 Jan 11.
Zotero 插件