Abstract
The majority of mouse HSP90 exists as alpha-alpha and beta-beta homodimers. Truncation of the 15-kDa carboxy-terminal region of mouse HSP90 by digestion with the Ca(2+)-dependent protease m-calpain caused dissociation of the dimer. When expressed in a reticulocyte lysate, the full-length human HSP90 alpha formed a dimeric form. A plasmid harboring human HSP90 alpha cDNA was constructed so that the carboxy-terminal 49 amino acid residues were removed when translated in vitro. This carboxy-terminally truncated human HSP90 alpha was found to exist as a monomer. In contrast, loss of the 118 amino acid residues from the amino terminus of human HSP90 alpha did not affect its in vitro dimerization. Introduction of an expression plasmid harboring the full-length human HSP90 alpha complements the lethality caused by the double mutations of two HSP90-related genes, hsp82 and hsc82, in a haploid strain of Saccharomyces cerevisiae. The carboxy-terminally truncated human HSP90 alpha neither formed dimers in yeast cells nor rescued the lethal double mutant.
Dates
| Type | When |
|---|---|
| Created | 9 years, 10 months ago (Oct. 5, 2015, 8:38 p.m.) |
| Deposited | 2 years, 8 months ago (Dec. 15, 2022, 9:07 a.m.) |
| Indexed | 1 month, 3 weeks ago (July 2, 2025, 2:35 p.m.) |
| Issued | 31 years, 6 months ago (Feb. 1, 1994) |
| Published | 31 years, 6 months ago (Feb. 1, 1994) |
| Published Online | 31 years, 6 months ago (Feb. 1, 1994) |
| Published Print | 31 years, 6 months ago (Feb. 1, 1994) |
@article{Minami_1994, title={The carboxy-terminal region of mammalian HSP90 is required for its dimerization and function in vivo.}, volume={14}, ISSN={1098-5549}, url={http://dx.doi.org/10.1128/mcb.14.2.1459}, DOI={10.1128/mcb.14.2.1459}, number={2}, journal={Molecular and Cellular Biology}, publisher={Informa UK Limited}, author={Minami, Y and Kimura, Y and Kawasaki, H and Suzuki, K and Yahara, I}, year={1994}, month=feb, pages={1459–1464} }