Xiao Ting, Xie Yue, Zhang Xin, Xu Ke, Zhang Xiaohui, Jin Zi-Bing, Li Yang
Beijing Ophthalmology & Visual Sciences Key Lab, Beijing Tongren Eye Center, Beijing Institute of Ophthalmology, Beijing Tongren Hospital, Capital Medical University, Beijing, China.
Front Cell Dev Biol. 2021 Feb 1;8:629994. doi: 10.3389/fcell.2020.629994. eCollection 2020.
Retinitis pigmentosa (RP) is the most common form of inherited retinal dystrophy, and 15-25% of RP is transmitted as an autosomal dominant (ad) trait. The objectives of this study were to establish the variant profile in a large cohort of adRP families and to elucidate the variant spectrum of each adRP gene in Chinese patients. A total of 138 probands clinically diagnosed with RP as a presumed autosomal dominant trait were recruited. All probands underwent ophthalmic examinations by specialists. A combination of molecular screening methods, including targeted next-generation sequencing, Sanger DNA sequencing, and multiplex ligation probe amplification assay, was used to detect variants. We identified heterozygous variants of 11 adRP genes in 73 probands, hemizygous, or heterozygous variants of X-linked RP genes in six patients, compound heterozygous variants of autosomal recessive RP genes in three pseudodominant families, and one heterozygous variant of one ad cone and rod dystrophy gene in one proband. One proband was found carrying both variants in and . The overall detection rate was 59.4% (82/138). We detected 72 distinct disease-causing variants involving 16 RP genes and one cone-rod dystrophy gene; 33 of these variants have not been reported previously. Disease-causing variants were identified in the adRP genes in 52.9% of the families, followed by 4.3% in the X-linked RP genes, and 2.2% in the autosomal recessive genes. The most frequent mutant genes were , and , which explained up to 78.0% of the genetically diagnosed families. Most of the variants identified in adRP genes were missense, and copy number variations were common (7/20) in the gene. We established the profile of the mutated genes and the variant spectrum of adRP genes in a large cohort of Chinese patients, providing essential information for genetic counseling and future development of therapeutics for retinal dystrophy inherited as a dominant trait.
视网膜色素变性(RP)是遗传性视网膜营养不良最常见的形式,15% - 25%的RP以常染色体显性(ad)性状遗传。本研究的目的是确定一大群常染色体显性RP家系中的变异谱,并阐明中国患者中每个常染色体显性RP基因的变异谱。共招募了138名临床诊断为RP且推测为常染色体显性性状的先证者。所有先证者均由专科医生进行眼科检查。采用包括靶向二代测序、桑格DNA测序和多重连接探针扩增分析在内的分子筛查方法组合来检测变异。我们在73名先证者中鉴定出11个常染色体显性RP基因的杂合变异,在6名患者中鉴定出X连锁RP基因的半合子或杂合变异,在3个假显性家系中鉴定出常染色体隐性RP基因的复合杂合变异,在1名先证者中鉴定出1个常染色体显性视锥视杆营养不良基因的杂合变异。发现1名先证者同时携带 和 的变异。总体检出率为59.4%(82/138)。我们检测到72个涉及16个RP基因和1个视锥视杆营养不良基因的不同致病变异;其中33个变异此前未被报道。在52.9%的家系中鉴定出常染色体显性RP基因的致病变异,其次是X连锁RP基因中的4.3%,以及常染色体隐性基因中的2.2%。最常见的突变基因是 、 和 ,它们在基因诊断的家系中占比高达78.0%。在常染色体显性RP基因中鉴定出的大多数变异为错义变异,且 基因中常见拷贝数变异(7/20)。我们确定了一大群中国患者中突变基因的谱以及常染色体显性RP基因的变异谱,为视网膜营养不良常染色体显性遗传的遗传咨询和未来治疗发展提供了重要信息。
Zotero 插件
