Samenvatting
The availability of complete genome sequences has allowed the prediction of all exported proteins of the corresponding organisms with dedicated algorithms. Even though numerous studies report oil genome-based predictions of signal peptides and cell retention signals, they lack a proteomic verification. For example, 180 secretory and 114 lipoprotein signal peptides were predicted recently for the Gram-positive eubacterium Bacillus subtilis. In the present studies, proteomic approaches were used to define the extracellular complement of the B, subtilis secretome. Using different growth conditions and a hyper-secreting mutant, similar to 200 extracellular proteins were Visualized by two-dimensional (2D) gel electrophoresis, of which 82 were identified by mass spectrometry. These include 41 proteins that have a potential signal peptide with a type I signal peptidase (SPase) cleavage site, and lack a retention signal. Strikingly, the remaining 41 proteins were predicted previously to be cell associated because of the apparent absence of a signal peptide (22), or the presence of specific cell retention signals in addition to an export signal (19). To test the importance of the five type I SPases and the Unique lipoprotein-specific SPase of B. subtilis, the extracellular proteome Of (Multiple) SPase Mutants was analyzed. Surprisingly, only the processing of the polytopic membrane protein Will was strongly inhibited ill Spase I mutants, showing for the first time that a native eubacterial membrane protein is a genuine Spase I substrate. Furthermore, a Mutation affecting lipoprotein modification and processing resulted in the shedding of at least 23 (lipo-)proteins into the medium. Ill Conclusion, our observations show that genome-based predictions reflect the actual composition of the extracellular proteome for similar to 50%. Major problems are currently encountered with the prediction of extracellular proteins lacking signal peptides (including cytoplasmic proteins) and lipoproteins.
Originele taal-2 | English |
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Pagina's (van-tot) | 1484-1502 |
Aantal pagina's | 19 |
Tijdschrift | Genome Research |
Volume | 11 |
Nummer van het tijdschrift | 9 |
DOI's | |
Status | Published - sep.-2001 |