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Star M. Dunham-Ems, Melissa J. Caimano, Utpal Pal, Charles W. Wolgemuth, Christian H. Eggers, Anamaria Balic, Justin D. Radolf
J Clin Invest. 2009;
119(12):3652
doi:10.1172/JCI39401
Abstract |
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L
yme disease is caused by transmission of the spirochete Borrelia burgdorferi from ticks to humans. Although much is known about B. burgdorferi replication, the routes and mechanisms by which it disseminates within the tick remain unclear. To better understand this process, we imaged live, infectious B. burgdorferi expressing a stably integrated, constitutively expressed GFP reporter. Using isolated tick midguts and salivary glands, we observed B. burgdorferi progress through the feeding tick via what we believe to be a novel, biphasic mode of dissemination. In the first phase, replicating spirochetes, positioned at varying depths throughout the midgut at the onset of feeding, formed networks of nonmotile organisms that advanced toward the basolateral surface of the epithelium while adhering to differentiating, hypertrophying, and detaching epithelial cells. In the second phase of dissemination, the nonmotile spirochetes transitioned into motile organisms that penetrated the basement membrane and entered the hemocoel, then migrated to and entered the salivary glands. We designated the first phase of dissemination “adherence-mediated migration” and provided evidence that it involves the inhibition of spirochete motility by one or more diffusible factors elaborated by the feeding tick midgut. Our studies, which we believe are the first to relate the transmission dynamics of spirochetes to the complex morphological and developmental changes that the midgut and salivary glands undergo during engorgement, challenge the conventional viewpoint that dissemination of Lyme disease–causing spirochetes within ticks is exclusively motility driven.
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| Title and authors |
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Year |
Of ticks, mice and men: understanding the dual-host lifestyle of Lyme disease spirochaetes
Justin D. Radolf, Melissa J. Caimano, Brian Stevenson, Linden T. Hu
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Nat Rev Micro
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2012 |
CD14 cooperates with complement receptor 3 to mediate MyD88-independent phagocytosis of Borrelia burgdorferi
K. L. Hawley, C. M. Olson, J. M. Iglesias-Pedraz, N. Navasa, J. L. Cervantes, M. J. Caimano, H. Izadi, R. R. Ingalls, U. Pal, J. C. Salazar
|
Proceedings of the National Academy of Sciences
|
2012 |
The heterogeneous motility of the Lyme disease spirochete in gelatin mimics dissemination through tissue
M. W. Harman, S. M. Dunham-Ems, M. J. Caimano, A. A. Belperron, L. K. Bockenstedt, H. C. Fu, J. D. Radolf, C. W. Wolgemuth
|
Proceedings of the National Academy of Sciences
|
2012 |
Current Protocols in Microbiology
Jenny A. Hyde, Eric H. Weening, Jon T. Skare
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Current Protocols in Microbiology
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2011 |
Gene Regulation in <i>Borrelia burgdorferi</i>
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Annu. Rev. Microbiol.
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2011 |
The coenzyme A disulphide reductase of Borrelia burgdorferi is important for rapid growth throughout the enzootic cycle and essential for infection of the mammalian host : CoADR requirement for growth of B. burgdorferi
Christian H. Eggers, Melissa J. Caimano, Robert A. Malizia, Toru Kariu, Brian Cusack, Daniel C. Desrosiers, Karsten R. O. Hazlett, Al Claiborne, Utpal Pal, Justin D. Radolf
|
Mol Microbiol
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2011 |
Carbon storage regulator A (CsrABb) is a repressor of Borrelia burgdorferi flagellin protein FlaB : Carbon storage regulator A and the flagella of Borrelia burgdorferi
Ching Wooen Sze, Dustin R. Morado, Jun Liu, Nyles W. Charon, Hongbin Xu, Chunhao Li
|
Mol Microbiol
|
2011 |
|