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   Detailed molecular characterization of a novel IDS exonic mutation associated with multiple pseudoexon activation  
   
نویسنده Grodecká L. ,Kováčová T. ,Kramárek M. ,Seneca S. ,Stouffs K. ,Laet C. De ,Majer F. ,Kršjaková T. ,Hujová P. ,Hrnčířová K. ,Souček P. ,Lissens W. ,Buratti E. ,Freiberger Tomas
منبع journal of molecular medicine - 2017 - دوره : 95 - شماره : 3 - صفحه:299 -309
چکیده    Mutations affecting splicing underlie the development of many human genetic diseases, but rather rarely through mechanisms of pseudoexon activation. here, we describe a novel c.1092t>a mutation in the iduronate-2-sulfatase (ids) gene detected in a patient with significantly decreased ids activity and a clinical diagnosis of mild mucopolysaccharidosis ii form. the mutation created an exonic de novo acceptor splice site and resulted in a complex splicing pattern with multiple pseudoexon activation in the patient’s fibroblasts. using an extensive series of minigene splicing experiments, we showed that the competition itself between the de novo and authentic splice site led to the bypass of the authentic one. this event then resulted in activation of several cryptic acceptor and donor sites in the upstream intron. as this was an unexpected and previously unreported mechanism of aberrant pseudoexon inclusion, we systematically analysed and disproved that the patient’s mutation induced any relevant change in surrounding splicing regulatory elements. interestingly, all pseudoexons included in the mature transcripts overlapped with the ids alternative terminal exon 7b suggesting that this sequence represents a key element in the ids pre-mrna architecture. these findings extend the spectrum of mechanisms enabling pseudoexon activation and underscore the complexity of mutation-induced splicing aberrations.
کلیدواژه Complex splicing aberration ,Splice site competition ,Pseudoexon ,De novo splice site ,IDS
آدرس Masaryk University, Czech Republic. Centre for Cardiovascular Surgery and Transplantation, Molecular Genetics Laboratory, Czech Republic, Masaryk University, Czech Republic. Centre for Cardiovascular Surgery and Transplantation, Molecular Genetics Laboratory, Czech Republic, Masaryk University, Czech Republic, UZ Brussel and Vrije Universiteit Brussel, Belgium, UZ Brussel and Vrije Universiteit Brussel, Belgium, University Children’s Hospital Queen Fabiola, Free University of Brussels (ULB), Nutrition and Metabolism Unit, Belgium, Charles University, Czech Republic, Masaryk University, Czech Republic, Centre for Cardiovascular Surgery and Transplantation, Molecular Genetics Laboratory, Czech Republic, Masaryk University, Czech Republic, Masaryk University, Czech Republic, UZ Brussel and Vrije Universiteit Brussel, Belgium, International Centre for Genetic Engineering and Biotechnology, Italy, Masaryk University, Czech Republic. Centre for Cardiovascular Surgery and Transplantation, Molecular Genetics Laboratory, Czech Republic. St. Anne’s University Hospital and Masaryk University, Czech Republic
 
     
   
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