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Identification and characterization of DSPIa, a novel isoform of human desmoplakin
Authors:Rita M. Cabral  Hong Wan  Clare L. Cole  Dominic J. Abrams  David P. Kelsell  Andrew P. South
Affiliation:1. Centre for Cutaneous Research, Blizard Institute of Cell and Molecular Science, University of London, London, UK
2. Centre for Clinical and Diagnostic Oral Sciences, Institute of Dentistry, Bart’s and The London School of Medicine and Dentistry, University of London, London, UK
3. Centre for Oncology & Molecular Medicine, University of Dundee, Ninewells Hospital & Medical School, Dundee, DD1 9SY, UK
4. Department of Cardiac Electrophysiology, St Bartholomew’s Hospital, London, UK
Abstract:Desmoplakin is a ubiquitous component of desmosomes and desmosome-like structures, such as the cardiomyocyte area composita. Two major isoforms, desmoplakin I (DSPI) and desmoplakin II (DSPII) are encoded by alternative mRNA transcripts differentially spliced from the same gene. The resulting proteins are identical in amino acid sequence with the exception that DSPII contains only one third of the central alpha-helical rod domain present in DSPI. Here we describe a novel minor isoform of desmoplakin that is also produced by alternative splicing of the desmoplakin gene and that we name desmoplakin Ia (DSPIa). DSPIa is an alternatively spliced DSPI mRNA with a unique splice donor site that is 90% homologous to and downstream of the DSPII specific donor. The resulting DSPIa mRNA is in-frame and encodes a protein that has a central alpha-helical rod domain of intermediate size and that is 156 amino acids larger than DSPII and 443 amino acids smaller than DSPI. We demonstrate, through recombinant expression and short interfering RNA knockdown, that the DSPIa protein is readily detectable, albeit at substantially lower levels than the dominant isoforms, DSPI and DSPII. DSPIa mRNA has a similar tissue distribution to that of DSPI and of DSPII.
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