MIR204 n.37C>T variant as a cause of chorioretinal dystrophy variably associated with iris coloboma, early‐onset cataracts and congenital glaucoma
Four members of a three‐generation Czech family with early‐onset chorioretinal dystrophy were shown to be heterozygous carriers of the n.37C>T in MIR204. The identification of this previously reported pathogenic variant confirms the existence of a distinct clinical entity caused by a sequence cha...
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| Veröffentlicht in: | Clinical genetics 2023-10, Vol.104 (4), p.418-426 |
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| creator | Jedlickova, Jana Vajter, Marie Barta, Tomas Black, Graeme C. M. Perveen, Rahat Mares, Jan Fichtl, Marek Kousal, Bohdan Dudakova, Lubica Liskova, Petra |
| description | Four members of a three‐generation Czech family with early‐onset chorioretinal dystrophy were shown to be heterozygous carriers of the n.37C>T in MIR204. The identification of this previously reported pathogenic variant confirms the existence of a distinct clinical entity caused by a sequence change in MIR204. Chorioretinal dystrophy was variably associated with iris coloboma, congenital glaucoma, and premature cataracts extending the phenotypic range of the condition. In silico analysis of the n.37C>T variant revealed 713 novel targets. Additionally, four family members were shown to be affected by albinism resulting from biallelic pathogenic OCA2 variants. Haplotype analysis excluded relatedness with the original family reported to harbour the n.37C>T variant in MIR204. Identification of a second independent family confirms the existence of a distinct MIR204‐associated clinical entity and suggests that the phenotype may also involve congenital glaucoma. |
| doi_str_mv | 10.1111/cge.14391 |
| format | Article |
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M. ; Perveen, Rahat ; Mares, Jan ; Fichtl, Marek ; Kousal, Bohdan ; Dudakova, Lubica ; Liskova, Petra</creator><creatorcontrib>Jedlickova, Jana ; Vajter, Marie ; Barta, Tomas ; Black, Graeme C. M. ; Perveen, Rahat ; Mares, Jan ; Fichtl, Marek ; Kousal, Bohdan ; Dudakova, Lubica ; Liskova, Petra</creatorcontrib><description>Four members of a three‐generation Czech family with early‐onset chorioretinal dystrophy were shown to be heterozygous carriers of the n.37C>T in MIR204. The identification of this previously reported pathogenic variant confirms the existence of a distinct clinical entity caused by a sequence change in MIR204. Chorioretinal dystrophy was variably associated with iris coloboma, congenital glaucoma, and premature cataracts extending the phenotypic range of the condition. In silico analysis of the n.37C>T variant revealed 713 novel targets. Additionally, four family members were shown to be affected by albinism resulting from biallelic pathogenic OCA2 variants. Haplotype analysis excluded relatedness with the original family reported to harbour the n.37C>T variant in MIR204. Identification of a second independent family confirms the existence of a distinct MIR204‐associated clinical entity and suggests that the phenotype may also involve congenital glaucoma.</description><identifier>ISSN: 0009-9163</identifier><identifier>EISSN: 1399-0004</identifier><identifier>DOI: 10.1111/cge.14391</identifier><identifier>PMID: 37321975</identifier><language>eng</language><publisher>Oxford, UK: Blackwell Publishing Ltd</publisher><subject>Albinism ; Cataracts ; chorioretinal dystrophy ; coloboma ; congenital glaucoma ; Dystrophy ; Glaucoma ; Haplotypes ; Iris ; MIR204 ; OCA2 ; Phenotypes ; premature cataract</subject><ispartof>Clinical genetics, 2023-10, Vol.104 (4), p.418-426</ispartof><rights>2023 The Authors. published by John Wiley & Sons Ltd.</rights><rights>2023 The Authors. Clinical Genetics published by John Wiley & Sons Ltd.</rights><rights>2023. 