Whole exome sequencing (WES) to elucidate the molecular basis of cardiac disease

Mastantuono, Elisa

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Original title:: Whole exome sequencing (WES) to elucidate the molecular basis of cardiac disease
Translated title:: Gesamt-Exom-Sequenzierung (WES) zur Aufklärung der molekularen Ursache von Herzerkrankungen
Author:: Mastantuono, Elisa
Year:: 2018
Document type:: Dissertation
Faculty/School:: Fakultät für Medizin
Advisor:: Meitinger, Thomas (Prof. Dr.)
Referee:: Laugwitz, Karl-Ludwig (Prof. Dr.); Schunkert, Heribert (Prof. Dr.)
Language:: en
Subject group:: MED Medizin
Keywords:: Whole exome sequencing (WES), arrhythmogenic right ventricular cardiomyopathy (ARVC), long QT syndrome (LQTS), mitochondrial cardiomyopathy, hypoplastic left heart syndrome (HLHS)
Translated keywords:: Exom-Sequenzierung, arrhythmogene rechtsventrikuläre kardiomyopathie, Long-QT-Syndrom, mitochondriale Kardiomyopathie, hypoplastisches Linksherzsyndrom
TUM classification:: MED 900d
Abstract:: Genome-wide screening using WES in patients with cardiac disease identified CDH2 and MYH10 as new candidates for arrhythmogenic cardiomyopathy and strengthened the hypothesis of involvement of cell adhesion network in its pathogenesis, discovered gene defects in primary cilium pathway in hypoplastic left heart syndrome, and provided molecular diagnosis for mitochondrial cardiomyopathy cases. The latter holds promise for a personalised treatment of ACAD9 patients using riboflavin supplementation. «
Genome-wide screening using WES in patients with cardiac disease identified CDH2 and MYH10 as new candidates for arrhythmogenic cardiomyopathy and strengthened the hypothesis of involvement of cell adhesion network in its pathogenesis, discovered gene defects in primary cilium pathway in hypoplastic left heart syndrome, and provided molecular diagnosis for mitochondrial cardiomyopathy cases. The latter holds promise for a personalised treatment of ACAD9 patients using riboflavin supplementation.... »
Translated abstract:: WES Untersuchungen in Patienten mit Herzinsuffizienz identifizierte CDH2 und MYH10 als Kandidatengene für arrhythmogenen Kardiomyopathie was die Beteiligung des Zelladhäsionsnetzwerkes in der Pathogenese suggeriert, entschlüsselte Gendefekte im primären Ziliensignalweg, lieferte die molekulare Diagnose für Patienten mit mitochondrialer Kardiomyopathie. Letzteres ist wegweisend für eine personalisierte Behandlung von ACAD9 Patienten mit Riboflavinsupplementation.
WWW:: https://mediatum.ub.tum.de/?id=1402220
Date of submission:: 21.11.2017
Oral examination:: 14.03.2018
File size:: 6648623 bytes
Pages:: 160
Urn (citeable URL):: https://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:91-diss-20180314-1402220-1-9
Last change:: 19.10.2018
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mediaTUM Gesamtbestand Elektronische Prüfungsarbeiten School TUM School of Medicine and Health

mediaTUM Gesamtbestand Elektronische Prüfungsarbeiten Fachgebiet Medizin

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