Characterization of zebrafish coagulation cofactors Fviii and Fv mutants and modeling hemophilia A and factor V deficiency.

IF 1.2 4区 医学 Q4 HEMATOLOGY Blood Coagulation & Fibrinolysis Pub Date : 2024-07-01 Epub Date: 2024-06-10 DOI:10.1097/MBC.0000000000001308
Sanchi Dhinoja, Anthony De Maria, Ayah Al Qaryoute, Pudur Jagadeeswaran
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Abstract

The aim of this study is to characterize zebrafish coagulation cofactors fviii and fv mutant fish and assess if they phenocopy classical hemophilia A and factor V deficiency in humans. The embryos from fviii and fv zebrafish heterozygote mutants generated by ENU mutagenesis were purchased from the ZIRC repository. They were reared to adulthood and genotyped. The heterozygote male and female were crossed to get homozygote, heterozygote, and wild-type fish. Functional kinetic coagulation assays and bleeding assays were performed on normal and mutant adult fish, and venous laser injury assays were performed on the larvae. The DNA from fviii and fv mutants were sequenced to confirm if they have a premature stop codon in exon 19, and in exon 2, respectively, and in both mutants, the amino acid glutamine is replaced with a stop codon. Homozygous and heterozygous 5 days post fertilization (dpf) larvae for fviii and fv deficient mutants exhibited prolonged time to occlusion after venous laser injury compared to wild-type controls. The homozygous and heterozygous fviii adult mutants showed modest bleeding and delayed fibrin formation in the kinetic partial thromboplastin time (kPTT) assay with their plasma. fv homozygous larvae had poor survival beyond 12 dpf. However, heterozygous fv mutants exhibited heavy bleeding and prolonged fibrin formation in the kPTT and kPT assay compared with wild-type siblings. Our characterization showed fviii and fv mutants from ZIRC phenocopied to a considerable extent classical hemophilia A and factor V deficiency in humans, respectively. These models should be useful in studying and developing novel drugs that reverse the phenotype and in generating suppressor mutations to identify novel factors that compensate for these deficiencies.

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斑马鱼凝血辅因子 Fviii 和 Fv 突变体的特征以及 A 型血友病和 V 型因子缺乏症的建模。
本研究的目的是描述斑马鱼凝血辅因子 fviii 和 fv 突变体的特征,并评估它们是否表征人类的典型血友病 A 和因子 V 缺乏症。由 ENU 诱变产生的 fviii 和 fv 斑马鱼杂合突变体的胚胎购自 ZIRC 储存库。它们被饲养至成年并进行基因分型。将杂合突变体雌雄杂交,得到同源突变体、杂合突变体和野生型斑马鱼。对正常和突变型成鱼进行功能动力学凝血试验和出血试验,对幼鱼进行静脉激光损伤试验。对 fviii 和 fv 突变体的 DNA 进行了测序,以确认它们是否分别在外显子 19 和外显子 2 中存在过早终止密码子,在这两个突变体中,谷氨酰胺氨基酸被终止密码子取代。与野生型对照组相比,fviii 和 fv 缺陷突变体的同卵和杂合受精后 5 天幼虫在静脉激光损伤后闭塞时间延长。同卵和杂合的 fviii 成体突变体在血浆部分凝血活酶时间(kPTT)测定中表现出适度出血和纤维蛋白形成延迟。然而,与野生型同胞相比,杂合子 fv 突变体在 kPTT 和 kPT 试验中表现出大量出血和纤维蛋白形成时间延长。我们的鉴定结果表明,ZIRC的fviii和fv突变体分别在相当程度上表征了人类的典型血友病A和因子V缺乏症。这些模型将有助于研究和开发可逆转表型的新型药物,并有助于产生抑制突变,以确定可补偿这些缺陷的新型因子。
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来源期刊
CiteScore
1.90
自引率
0.00%
发文量
111
审稿时长
4-8 weeks
期刊介绍: Blood Coagulation & Fibrinolysis is an international fully refereed journal that features review and original research articles on all clinical, laboratory and experimental aspects of haemostasis and thrombosis. The journal is devoted to publishing significant developments worldwide in the field of blood coagulation, fibrinolysis, thrombosis, platelets and the kininogen-kinin system, as well as dealing with those aspects of blood rheology relevant to haemostasis and the effects of drugs on haemostatic components
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