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Mutations in mitochondrial DNA causing tubulointerstitial kidney disease
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نویسنده
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connor t.m. ,hoer s. ,mallett a. ,gale d.p. ,gomez-duran a. ,posse v. ,antrobus r. ,moreno p. ,sciacovelli m. ,frezza c. ,duff j. ,sheerin n.s. ,sayer j.a. ,ashcroft m. ,wiesener m.s. ,hudson g. ,gustafsson c.m. ,chinnery p.f. ,maxwell p.h.
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منبع
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plos genetics - 2017 - دوره : 13 - شماره : 3
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چکیده
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Tubulointerstitial kidney disease is an important cause of progressive renal failure whose aetiology is incompletely understood. we analysed a large pedigree with maternally inherited tubulointerstitial kidney disease and identified a homoplasmic substitution in the control region of the mitochondrial genome (m.547a>t). while mutations in mtdna coding sequence are a well recognised cause of disease affecting multiple organs,mutations in the control region have never been shown to cause disease. strikingly,our patients did not have classical features of mitochondrial disease. patient fibroblasts showed reduced levels of mitochondrial trnaphe,trnaleu1and reduced mitochondrial protein translation and respiration. mitochondrial transfer demonstrated mitochondrial transmission of the defect and in vitro assays showed reduced activity of the heavy strand promoter. we also identified further kindreds with the same phenotype carrying a homoplasmic mutation in mitochondrial trnaphe(m.616t>c). thus mutations in mitochondrial dna can cause maternally inherited renal disease,likely mediated through reduced function of mitochondrial trnaphe. © 2017 connor et al.
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آدرس
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oxford kidney unit,churchill hospital,oxford, United Kingdom, cambridge institute for medical research,university of cambridge, United Kingdom, kidney health service,royal brisbane and women’s hospital,school of medicine,the university of queensland, Australia, ucl centre for nephrology,royal free hospital,london, United Kingdom, mrc-mitochondrial biology unit,university of cambridge, United Kingdom, institute of biomedicine,university of gothenburg, Sweden, cambridge institute for medical research,university of cambridge, United Kingdom, cambridge institute for medical research,university of cambridge, United Kingdom, mrc cancer unit,university of cambridge, United Kingdom, mrc cancer unit,university of cambridge, United Kingdom, institute of genetic medicine,international centre for life,newcastle university,newcastle upon tyne, United Kingdom, institute of cellular medicine,newcastle university,newcastle upon tyne, United Kingdom, institute of genetic medicine,international centre for life,newcastle university,newcastle upon tyne, United Kingdom, department of medicine,university of cambridge, United Kingdom, department of nephrology and hypertension,friedrich-alexander university erlangen-nürnberg,erlangen, Germany, institute of genetic medicine,international centre for life,newcastle university,newcastle upon tyne, United Kingdom, institute of biomedicine,university of gothenburg, Sweden, mrc-mitochondrial biology unit,university of cambridge, United Kingdom, school of clinical medicine,cambridge university,cambridge, United Kingdom
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Authors
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