Uveitis and Multiple Sclerosis: Potential Common Causal Mutations

Uveitis, defined as inflammation of the uveal tract of the eye, is a leading cause of blindness and visual impairment throughout the world. The etiology of uveitis is complex, and autoimmunity plays a major role in its pathogenesis. Intermediate uveitis (IU), a subtype of ocular inflammation, has be...

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Fecha de publicación:: 2019

Institución:: Universidad del Rosario

Repositorio:: Repositorio EdocUR - U. Rosario

Idioma:: eng

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dc.title.spa.fl_str_mv	Uveitis and Multiple Sclerosis: Potential Common Causal Mutations
title	Uveitis and Multiple Sclerosis: Potential Common Causal Mutations
spellingShingle	Uveitis and Multiple Sclerosis: Potential Common Causal Mutations B cell activating factor Adolescent Adult Article BAFF gene Child Comorbidity Controlled study CPAMD8 gene DGKI gene Disease association Female Gene Gene expression Gene mutation Gene segregation Genetic analysis Genetic linkage GNGT1 gene Heterozygosity Homozygosity Human Intermediate uveitis Male Minimal critical region Multiple sclerosis Pathogenesis School child TNFRSF10A gene Whole exome sequencing Young adult Complication Diagnostic imaging Genetics Multiple sclerosis Mutation Pedigree Procedures Uveitis Child Female Humans Male Multiple Sclerosis Mutation Pedigree Uveitis Whole Exome Sequencing Young Adult Genetics Multiple sclerosis Mutations Pedigree Uveitis Whole exome sequencing
title_short	Uveitis and Multiple Sclerosis: Potential Common Causal Mutations
title_full	Uveitis and Multiple Sclerosis: Potential Common Causal Mutations
title_fullStr	Uveitis and Multiple Sclerosis: Potential Common Causal Mutations
title_full_unstemmed	Uveitis and Multiple Sclerosis: Potential Common Causal Mutations
title_sort	Uveitis and Multiple Sclerosis: Potential Common Causal Mutations
dc.subject.keyword.spa.fl_str_mv	B cell activating factor Adolescent Adult Article BAFF gene Child Comorbidity Controlled study CPAMD8 gene DGKI gene Disease association Female Gene Gene expression Gene mutation Gene segregation Genetic analysis Genetic linkage GNGT1 gene Heterozygosity Homozygosity Human Intermediate uveitis Male Minimal critical region Multiple sclerosis Pathogenesis School child TNFRSF10A gene Whole exome sequencing Young adult Complication Diagnostic imaging Genetics Multiple sclerosis Mutation Pedigree Procedures Uveitis Child Female Humans Male Multiple Sclerosis Mutation Pedigree Uveitis Whole Exome Sequencing Young Adult Genetics Multiple sclerosis Mutations Pedigree Uveitis Whole exome sequencing
topic	B cell activating factor Adolescent Adult Article BAFF gene Child Comorbidity Controlled study CPAMD8 gene DGKI gene Disease association Female Gene Gene expression Gene mutation Gene segregation Genetic analysis Genetic linkage GNGT1 gene Heterozygosity Homozygosity Human Intermediate uveitis Male Minimal critical region Multiple sclerosis Pathogenesis School child TNFRSF10A gene Whole exome sequencing Young adult Complication Diagnostic imaging Genetics Multiple sclerosis Mutation Pedigree Procedures Uveitis Child Female Humans Male Multiple Sclerosis Mutation Pedigree Uveitis Whole Exome Sequencing Young Adult Genetics Multiple sclerosis Mutations Pedigree Uveitis Whole exome sequencing
description	Uveitis, defined as inflammation of the uveal tract of the eye, is a leading cause of blindness and visual impairment throughout the world. The etiology of uveitis is complex, and autoimmunity plays a major role in its pathogenesis. Intermediate uveitis (IU), a subtype of ocular inflammation, has been associated with systemic autoimmune disorders, specifically with multiple sclerosis (MS). This article reports a rare three-generation family with several members affected by IU (four siblings) and comorbid MS (two siblings fulfilling MS diagnostic criteria and a third sibling presenting some neurological symptoms). Based on the clinical findings, we captured and sequenced whole exomes of seven pedigree members (affected and unaffected). Using a recessive model of transmission with full penetrance, we applied genetic linkage analysis to define minimal critical regions (MCRs) in suggestive or nominal regions of linkage. In these MCRs, we defined functional (some pathogenic), novel, and rare mutations that segregated as homozygous in affected and heterozygous in unaffected family members. The genes harboring these mutations, including DGKI, TNFRSF10A, GNGT1, CPAMD8, and BAFF, which are expressed in both eye and brain tissues and/or are related to autoimmune diseases, provide new avenues to evaluate the inherited causes of these devastating autoimmune conditions. © 2019, The Author(s).
publishDate	2019
dc.date.created.spa.fl_str_mv	2019
dc.date.accessioned.none.fl_str_mv	2020-05-25T23:57:10Z
dc.date.available.none.fl_str_mv	2020-05-25T23:57:10Z
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dc.identifier.doi.none.fl_str_mv	https://doi.org/10.1007/s12035-019-1630-2
dc.identifier.issn.none.fl_str_mv	8937648
