FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2078046965> ?p ?o ?g. }

• W2078046965 endingPage "841" @default.
• W2078046965 startingPage "833" @default.
• W2078046965 abstract "Variations in the content and translatability of the poly(A) + RNA and mRNA molecules coding for myosin (M) were studied in the hind leg muscles of genetically dystrophic mice. The poly(A) + RNA content of total skeletal muscle failed to increase normally during progression of the disease. M mRNA, isolated from dystrophic murine muscle poly(A) + RNA, was mostly found to be associated with the 26S RNA species. The translation of M mRNA in an in vitro heterologous wheat germ system was lower at 8 and 16 weeks in the dystrophic group as compared with the controls. Analysis of the translation products via sodium dodecyl sulfate – polyacrylamide gel electrophoresis, autoradiography, and densitometric autoradiographic tracing demonstrated the gradual disappearance of a protein band corresponding to M, the major component of skeletal muscle. cDNA was synthesized, using M mRNA that was isolated and purified from normal and dystrophic mouse muscle as a template. Total radioactivity was measured in some cDNA fractions produced from normal and dystrophic mouse muscle, while other fractions were utilized for separation and sizing of cDNA by disc gel electrophoresis. The cDNA from normal muscle was hybridized with M mRNA from normal and 16-week-old dystrophic mouse muscles. The cDNA probe, hybridization experiments, and studies involving the content and synthesis of M mRNA suggest that murine muscular dystrophy elicited a shorter species of mRNA or shorter sequences of the same species of mRNA coding for M. Not all poly(A) + mRNA sequences coding for M, found in control mice, were present in their dystrophic counterparts. In conclusion, it appears that murine muscular dystrophy produces a shorter species of pre-M mRNA via decreased polynucleotide elongation." @default.
• W2078046965 created "2016-06-24" @default.
• W2078046965 creator A5056545869 @default.
• W2078046965 creator A5070381263 @default.
• W2078046965 creator A5071440017 @default.
• W2078046965 creator A5072866417 @default.
• W2078046965 creator A5078157438 @default.
• W2078046965 date "1987-09-01" @default.
• W2078046965 modified "2023-09-26" @default.
• W2078046965 title "Biochemical changes in progressive muscular dystrophy. XIV. Skeletal muscle myosin mRNA translatability in dystrophic mice" @default.
• W2078046965 cites W1970403529 @default.
• W2078046965 cites W2000924107 @default.
• W2078046965 cites W2002164128 @default.
• W2078046965 cites W2015028990 @default.
• W2078046965 cites W2054073262 @default.
• W2078046965 cites W2054220556 @default.
• W2078046965 cites W2100837269 @default.
• W2078046965 cites W2128330955 @default.
• W2078046965 cites W305244220 @default.
• W2078046965 cites W3111630834 @default.
• W2078046965 doi "https://doi.org/10.1139/o87-108" @default.
• W2078046965 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/2449899" @default.
• W2078046965 hasPublicationYear "1987" @default.
• W2078046965 type Work @default.
• W2078046965 sameAs 2078046965 @default.
• W2078046965 citedByCount "3" @default.
• W2078046965 crossrefType "journal-article" @default.
• W2078046965 hasAuthorship W2078046965A5056545869 @default.
• W2078046965 hasAuthorship W2078046965A5070381263 @default.
• W2078046965 hasAuthorship W2078046965A5071440017 @default.
• W2078046965 hasAuthorship W2078046965A5072866417 @default.
• W2078046965 hasAuthorship W2078046965A5078157438 @default.
• W2078046965 hasConcept C104317684 @default.
• W2078046965 hasConcept C105580179 @default.
• W2078046965 hasConcept C105702510 @default.
• W2078046965 hasConcept C116084860 @default.
• W2078046965 hasConcept C150194340 @default.
• W2078046965 hasConcept C153911025 @default.
• W2078046965 hasConcept C187882448 @default.
• W2078046965 hasConcept C2779030066 @default.
• W2078046965 hasConcept C2779959927 @default.
• W2078046965 hasConcept C54355233 @default.
• W2078046965 hasConcept C55493867 @default.
• W2078046965 hasConcept C67705224 @default.
• W2078046965 hasConcept C6997183 @default.
• W2078046965 hasConcept C86803240 @default.
• W2078046965 hasConceptScore W2078046965C104317684 @default.
• W2078046965 hasConceptScore W2078046965C105580179 @default.
• W2078046965 hasConceptScore W2078046965C105702510 @default.
• W2078046965 hasConceptScore W2078046965C116084860 @default.
• W2078046965 hasConceptScore W2078046965C150194340 @default.
• W2078046965 hasConceptScore W2078046965C153911025 @default.
• W2078046965 hasConceptScore W2078046965C187882448 @default.
• W2078046965 hasConceptScore W2078046965C2779030066 @default.
• W2078046965 hasConceptScore W2078046965C2779959927 @default.
• W2078046965 hasConceptScore W2078046965C54355233 @default.
• W2078046965 hasConceptScore W2078046965C55493867 @default.
• W2078046965 hasConceptScore W2078046965C67705224 @default.
• W2078046965 hasConceptScore W2078046965C6997183 @default.
• W2078046965 hasConceptScore W2078046965C86803240 @default.
• W2078046965 hasIssue "9" @default.
• W2078046965 hasLocation W20780469651 @default.
• W2078046965 hasLocation W20780469652 @default.
• W2078046965 hasOpenAccess W2078046965 @default.
• W2078046965 hasPrimaryLocation W20780469651 @default.
• W2078046965 hasRelatedWork W1969691270 @default.
• W2078046965 hasRelatedWork W2029766340 @default.
• W2078046965 hasRelatedWork W2042426634 @default.
• W2078046965 hasRelatedWork W2067544802 @default.
• W2078046965 hasRelatedWork W2078899906 @default.
• W2078046965 hasRelatedWork W2082895839 @default.
• W2078046965 hasRelatedWork W2091990958 @default.
• W2078046965 hasRelatedWork W2388047774 @default.
• W2078046965 hasRelatedWork W96471758 @default.
• W2078046965 hasRelatedWork W2185245252 @default.
• W2078046965 hasVolume "65" @default.
• W2078046965 isParatext "false" @default.
• W2078046965 isRetracted "false" @default.
• W2078046965 magId "2078046965" @default.
• W2078046965 workType "article" @default.