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   Evolution meets disease: Penetrance and functional epistasis of mitochondrial tRNA mutations  
   
نویسنده moreno-loshuertos r. ,ferrín g. ,acín-pérez r. ,gallardo m.e. ,viscomi c. ,pérez-martos a. ,zeviani m. ,fernández-silva p. ,enríquez j.a.
منبع plos genetics - 2011 - دوره : 7 - شماره : 4
چکیده    About half of the mitochondrial dna (mtdna) mutations causing diseases in humans occur in trna genes. particularly intriguing are those pathogenic trna mutations than can reach homoplasmy and yet show very different penetrance among patients. these mutations are scarce and,in addition to their obvious interest for understanding human pathology,they can be excellent experimental examples to model evolution and fixation of mitochondrial trna mutations. to date,the only source of this type of mutations is human patients. we report here the generation and characterization of the first mitochondrial trna pathological mutation in mouse cells,an m.3739g>a transition in the mitochondrial mt-ti gene. this mutation recapitulates the molecular hallmarks of a disease-causing mutation described in humans,an m.4290t>c transition affecting also the human mt-ti gene. we could determine that the pathogenic molecular mechanism,induced by both the mouse and the human mutations,is a high frequency of abnormal folding of the trnaile that cannot be charged with isoleucine. we demonstrate that the cells harboring the mouse or human mutant trna have exacerbated mitochondrial biogenesis triggered by an increase in mitochondrial ros production as a compensatory response. we propose that both the nature of the pathogenic mechanism combined with the existence of a compensatory mechanism can explain the penetrance pattern of this mutation. this particular behavior can allow a scenario for the evolution of mitochondrial trnas in which the fixation of two alleles that are individually deleterious can proceed in two steps and not require the simultaneous mutation of both. © 2011 moreno-loshuertos et al.
آدرس departamento de bioquímica y biología molecular y celular,universidad de zaragoza,zaragoza, Spain, departamento de bioquímica y biología molecular y celular,universidad de zaragoza,zaragoza,spain,unidad de investigación,hospital universitario reina sofía,córdoba, Spain, departamento de bioquímica y biología molecular y celular,universidad de zaragoza,zaragoza,spain,department of neurology and neuroscience,weill medical college of cornell university,ithaca,ny, United States, departamento de bioquímica,instituto de investigaciones biomédicas alberto sols,facultad de medicina,csic-universidad autónoma de madrid,ciberer,isciii,madrid, Spain, division of molecular neurogenetics,istituto neurologico carlo besta,milano, Italy, departamento de bioquímica y biología molecular y celular,universidad de zaragoza,zaragoza, Spain, division of molecular neurogenetics,istituto neurologico carlo besta,milano, Italy, departamento de bioquímica y biología molecular y celular,universidad de zaragoza,zaragoza, Spain, departamento de bioquímica y biología molecular y celular,universidad de zaragoza,zaragoza,spain,regenerative cardiology department,centro nacional de investigaciones cardiovasculares carlos iii,madrid, Spain
 
     
   
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