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   Patterns of late gadolinium enhancement in Duchenne muscular dystrophy carriers  
   
نویسنده giglio v. ,puddu p.e. ,camastra g. ,sbarbati s. ,della sala s.w. ,ferlini a. ,gualandi f. ,ricci e. ,sciarra f. ,ansalone g. ,di gennaro m.
منبع journal of cardiovascular magnetic resonance - 2014 - دوره : 16 - شماره : 1
چکیده    Background: this study was designed to assess whether cardiovascular magnetic resonance imaging (cmr) in duchenne muscular dystrophy carriers (dmdc) may index any cell milieu elements of lv dysfunction and whether this cardiac phenotype may be related to genotype. the null hypothesis was that myocardial fibrosis,assessed by late gadolinium enhancement (lge),might be similarly accounted for in dmdc and gender and age-matched controls. methods. thirty dmdc patients had cmr and genotyping with 37 gender and age-matched controls. systolic and diastolic lv function was assessed by 2d-echocardiography. results: absolute and percent lge were higher in muscular symptomatic (sym) than asymptomatic (asy) dmdc (1.77 ± 0.27 vs 0.76 ± 0.17 ml; f = 19.6,p < 0.0001 and 1.86 ± 0.26% vs 0.68 ± 0.17%,f = 22.1,p < 0.0001,respectively). there was no correlation between lge and age. lge was seen most frequently in segments 5 and 6; segment 5 was involved in all asy-dmdc. subepicardial lge predominated,compared to the mid-myocardial one (11 out of 14 dmdc). lge was absent in the subendocardium. no correlations were seen between genotyping (type of mutation,gene region and protein domain),confined to the exon's study,and cardiac phenotype. conclusions: a typical myocardial lge-pattern location (lv segments 5 and 6) was a common finding in dmdc. lge was more frequently subepicardial plus midmyocardial in sym-dmdc,with normal lv systolic and diastolic function. no genotype-phenothype correlation was found. © 2014 giglio et al.; licensee biomed central ltd.
کلیدواژه Cardiovascular magnetic resonance; Duchenne muscular dystrophy carriers; Genetics
آدرس center for neuromuscular disease,uildm,prospero santacroce st. 5,rome 00167,italy,cardiology division,icu,ospedale san paolo,civitavecchia,rome, Italy, department of cardiovascular,laboratory of biotechnologies applied to cardiovascular diseases,university of rome,rome, Italy, cardiology division,icu,ospedale madre giuseppina vannini,rome, Italy, radiology department,ospedale madre giuseppina vannini,rome, Italy, radiology department,ospedale madre giuseppina vannini,rome, Italy, department of medical science,section of medical genetics,university of ferrara,ferrara, Italy, department of medical science,section of medical genetics,university of ferrara,ferrara, Italy, center for neuromuscular disease,uildm,prospero santacroce st. 5,rome 00167,italy,neurology institute,catholic university,rome, Italy, center for neuromuscular disease,uildm,prospero santacroce st. 5,rome 00167, Italy, cardiology division,icu,ospedale madre giuseppina vannini,rome, Italy, cardiology division,icu,ospedale san paolo,civitavecchia,rome, Italy
 
     
   
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