20例先天性纤维蛋白原病患者临床表现和基因突变分析

目的回顾性分析2017年2月至2021年12月就诊于本院的20例先天性纤维蛋白原病(congenital Fibrinogen disorders,CFD)患者的临床表现、相关实验室检查及基因突变分析,以此提高对CFD诊断方法的认识。方法收集20例CFD患者临床特征及实验室检查,排除了常见的获得性低纤维蛋白原血症因素,对其纤维蛋白原(Fib)的FGA、FGB和FGG基因所有外显子和侧翼序列进行基因测序寻找基因突变位点。对2例CFD患者家系成员采集外周血基因组DNA,进行先证者相应突变位点区域基因检测。结果20例CFD患者既往无明显出血病史,11例女性患者亦无自发流产史,20例患者Fib均减低,凝血酶时间(TT)均延长。20例患者检出13种基因突变,其中90%(18/20)为错义突变,5%(1/20)为缺失变异,5%(1/20)为移码变异,35%(7/20)患者存在FGA链104位点Arg35His突变,其中3种新基因突变国内尚未报道。结论多数CFD患者症状轻微或者无症状,通过基因检测筛查后方可确诊,FGA链Arg35His是本地区的突变热点,均为维吾尔族,此位点突变是否与维吾尔族有关有待于进一步研究证实。

Primary myelofibrosis with thrombophilia as first symptom combined with thalassemia and Gilbert syndrome:A case report

BACKGROUND A 46-year-old Han man first had sigmoid sinus and transverse sinus venous thrombosis at the age of 42.At the age of 44,he once again developed thrombosis.Genetic testing showed heterozygous SERPINC1 mutation,bone marrow biopsy showed fibrosis grade 1(MF-1),and JAK2 V617F mutation was positive,accompanied by UGT1A1 mutation andβ-thalassemia gene mutation.CASE SUMMARY A 46-year-old Han man was first found to have sigmoid sinus and transverse sinus venous thrombosis at the age of 42 but had no individual or family thrombosis history,and he had been regularly taking warfarin anticoagulant therapy for a long period of time.At the age of 44,venous thrombosis reappeared in parts of the intrahepatic vein,main portal vein,splenic vein,and superior mesenteric vein,and his spleen was obviously enlarged.He had a history of jaundice for many years,and genetic testing revealed that he carried a heterozygous SERPINC1 mutation.Bone marrow biopsy showed multifocal fibrous tissue hyperplasia among trabeculae and focal fibrosis.He was positive for the JAK2 V617F mutation.At the same time,UGT1A1 andβ-thalassemia gene mutations existed,and a SERPINC1 mutation and UGT1A1 mutation were both found in his parents.CONCLUSION The patient in this case had thrombophilia as the primary symptom,JAK2V617-positive myeloproliferative neoplasm(MPN)was the main potential cause,and hereditary AT-III deficiency may have been one of multiple secondary causes.It remains to be determined whether UGT1A1 andβ-thalassemia gene mutations are related to thrombophilia.However,the clinical features of MPN in this patient were hidden,and the relevant clinical features of coexisting thalassemia and hereditary Gilbert syndrome,reported here for the first time domestically and abroad,were complicating factors,causing great difficulties for a clear diagnosis.Thus,when thrombophilia has been determined,it is necessary to screen the relevant latent problems overall.When the clinical features cannot be perfectly explained by one etiology,a relevant comprehensive examination should also be initiated from the perspective of multiple etiologies.

伴TRIM24/FGFR1和FGFR1/TRIM24融合基因阳性8p11骨髓增殖综合征1例

患者,男,71岁,2021年6月因"刺激性咳嗽1个月"住院治疗。因入院血常规显示"白细胞增高、贫血、血小板减少"而转入血液科。查体:贫血貌,全身未见皮疹、瘀点,浅表淋巴结不大,双肺呼吸音稍粗,心律齐、无杂音,腹软,肝脾肋缘下未触及。血常规:WBC 22.63×10^(9)/L,HGB 97 g/L,PLT 28×10^(9)/L,中性粒细胞11.61×10^(9)/L,淋巴细胞1.58×10^(9)/L,单核细胞6×10^(9)/L,嗜酸性粒细胞1.59×10^(9)/L;肝肾功能、血电解质、心肌酶正常,肿瘤标志物正常,ANA、dsDNA、ENA、ANCA阴性,血清IgE阴性。腹部B超:肝脾不大。胸部CT:两下肺散在微小结节。骨髓象:有核细胞增生明显活跃,粒系占72.5%,各阶段细胞均可见,早幼粒细胞比值增高,部分粒细胞可见核浆发育不平衡、内外浆、空泡,可见少数巨幼变、巨多分叶及假P-H畸形细胞,嗜酸性粒细胞占30%,易见幼稚嗜酸性粒细胞,嗜碱性粒细胞可见;红系占16.5%,以中晚幼红细胞为主,可见核固缩、胞浆量少,偶见花瓣核、嗜碱性点彩幼红细胞,成熟红细胞大小不等;全片巨核细胞14个,其中裸巨核3个,颗粒巨核11个,巨核细胞形态未见明显异常,淋巴细胞占1.5%;单核细胞占9%。