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Chorioretinal dystrophy was variably associated with iris coloboma, congenital glaucoma, and premature cataracts extending the phenotypic range of the condition. In silico analysis of the n.37C>T variant revealed 713 novel targets. Additionally, four family members were shown to be affected by albinism resulting from biallelic pathogenic OCA2 variants. Haplotype analysis excluded relatedness with the original family reported to harbour the n.37C>T variant in MIR204. Identification of a second independent family confirms the existence of a distinct MIR204‐associated clinical entity and suggests that the phenotype may also involve congenital glaucoma.</description><subject>Albinism</subject><subject>Cataracts</subject><subject>chorioretinal dystrophy</subject><subject>coloboma</subject><subject>congenital glaucoma</subject><subject>Dystrophy</subject><subject>Glaucoma</subject><subject>Haplotypes</subject><subject>Iris</subject><subject>MIR204</subject><subject>OCA2</subject><subject>Phenotypes</subject><subject>premature cataract</subject><issn>0009-9163</issn><issn>1399-0004</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2023</creationdate><recordtype>article</recordtype><sourceid>24P</sourceid><sourceid>WIN</sourceid><recordid>eNpdkc1OGzEUha0KVALtoi9QWeqGRSf4J7bjTSUUUUACIVV0Pbrj8SRGzji1PaDZ8QgseEKeBEOgC-7mXMufz5XvQegbJVNa6sgs7ZTOuKaf0IRyrStCyGwHTYroSlPJ99B-SjflyJXQn9EeV5xRrcQEPV6e_2FkhvspV4tf1_gWooM-Y0gYsIEhWRw6bFYhuhBtdj143I4px7BZjVu68WPBUzAOsm3xncsr7KJL2AQfmrCGn9hC9OPT_UPok83FNkMEk8uIvi1Uv7S9y8V46WEw5cEXtNuBT_brmx6gv79Prhdn1cXV6fni-KLaMKZp1fF2biTnpmVKd0R1bC5nnFBFpGil0so0mpffQycFUCop60RDlTZWaWZFww_Q4dZ3E8O_waZcr10y1nvobRhSzeZMMcEkFQX98QG9CUMs23ihJGFUCC4L9f2NGpq1betNdGuIY_2-7wIcbYE75-34_56S-iXIugRZvwZZL05PXhv-DDkakCo</recordid><startdate>202310</startdate><enddate>202310</enddate><creator>Jedlickova, Jana</creator><creator>Vajter, Marie</creator><creator>Barta, Tomas</creator><creator>Black, Graeme C. 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M.</au><au>Perveen, Rahat</au><au>Mares, Jan</au><au>Fichtl, Marek</au><au>Kousal, Bohdan</au><au>Dudakova, Lubica</au><au>Liskova, Petra</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>MIR204 n.37C>T variant as a cause of chorioretinal dystrophy variably associated with iris coloboma, early‐onset cataracts and congenital glaucoma</atitle><jtitle>Clinical genetics</jtitle><addtitle>Clin Genet</addtitle><date>2023-10</date><risdate>2023</risdate><volume>104</volume><issue>4</issue><spage>418</spage><epage>426</epage><pages>418-426</pages><issn>0009-9163</issn><eissn>1399-0004</eissn><abstract>Four members of a three‐generation Czech family with early‐onset chorioretinal dystrophy were shown to be heterozygous carriers of the n.37C>T in MIR204. The identification of this previously reported pathogenic variant confirms the existence of a distinct clinical entity caused by a sequence change in MIR204. Chorioretinal dystrophy was variably associated with iris coloboma, congenital glaucoma, and premature cataracts extending the phenotypic range of the condition. In silico analysis of the n.37C>T variant revealed 713 novel targets. Additionally, four family members were shown to be affected by albinism resulting from biallelic pathogenic OCA2 variants. Haplotype analysis excluded relatedness with the original family reported to harbour the n.37C>T variant in MIR204. 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| subjects | Albinism Cataracts chorioretinal dystrophy coloboma congenital glaucoma Dystrophy Glaucoma Haplotypes Iris MIR204 OCA2 Phenotypes premature cataract |
| title | MIR204 n.37C>T variant as a cause of chorioretinal dystrophy variably associated with iris coloboma, early‐onset cataracts and congenital glaucoma |
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