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dc.language.iso.spa.fl_str_mv	eng
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dc.relation.citationEndPage.none.fl_str_mv	8017
dc.relation.citationIssue.none.fl_str_mv	No. 12
dc.relation.citationStartPage.none.fl_str_mv	8008
dc.relation.citationTitle.none.fl_str_mv	Molecular Neurobiology
dc.relation.citationVolume.none.fl_str_mv	Vol. 56
dc.relation.ispartof.spa.fl_str_mv	Molecular Neurobiology, ISSN:8937648, Vol.56, No.12 (2019); pp. 8008-8017
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institution	Universidad del Rosario
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spelling	5170135560088a0d9e6-8ba0-4d54-bc18-0ba272dc7994d975d6cb-a9d8-4221-a9a9-3de14928a5ec816d71d0-99af-43c4-8828-a9f3a942d82b3e6825a2-5bf4-4efe-8757-67783a8f3c535fa71b03-8bc7-4e15-ad36-74d13d002e7af49c92d4-24bd-4038-8c36-09d01aa8e367e66f46c4-aef0-43bb-b17f-137724131dad6816832360597260019331819600105486106002020-05-25T23:57:10Z2020-05-25T23:57:10Z2019Uveitis, defined as inflammation of the uveal tract of the eye, is a leading cause of blindness and visual impairment throughout the world. The etiology of uveitis is complex, and autoimmunity plays a major role in its pathogenesis. Intermediate uveitis (IU), a subtype of ocular inflammation, has been associated with systemic autoimmune disorders, specifically with multiple sclerosis (MS). This article reports a rare three-generation family with several members affected by IU (four siblings) and comorbid MS (two siblings fulfilling MS diagnostic criteria and a third sibling presenting some neurological symptoms). Based on the clinical findings, we captured and sequenced whole exomes of seven pedigree members (affected and unaffected). Using a recessive model of transmission with full penetrance, we applied genetic linkage analysis to define minimal critical regions (MCRs) in suggestive or nominal regions of linkage. In these MCRs, we defined functional (some pathogenic), novel, and rare mutations that segregated as homozygous in affected and heterozygous in unaffected family members. The genes harboring these mutations, including DGKI, TNFRSF10A, GNGT1, CPAMD8, and BAFF, which are expressed in both eye and brain tissues and/or are related to autoimmune diseases, provide new avenues to evaluate the inherited causes of these devastating autoimmune conditions. © 2019, The Author(s).application/pdfhttps://doi.org/10.1007/s12035-019-1630-28937648https://repository.urosario.edu.co/handle/10336/22619engHumana Press Inc.8017No. 128008Molecular NeurobiologyVol. 56Molecular Neurobiology, ISSN:8937648, Vol.56, No.12 (2019); pp. 8008-8017https://www.scopus.com/inward/record.uri?eid=2-s2.0-85067029220&doi=10.1007%2fs12035-019-1630-2&partnerID=40&md5=5c91fcb0538de20d788bc5b5517414dcAbierto (Texto Completo)http://purl.org/coar/access_right/c_abf2instname:Universidad del Rosarioreponame:Repositorio Institucional EdocURB cell activating factorAdolescentAdultArticleBAFF geneChildComorbidityControlled studyCPAMD8 geneDGKI geneDisease associationFemaleGeneGene expressionGene mutationGene segregationGenetic analysisGenetic linkageGNGT1 geneHeterozygosityHomozygosityHumanIntermediate uveitisMaleMinimal critical regionMultiple sclerosisPathogenesisSchool childTNFRSF10A geneWhole exome sequencingYoung adultComplicationDiagnostic imagingGeneticsMultiple sclerosisMutationPedigreeProceduresUveitisChildFemaleHumansMaleMultiple SclerosisMutationPedigreeUveitisWhole Exome SequencingYoung AdultGeneticsMultiple sclerosisMutationsPedigreeUveitisWhole exome sequencingUveitis and Multiple Sclerosis: Potential Common Causal MutationsarticleArtículohttp://purl.org/coar/version/c_970fb48d4fbd8a85http://purl.org/coar/resource_type/c_6501de-la-Torre, AlejandraSilva-Aldana, Claudia T.Muñoz-Ortiz, JulianaPiñeros-Hernández, Laura B.Otero, OscarDomínguez, AlejandraFaciolince, León A.Arcos-Holzinger, MauricioMastronardi, ClaudioContreras Bravo, Nora ConstanzaRestrepo Fernández, Carlos MartínArcos-Burgos, MauricioORIGINALDe-la-Torre2019_Article_UveitisAndMultipleSclerosisPot.pdfapplication/pdf2825309https://repository.urosario.edu.co/bitstreams/3815020a-600b-4b2d-b214-b6e8b0aa0de1/downloadeab06b8951144a889abb34e28f238458MD51TEXTDe-la-Torre2019_Article_UveitisAndMultipleSclerosisPot.pdf.txtDe-la-Torre2019_Article_UveitisAndMultipleSclerosisPot.pdf.txtExtracted texttext/plain38211https://repository.urosario.edu.co/bitstreams/46881d95-f49d-445b-88ea-a11abd2115a9/download3d63ee61c7d28ad3abfbef7e76014a12MD52THUMBNAILDe-la-Torre2019_Article_UveitisAndMultipleSclerosisPot.pdf.jpgDe-la-Torre2019_Article_UveitisAndMultipleSclerosisPot.pdf.jpgGenerated Thumbnailimage/jpeg4660https://repository.urosario.edu.co/bitstreams/3b61eb73-671b-4fdf-9c4b-72a34d4bd113/downloade9daaf1344e99cd72eebe4f8c738f9a3MD5310336/22619oai:repository.urosario.edu.co:10336/226192022-05-02 07:37:15.99999https://repository.urosario.edu.coRepositorio institucional EdocURedocur@urosario.edu.co

Uveitis and Multiple Sclerosis: Potential Common Causal Mutations

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