目的:探寻精子鞭毛多发形态异常(MMAF)可能的致病基因。方法:通过对1例典型的MMAF患者进行全外显子组测序(WES),分析可能的致病基因;运用扫描电镜和透射电镜观察MMAF患者精液样本,明确其鞭毛超微结构特点;通过精子免疫荧光技术分析cilia...目的:探寻精子鞭毛多发形态异常(MMAF)可能的致病基因。方法:通过对1例典型的MMAF患者进行全外显子组测序(WES),分析可能的致病基因;运用扫描电镜和透射电镜观察MMAF患者精液样本,明确其鞭毛超微结构特点;通过精子免疫荧光技术分析cilia and flagella-associated protein 65(CFAP65)在精子发生过程中的表达模式。结果:该例患者存在CFAP65基因的一个纯合致病性突变c.2675G>A(p.Trp892*);扫描电镜发现该患者精子具有典型的MMAF特征,即表现为无尾,折尾,卷尾,短尾或不规则尾巴;透射电镜发现患者精子鞭毛"9+2"结构缺失和紊乱:精子鞭毛纤维鞘组装异常,伴有中心微管缺失和动力蛋白臂缺失。细胞免疫荧光提示该CFAP65基因在小鼠各级生殖细胞均有表达。结论:CFAP65基因参与了精子鞭毛结构的组装,其突变可引起MMAF表型而导致男性不育。展开更多
Purpose Fundus autofluorescence is due to accumulation of lipofuscin in the retinal pigment ep ithelium(RPE)resulting from incomplete digestion of N-retinylidene-phosphatidyl-ethanolamine from shed photorecep tor oute...Purpose Fundus autofluorescence is due to accumulation of lipofuscin in the retinal pigment ep ithelium(RPE)resulting from incomplete digestion of N-retinylidene-phosphatidyl-ethanolamine from shed photorecep tor outer segment discs.Alteration in autofluorescence reflects changes in lipofuscin content of the RPE.Mutations on both alleles of RPE65result in absent or largely decrease d formation of rhodopsin,due to a defect in alltrans retinol is omerization in the RPE.Autofluorescence could therefore b e altered.This study was conducted to evaluate fundus autofl uorescence in patients with early-onset severe retinal dystrophy(EOSRD,or ear-ly-onset rod-cone dystrophy)associated with mutations on both alleles of RPE65.Design Case se ries.Participants and controls Ten 10-to 55-year-old p atients with EOSRD and compound heterozygous or homozy gous mutations in RPE65.For comparison,6heterozygous parents and 2patients with other forms of EOSRD we re examined.Methods Participants underwent,in addition to standard clinical and electrophysiological examination,autofluores-cence imaging using a confocal scanning laser ophthalmo-scope.Three of the patients were als o examined by optical coherence tomography(OCT)to evaluate the status of retinal degeneration.Mutations in7patients have been reported previously;the other pati ents were investigated by polymerase chain reaction-single-strand conformation poly-morphism and direct sequencing for mutations in RPE65and lecithin retinol acyltransfera se(LRAT).Main outcome measures Fundus autofluorescence a nd OCT.Results Ab-sent or minimal autofluorescence wa s found in all patients with compound heterozygous or homozygous RPE65muta-tions.Autofluorescence was normal in the heterozygous parents.Autofluorescence was present in 2children with EOSRD not associated with mutations in RPE65or LRAT,another gene involved in retinol recycling.Optical coher-ence tomography in younger patients revealed an intraretinal appearance similar to that of their h ealthy,heterozygous parents.Conclusions Lack of autofl uorescence in patients with EOSRD associated with mutation s in RPE65is in ac-cordance with the biochemical defect and can be used as a clinical marker of this genotype.Optical coherence tomog-raphy results in younger patients wo uld indicate still viable photoreceptors despite the absence of autofluorescence.展开更多
文摘目的:探寻精子鞭毛多发形态异常(MMAF)可能的致病基因。方法:通过对1例典型的MMAF患者进行全外显子组测序(WES),分析可能的致病基因;运用扫描电镜和透射电镜观察MMAF患者精液样本,明确其鞭毛超微结构特点;通过精子免疫荧光技术分析cilia and flagella-associated protein 65(CFAP65)在精子发生过程中的表达模式。结果:该例患者存在CFAP65基因的一个纯合致病性突变c.2675G>A(p.Trp892*);扫描电镜发现该患者精子具有典型的MMAF特征,即表现为无尾,折尾,卷尾,短尾或不规则尾巴;透射电镜发现患者精子鞭毛"9+2"结构缺失和紊乱:精子鞭毛纤维鞘组装异常,伴有中心微管缺失和动力蛋白臂缺失。细胞免疫荧光提示该CFAP65基因在小鼠各级生殖细胞均有表达。结论:CFAP65基因参与了精子鞭毛结构的组装,其突变可引起MMAF表型而导致男性不育。
文摘Purpose Fundus autofluorescence is due to accumulation of lipofuscin in the retinal pigment ep ithelium(RPE)resulting from incomplete digestion of N-retinylidene-phosphatidyl-ethanolamine from shed photorecep tor outer segment discs.Alteration in autofluorescence reflects changes in lipofuscin content of the RPE.Mutations on both alleles of RPE65result in absent or largely decrease d formation of rhodopsin,due to a defect in alltrans retinol is omerization in the RPE.Autofluorescence could therefore b e altered.This study was conducted to evaluate fundus autofl uorescence in patients with early-onset severe retinal dystrophy(EOSRD,or ear-ly-onset rod-cone dystrophy)associated with mutations on both alleles of RPE65.Design Case se ries.Participants and controls Ten 10-to 55-year-old p atients with EOSRD and compound heterozygous or homozy gous mutations in RPE65.For comparison,6heterozygous parents and 2patients with other forms of EOSRD we re examined.Methods Participants underwent,in addition to standard clinical and electrophysiological examination,autofluores-cence imaging using a confocal scanning laser ophthalmo-scope.Three of the patients were als o examined by optical coherence tomography(OCT)to evaluate the status of retinal degeneration.Mutations in7patients have been reported previously;the other pati ents were investigated by polymerase chain reaction-single-strand conformation poly-morphism and direct sequencing for mutations in RPE65and lecithin retinol acyltransfera se(LRAT).Main outcome measures Fundus autofluorescence a nd OCT.Results Ab-sent or minimal autofluorescence wa s found in all patients with compound heterozygous or homozygous RPE65muta-tions.Autofluorescence was normal in the heterozygous parents.Autofluorescence was present in 2children with EOSRD not associated with mutations in RPE65or LRAT,another gene involved in retinol recycling.Optical coher-ence tomography in younger patients revealed an intraretinal appearance similar to that of their h ealthy,heterozygous parents.Conclusions Lack of autofl uorescence in patients with EOSRD associated with mutation s in RPE65is in ac-cordance with the biochemical defect and can be used as a clinical marker of this genotype.Optical coherence tomog-raphy results in younger patients wo uld indicate still viable photoreceptors despite the absence of autofluorescence.