Wang D Y, Zhang Y M, Che F Y, Chu J P, Zhang L Y, Li H, Liu B L, Yao Z Y, Zhao Y W
Department of Cardiology, Xi'an Children's Hospital, Shaanxi Institute for Pediatric Diseases, Xi'an Key Laboratory of Children's Health and Diseases, Xi'an 710003, China.
Department of PICU, Xi'an Children's Hospital, Xi'an 710003, China.
Zhonghua Er Ke Za Zhi. 2020 Feb 2;58(2):101-106. doi: 10.3760/cma.j.issn.0578-1310.2020.02.007.
To analyze the genetic characteristics of a five generations pedigree with homozygous familial hypercholesterolemia (HoFH). Prospective study. Twenty family members included a proband diagnosed as familial hyperlipidemia at the cardiology Department of Xi'an Children's Hospital in October 2018 were research object. Clinical data were collected. Genome DNAs were extracted. Whole exons sequencing was performed on the proband using target capture next generation sequencing. Candidate gene mutation sites identified by bioinformatics were verified by Sanger sequencing in the family members. The genotype-phenotype correlation of the pedigree was analyzed between heterozygous mutation carriers and non-carriers. The proband was a 7-years and 10-month-old boy. He was born with a roundgreen bean size yellow skin protuberance in the skin of the coccyx. Since the age of 3-4 years old, xanthoma-like lesions with a diameter of 0.5-1.5 cm gradually appeared in the skin of bilateral elbow joints, knee joints and Achilles tendon. The height, weight and intellectual development of the child were the same as those of normal children at the same age. No similar xanthoma-like lesion was found in the other family members. The proband's total cholesterol (TC) reached 18.16-21.24 mmol/L, and his low density lipoproteincholesterol (LDL-C) was 14.08-15.51 mmol/L. Carotid ultrasonography showed diffuse sclerotic plaques in bilateral carotid and vertebral arteries, and color Doppler echocardiography revealed aortic valve thickening and calcification. Gene testing identified that the proband carried a homozygous mutation C. 418G>A (p. E140K) in LDLR gene inherited from his parents who had a consanguineous marriage and carried a heterozygous mutation of LDLR-E140K, respectively.The TC, LDL-C and apolipoproteinB (ApoB) of LDLR-E140K gene heterozygous carriers ((8.40±0.13), (6.79±0.01) and (1.95±0.05) mmol/L, respectively) were significantly higher than those of non-carriers ((4.59±0.28), (3.35±0.39) and (0.86±0.10) mmol/L, 7.269, 4.595, 6.311, respectively, 0.05). LDLR-E140K gene homozygous mutation is first reported to be associated with most severe phenotype HoFH. The genotype-phenotype analysis of the pedigree shows that the clinical phenotype of the proband with homozygous mutation is the most serious, and all the heterozygous mutation carriers present with hypercholesterolemia phenotype. The investigation confirms that LDLR-E140K is the pathogenic variation of familial hyperlipidemia.
分析一个患有纯合子家族性高胆固醇血症(HoFH)的五代家系的遗传特征。前瞻性研究。以20名家庭成员为研究对象,其中先证者于2018年10月在西安市儿童医院心内科被诊断为家族性高脂血症。收集临床资料。提取基因组DNA。使用靶向捕获二代测序技术对先证者进行全外显子测序。通过生物信息学鉴定出的候选基因突变位点在家庭成员中用桑格测序法进行验证。分析该家系杂合突变携带者与非携带者之间的基因型-表型相关性。先证者为一名7岁10个月大的男孩。他出生时尾骨皮肤处有一个绿豆大小的黄色皮肤隆起。3-4岁起,双侧肘关节、膝关节及跟腱皮肤逐渐出现直径0.5-1.5厘米的黄色瘤样病变。该患儿的身高、体重及智力发育与同龄正常儿童相同。其他家庭成员未发现类似黄色瘤样病变。先证者总胆固醇(TC)达18.16-21.24毫摩尔/升,低密度脂蛋白胆固醇(LDL-C)为14.08-15.51毫摩尔/升。颈动脉超声显示双侧颈动脉和椎动脉弥漫性硬化斑块,彩色多普勒超声心动图显示主动脉瓣增厚及钙化。基因检测发现先证者携带一个来自其父母的LDLR基因纯合突变C.418G>A(p.E140K),其父母为近亲结婚,分别携带LDLR-E140K杂合突变。LDLR-E140K基因杂合携带者的TC、LDL-C和载脂蛋白B(ApoB)(分别为(8.40±0.13)、(6.79±0.01)和(1.95±0.05)毫摩尔/升)显著高于非携带者(分别为(4.59±0.28)、(3.35±0.39)和(0.86±0.10)毫摩尔/升,P值分别为7.269、4.595、6.311,均<0.05)。首次报道LDLR-E140K基因纯合突变与最严重的HoFH表型相关。该家系的基因型-表型分析表明,纯合突变先证者的临床表型最严重,所有杂合突变携带者均表现为高胆固醇血症表型。该研究证实LDLR-E140K是家族性高脂血症的致病变异。
