| Article ID | Journal | Published Year | Pages | File Type | 
|---|---|---|---|---|
| 9126926 | Gene | 2005 | 8 Pages | 
Abstract
												A rare mRNA variant of the human lymphocyte-specific protein tyrosine kinase LCK gene that retains intron B and excludes exon 7 (B+7â) due to alternative splicing of the canonical LCK transcripts was identified and characterized. LCK B+7â mRNA is detected in all tested peripheral blood T lymphocytes total RNA samples but is apparently sequestered in the nucleus. The presence of intron B sequence does not disrupt the reading frame and results in the insertion of 58 aminoacids, containing a proline-rich region just upstream of p56lck SH3 domain. This putative isoform encodes an unstable 516 aminoacids protein (LckB+7â) which can be expressed in transfected COS-7 cells. Furthermore in Jurkat T cell extracts, a recombinant intron B plus SH3 p56lck domain fails to interact with some TCR-induced tyrosine phosphorylated polypeptides and known p56lck partners such as Sam68 and c-Cbl. The biological function of this rare messenger remains to be elucidated.
											Keywords
												PBSRas-GAPcdc2CytidineSam68LCKOligo(dT)GRB-2SLP-76AMVSCIDPTKPBLSRCWASPTECDMEMkDaC/TTCrPBMCPVDFGSTA/CA/Gc-CblcDNADNA complementary to RNAkiloDalton(s)MAPKAdenosineAdenosine TriphosphateATPSodium dodecylsulfate-polyacrylamide gel electrophoresisSDS-PAGEReverse transcriptaseThymidineAlternative splicingBase pair(s)Intron retentionpolyvinyl difluoridecell division cycle 2Phosphate buffered salinePhosphatidylinositol 3-kinaseinternational unit(s)polymerase chain reactionPCRexon skippingProtein tyrosine kinaselymphocyte-specific protein tyrosine kinasemitogen-activated protein kinasegrowth factor receptor-bound protein 2severe combined immunodeficiencykilobase(s)glutathione-S-transferaseguanosineT cell receptor
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											Authors
												Solange Nervi, Rodolphe Guinamard, Bénédicte Delaval, Patrick Lécine, Bernard Vialettes, Philippe Naquet, Jean Imbert, 
											