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Comparative Investigation of the Genomic Regions Involved in Antigenic Variation of the TprK Antigen among Treponemal Species,Subspecies, and Strains

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2012

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Giacani, Lorenzo
Brandt, Stephanie L.
Puray-Chavez, Maritza
Brinck Reid, Tara
Godornes, Charmie
Molini, Barbara J.
Benzler, Martin
Lukehart, Sheila A.
Centurion-Lara, Arturo

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http://nbn-resolving.de/urn:nbn:de:bsz:352-211555
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https://doi.org/10.1128/JB.00863-12
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Journal of Bacteriology. 2012, 194(16), pp. 4208-4225. ISSN 0021-9193. eISSN 1098-5530. Available under: doi: 10.1128/JB.00863-12

Zusammenfassung

Although the three Treponema pallidum subspecies (T. pallidum subsp. pallidum, T. pallidum subsp. pertenue, and T. pallidum subsp. endemicum), Treponema paraluiscuniculi, and the unclassified Fribourg-Blanc treponeme cause clinically distinct diseases, these pathogens are genetically and antigenically highly related and are able to cause persistent infection. Recent evidence suggests that the putative surface-exposed variable antigen TprK plays an important role in both treponemal immune evasion and persistence. tprK heterogeneity is generated by nonreciprocal gene conversion between the tprK expression site and donor sites. Although each of the above-mentioned species and subspecies has a functional tprK antigenic variation system, it is still unclear why the level of expression and the rate at which tprK diversifies during infection can differ significantly among isolates. To identify genomic differences that might affect the generation and expression of TprK variants among these pathogens, we performed comparative sequence analysis of the donor sites, as well as the tprK expression sites, among eight T. pallidum subsp. pallidum isolates (Nichols Gen, Nichols Sea, Chicago, Sea81-4, Dal-1, Street14, UW104, and UW126), three T. pallidum subsp. pertenue isolates (Gauthier, CDC2, and Samoa D), one T. pallidum subsp. endemicum isolate (Iraq B), the unclassified Fribourg-Blanc isolate, and the Cuniculi A strain of T. paraluiscuniculi. Synteny and sequence conservation, as well as deletions and insertions, were found in the regions harboring the donor sites. These data suggest that the tprK recombination system is harbored within dynamic genomic regions and that genomic differences might be an important key to explain discrepancies in generation and expression of tprK variants among these Treponema isolates.

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ISO 690GIACANI, Lorenzo, Stephanie L. BRANDT, Maritza PURAY-CHAVEZ, Tara BRINCK REID, Charmie GODORNES, Barbara J. MOLINI, Martin BENZLER, Jörg S. HARTIG, Sheila A. LUKEHART, Arturo CENTURION-LARA, 2012. Comparative Investigation of the Genomic Regions Involved in Antigenic Variation of the TprK Antigen among Treponemal Species,Subspecies, and Strains. In: Journal of Bacteriology. 2012, 194(16), pp. 4208-4225. ISSN 0021-9193. eISSN 1098-5530. Available under: doi: 10.1128/JB.00863-12
BibTex
@article{Giacani2012-08Compa-21155,
  year={2012},
  doi={10.1128/JB.00863-12},
  title={Comparative Investigation of the Genomic Regions Involved in Antigenic Variation of the TprK Antigen among Treponemal Species,Subspecies, and Strains},
  number={16},
  volume={194},
  issn={0021-9193},
  journal={Journal of Bacteriology},
  pages={4208--4225},
  author={Giacani, Lorenzo and Brandt, Stephanie L. and Puray-Chavez, Maritza and Brinck Reid, Tara and Godornes, Charmie and Molini, Barbara J. and Benzler, Martin and Hartig, Jörg S. and Lukehart, Sheila A. and Centurion-Lara, Arturo}
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