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   Mutations in or near the transmembrane domain alter PMEL amyloid formation from functional to pathogenic  
   
نویسنده watt b. ,tenza d. ,lemmon m.a. ,kerje s. ,raposo g. ,andersson l. ,marks m.s.
منبع plos genetics - 2011 - دوره : 7 - شماره : 9
چکیده    Pmel is a pigment cell-specific protein that forms physiological amyloid fibrils upon which melanins ultimately deposit in the lumen of the pigment organelle,the melanosome. whereas hypomorphic pmel mutations in several species result in a mild pigment dilution that is inherited in a recessive manner,pmel alleles found in the dominant white (dw) chicken and silver horse (hosi)-which bear mutations that alter the pmel transmembrane domain (tmd) and that are thus outside the amyloid core-are associated with a striking loss of pigmentation that is inherited in a dominant fashion. here we show that the dw and hosi mutations alter pmel tmd oligomerization and/or association with membranes,with consequent formation of aberrantly packed fibrils. the aberrant fibrils are associated with a loss of pigmentation in cultured melanocytes,suggesting that they inhibit melanin production and/or melanosome integrity. a secondary mutation in the smoky chicken,which reverts the dominant dw phenotype,prevents the accumulation of pmel in fibrillogenic compartments and thus averts dw-associated pigment loss; a secondary mutation found in the dun chicken likely dampens a hosi-like dominant mutation in a similar manner. we propose that the dw and hosi mutations alter the normally benign amyloid to a pathogenic form that antagonizes melanosome function,and that the secondary mutations found in the smoky and dun chickens revert or dampen pathogenicity by functioning as null alleles,thus preventing the formation of aberrant fibrils. we speculate that pmel mutations can model the conversion between physiological and pathological amyloid. © 2011 watt et al.
آدرس department of pathology and laboratory medicine and department of physiology,university of pennsylvania,philadelphia,pa,united states,cell and molecular biology graduate group,university of pennsylvania,philadelphia,pa, United States, institut curie,centre de recherche,paris,france,cnrs,umr-144,paris, France, department of biochemistry and biophysics,university of pennsylvania,philadelphia,pa, United States, science for life laboratory,department of medical biochemistry and microbiology,uppsala university,uppsala, Sweden, institut curie,centre de recherche,paris,france,cnrs,umr-144,paris, France, science for life laboratory,department of medical biochemistry and microbiology,uppsala university,uppsala,sweden,department of animal breeding and genetics,swedish university of agricultural sciences,uppsala, Sweden, department of pathology and laboratory medicine and department of physiology,university of pennsylvania,philadelphia,pa,united states,cell and molecular biology graduate group,university of pennsylvania,philadelphia,pa, United States
 
     
   
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