FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W1781486281> ?p ?o ?g. }

• W1781486281 abstract "In the research described in this thesis, the trafficking of each CD23 isoform was studied in detail in both wild-type and mutant CD23 proteins, using an identical cell system and the same method of CD23 ligation for both isoforms. Confocal microscopic analysis demonstrated intracellular sorting differences to exist between the two isoforms, with CD23a utilising the endocytic pathway, and CD23b following both the endocytic and phagocytic pathways in a B-cell line. Site-directed mutagenesis was used to investigate a number of potentially key residues present in the unique N-terminal tail of each isoform. The serine groups at positions 7 and 5 in the CD23a and b isoforms, respectively, and the NNP tri-peptide motif in the b isoform were found to be necessary for accurate trafficking of these proteins. The discovery that the CD23 isoforms utilise different trafficking pathways corroborates the hypothesis that CD23a and CD23b may have functionally different roles.Current models of human CD23 signalling link the CD23a isoforms to a cAMP-generating pathway and the CD23b isoform to stimulation of inositol-1,4,5-trisphosphate production and calcium mobilisation. The ability of CD23 to transmit a signal within various cells and the fact it has a very short cytoplasmic tail, of only 23 amino acids and bereft of catalytic motifs, strongly suggests that CD23 may associate with other molecules involved in signal transduction. The divergence in the signalling pathways associated with each CD23 isoform has been attributed to the unique amino acids at the N-terminal cytoplasmic tails, as the remainder of the proteins are identical. However, there is no definitive evidence to link directly CD23 to any of these individual signalling pathways. The research presented in this thesis utilises the yeast two-hybrid assay to investigate binding partners for the N-terminal tail of CD23. Filamin A was identified as a potential interacting protein, and was found to interact with both the CD23a and CD23b isoforms. It is hypothesised that CD23 interacts with filamin A, which functions as an adaptor protein, to enable downstream responses to CD23 through connections to the appropriate signalling pathways in an isoform-specific manner." @default.
• W1781486281 created "2016-06-24" @default.
• W1781486281 creator A5007097798 @default.
• W1781486281 date "2001-01-01" @default.
• W1781486281 modified "2023-09-24" @default.
• W1781486281 title "Molecular analysis of human CD23 (Fc[epsilon]RII) protein isoform function" @default.
• W1781486281 hasPublicationYear "2001" @default.
• W1781486281 type Work @default.
• W1781486281 sameAs 1781486281 @default.
• W1781486281 citedByCount "0" @default.
• W1781486281 crossrefType "dissertation" @default.
• W1781486281 hasAuthorship W1781486281A5007097798 @default.
• W1781486281 hasConcept C104317684 @default.
• W1781486281 hasConcept C141105273 @default.
• W1781486281 hasConcept C159654299 @default.
• W1781486281 hasConcept C170493617 @default.
• W1781486281 hasConcept C190062978 @default.
• W1781486281 hasConcept C28005876 @default.
• W1781486281 hasConcept C34814297 @default.
• W1781486281 hasConcept C53345823 @default.
• W1781486281 hasConcept C54355233 @default.
• W1781486281 hasConcept C55493867 @default.
• W1781486281 hasConcept C62478195 @default.
• W1781486281 hasConcept C79747257 @default.
• W1781486281 hasConcept C86803240 @default.
• W1781486281 hasConcept C95444343 @default.
• W1781486281 hasConceptScore W1781486281C104317684 @default.
• W1781486281 hasConceptScore W1781486281C141105273 @default.
• W1781486281 hasConceptScore W1781486281C159654299 @default.
• W1781486281 hasConceptScore W1781486281C170493617 @default.
• W1781486281 hasConceptScore W1781486281C190062978 @default.
• W1781486281 hasConceptScore W1781486281C28005876 @default.
• W1781486281 hasConceptScore W1781486281C34814297 @default.
• W1781486281 hasConceptScore W1781486281C53345823 @default.
• W1781486281 hasConceptScore W1781486281C54355233 @default.
• W1781486281 hasConceptScore W1781486281C55493867 @default.
• W1781486281 hasConceptScore W1781486281C62478195 @default.
• W1781486281 hasConceptScore W1781486281C79747257 @default.
• W1781486281 hasConceptScore W1781486281C86803240 @default.
• W1781486281 hasConceptScore W1781486281C95444343 @default.
• W1781486281 hasLocation W17814862811 @default.
• W1781486281 hasOpenAccess W1781486281 @default.
• W1781486281 hasPrimaryLocation W17814862811 @default.
• W1781486281 hasRelatedWork W152231097 @default.
• W1781486281 hasRelatedWork W1653032956 @default.
• W1781486281 hasRelatedWork W1902341226 @default.
• W1781486281 hasRelatedWork W1987764898 @default.
• W1781486281 hasRelatedWork W2035569405 @default.
• W1781486281 hasRelatedWork W2118298665 @default.
• W1781486281 hasRelatedWork W2122618035 @default.
• W1781486281 hasRelatedWork W2181788579 @default.
• W1781486281 hasRelatedWork W2407260754 @default.
• W1781486281 hasRelatedWork W2523484231 @default.
• W1781486281 hasRelatedWork W2611281893 @default.
• W1781486281 hasRelatedWork W2734133921 @default.
• W1781486281 hasRelatedWork W2887142892 @default.
• W1781486281 hasRelatedWork W2914217294 @default.
• W1781486281 hasRelatedWork W73875301 @default.
• W1781486281 hasRelatedWork W2184327294 @default.
• W1781486281 hasRelatedWork W2197418714 @default.
• W1781486281 hasRelatedWork W2419858270 @default.
• W1781486281 hasRelatedWork W2499860680 @default.
• W1781486281 hasRelatedWork W2519439782 @default.
• W1781486281 isParatext "false" @default.
• W1781486281 isRetracted "false" @default.
• W1781486281 magId "1781486281" @default.
• W1781486281 workType "dissertation" @default.