Borrelia burgdorferi Genetic Markers and Disseminated Disease in Patients with Early Lyme Disease
| Autor: | Gail McHugh, Lisa J. Glickstein, Vijay K. Sikand, Kathryn L. Jones, Allen C. Steere, Nitin Damle |
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| Rok vydání: | 2006 |
| Předmět: |
DNA
Bacterial Microbiology (medical) Genotype Lipoproteins Statistics as Topic Spirochaetaceae Polymerase Chain Reaction Microbiology law.invention Lyme disease Bacterial Proteins Gene Frequency law DNA Ribosomal Spacer medicine Humans Disseminated disease Borrelia burgdorferi Polymerase chain reaction Skin Antigens Bacterial Lyme Disease Virulence biology Bacteriology biology.organism_classification medicine.disease Virology Genes Bacterial Genetic marker Restriction fragment length polymorphism Biomarkers Polymorphism Restriction Fragment Length Bacterial Outer Membrane Proteins |
| Zdroj: | Journal of Clinical Microbiology. 44:4407-4413 |
| ISSN: | 1098-660X 0095-1137 |
| Popis: | Three genetic markers of Borrelia burgdorferi have been associated with disseminated disease: the OspC type, the 16S-23S rRNA intergenic spacer type (RST), and vlsE . Here, we modified previous methods so as to identify the three markers by PCR and restriction fragment length polymorphism in parallel, analyzed B. burgdorferi isolates from erythema migrans (EM) skin lesions in 91 patients, and correlated the results with evidence of dissemination. OspC type A was found approximately twice as frequently in patients with disseminated disease, whereas type K was identified approximately twice as often in those without evidence of dissemination, but these trends were not statistically significant. The remaining seven types identified were found nearly equally in patients with or without evidence of dissemination. RST 1 strains were significantly associated with dissemination ( P = 0.03), whereas RST 2 and RST 3 strains tended to have an inverse association with this outcome. The vlsE gene was identified in all 91 cases, using primer sets specific for an N-terminal sequence of B. burgdorferi strain B31 ( vlsE B31 ) or strain 297 ( vlsE 297 ), but neither marker was associated with dissemination. Specific combinations of the three genetic markers usually occurred together. OspC type A was always found with RST 1 and vlsE B31 , type K was always identified with RST 2 and more often with vlsE 297 , and types E and I were almost always found with RST 3 and equally often with vlsE B31 and vlsE 297 . We conclude that B. burgdorferi strains vary in their capacity to disseminate, but almost all strains isolated from EM lesions sometimes caused disseminated disease. |
| Databáze: | OpenAIRE |
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