Lyme disease is a multisystem disorder caused by the tick vector Borrelia burgdorferi. During its life cycle between the tick vector and the mammalian host, Borrelia up- and down-regulates the expression of its surface lipoproteins. Of its many surface lipoproteins, the Outer surface protein C (OspC) is crucial for initial mammalian infection. OspC has a common role shared with other lipoproteins of protection against host innate defences and a unique function in facilitating the dissemination of B. burgdorferi in the murine host.
The structure of OspC was solved in 2001 and the lipoprotein was found to be predominantly alpha-helical with 5 alpha helices and 2 beta sheets interconnected by 6 loops, and an N- and C-terminus. Not much is known as to how the OspC structure relates to the function of the lipoprotein and/or possible regulation. The up-and down-regulation of OspC is achieved by the rpoS alternative sigma factor and by an unidentified repressor, respectively.
Several truncated versions of OspC were tested in an OspC-deficient background to better understand the role of the amino acid sequences deleted. Structural deletions of 5 to 8-AA made within the OspC core, resulted in loss of infectivity. Longer deletions of 10- and 13 AA towards the N- and C-terminus of OspC, respectively, also resulted in loss of infectivity. Interestingly, a deletion of only 5-AA of the N-terminus of OspC did not affect the role of OspC in evasion but caused inefficient dissemination of B. burgdorferi in SCID mice.
Interestingly, whereas the deletion of N-terminus 5-AA of OspC resulted in upregulation, a deletion of 6- and 9-AA of the C-terminus of OspC resulted in downregulation of ospC mRNA in joints, indicating that OspC may be involved in self-regulation. This hypothesis was confirmed by the use of monoclonal antibody treatment. Deletion of 6-AA of the C-terminus of OspC resulted in lower spirochete burdens in heart and joint, whereas deletion of 9-AA resulted in higher spirochete burden in skin, indicating the tissue-dependent effects resulting from the deletion of the C-terminal sequence. Taken together, these results indicate that OspC is involved in the pathogenesis of B. burgdorferi.
| Identifer | oai:union.ndltd.org:LSU/oai:etd.lsu.edu:etd-02202010-133406 |
| Date | 24 February 2010 |
| Creators | Seemanapalli, Sunita V |
| Contributors | Liang, Fang-Ting, Elzer, Philip H., Schowalter, Timothy D., Macaluso, Kevin, Kousoulas, Konstantin G. |
| Publisher | LSU |
| Source Sets | Louisiana State University |
| Language | English |
| Detected Language | English |
| Type | text |
| Format | application/pdf |
| Source | http://etd.lsu.edu/docs/available/etd-02202010-133406/ |
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