Localized Tufts of Fibrils onStaphylococcus epidermidisNCTC 11047 Are Comprised of the Accumulation-Associated Protein | Zendy

Miriam A. Banner | Zendy; J.G. Cunniffe | Zendy; Robin L. Macintosh | Zendy; Timothy J. Foster | Zendy; Holger Rohde | Zendy; Dietrich Mack | Zendy; Emmy Hoyes | Zendy; Jeremy P. Derrick | Zendy; Mathew Upton | Zendy; Pauline S. Handley | Zendy

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Localized Tufts of Fibrils onStaphylococcus epidermidisNCTC 11047 Are Comprised of the Accumulation-Associated Protein

Author(s) -

Miriam A. Banner,

J.G. Cunniffe,

Robin L. Macintosh,

Timothy J. Foster,

Holger Rohde,

Dietrich Mack,

Emmy Hoyes,

Jeremy P. Derrick,

Mathew Upton,

Pauline S. Handley

Publication year - 2007

Publication title -

journal of bacteriology

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 1.652

H-Index - 246

eISSN - 1067-8832

pISSN - 0021-9193

DOI - 10.1128/jb.00952-06

Subject(s) - biology , staphylococcus epidermidis , microbiology and biotechnology , fibril , staphylococcus aureus , bacterial protein , staphylococcus , bacteria , biochemistry , genetics

Staphylococcus epidermidis is both a human skin commensal and an opportunistic pathogen, causing infections linked to implanted medical devices. This paper describes localized tufts of fibrillar appendages on a subpopulation (25%) of wild-type (WT) S. epidermidis NCTC 11047 cells. The fibrils (122.2 +/- 10.8 nm long) are usually in a lateral position on the cells. Fibrillar (Fib(+)) and nonfibrillar (Fib(-)) subpopulations were separated (enriched) by 34 sequential partitions of WT cells between a buffer phase and a hexadecane phase. Following enrichment, hydrophobic cells from the hexadecane phase comprised 70% Fib(+) cells and the less hydrophobic cells from the buffer phase entirely comprised Fib(-) cells. The Fib(+) and Fib(-) subpopulations did not revert on subculture (34 times) on solid medium. Sodium dodecyl sulfate-polyacrylamide gel electrophoresis of cell surface proteins from WT, Fib(+), and Fib(-) cells revealed two high-molecular-mass proteins (280 kDa and 230 kDa) on the WT and Fib(+) cells that were absent from the Fib(-) cells. Amino acid sequencing revealed that fragments of both the 280- and 230-kDa proteins had 100% identity to the accumulation-associated protein (Aap). Aap is known to cause biofilm formation if it is truncated by loss of the terminal A domain. Immunogold staining with anti-Aap antibodies labeled tuft fibrils of the WT and Fib(+) cells but not the cell surface of Fib(-) cells. The tufts were labeled with N-terminally directed antibodies (anti-A domain), showing that the fibrillar Aap was not truncated on the cell surface. Thus, the presence of full-length Aap correlated with the low biofilm-forming abilities of both WT and Fib(+) S. epidermidis NCTC 11047 populations. Reverse transcription-PCR showed that aap was transcribed in both Fib(+) and Fib(-) cells. We therefore propose that full-length Aap is expressed on cells of S. epidermidis NCTC 11047 as tufts of short fibrils and that fibril expression is regulated at a posttranscriptional level.

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