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Role of Sca2 and RickA in the Dissemination of Rickettsia parkeri in Amblyomma maculatum

The Gram-negative obligate intracellular bacterium Rickettsia parkeri is an emerging tick-borne human pathogen. Recently, R. parkeri Sca2 and RickA have been implicated in adherence and actin-based motility in vertebrate host cell infection models; however, the rickettsia-derived factors essential t...

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Autores principales: Harris, Emma K., Jirakanwisal, Krit, Verhoeve, Victoria I., Fongsaran, Chanida, Suwanbongkot, Chanakan, Welch, Matthew D., Macaluso, Kevin R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Microbiology 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5964526/
https://www.ncbi.nlm.nih.gov/pubmed/29581194
http://dx.doi.org/10.1128/IAI.00123-18
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author Harris, Emma K.
Jirakanwisal, Krit
Verhoeve, Victoria I.
Fongsaran, Chanida
Suwanbongkot, Chanakan
Welch, Matthew D.
Macaluso, Kevin R.
author_facet Harris, Emma K.
Jirakanwisal, Krit
Verhoeve, Victoria I.
Fongsaran, Chanida
Suwanbongkot, Chanakan
Welch, Matthew D.
Macaluso, Kevin R.
author_sort Harris, Emma K.
collection PubMed
description The Gram-negative obligate intracellular bacterium Rickettsia parkeri is an emerging tick-borne human pathogen. Recently, R. parkeri Sca2 and RickA have been implicated in adherence and actin-based motility in vertebrate host cell infection models; however, the rickettsia-derived factors essential to tick infection are unknown. Using R. parkeri mutants lacking functional Sca2 or RickA to compare actin polymerization, replication, and cell-to-cell spread in vitro, similar phenotypes in tick and mammalian cells were observed. Specifically, actin polymerization in cultured tick cells is controlled by the two separate proteins in a time-dependent manner. To assess the role of Sca2 and RickA in dissemination in the tick host, Rickettsia-free Amblyomma maculatum, the natural vector of R. parkeri, was exposed to wild-type, R. parkeri rickA::tn, or R. parkeri sca2::tn bacteria, and individual tick tissues, including salivary glands, midguts, ovaries, and hemolymph, were analyzed at 12 h and after continued bloodmeal acquisition for 3 or 7 days postexposure. Initially, ticks exposed to wild-type R. parkeri had the highest rickettsial load across all organs; however, rickettsial loads decreased and wild-type rickettsiae were cleared from the ovaries at 7 days postexposure. In contrast, ticks exposed to R. parkeri rickA::tn or R. parkeri sca2::tn had comparatively lower rickettsial loads, but bacteria persisted in all organs for 7 days. These data suggest that while RickA and Sca2 function in actin polymerization in tick cells, the absence of these proteins did not change dissemination patterns within the tick vector.
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spelling pubmed-59645262018-05-30 Role of Sca2 and RickA in the Dissemination of Rickettsia parkeri in Amblyomma maculatum Harris, Emma K. Jirakanwisal, Krit Verhoeve, Victoria I. Fongsaran, Chanida Suwanbongkot, Chanakan Welch, Matthew D. Macaluso, Kevin R. Infect Immun Bacterial Infections The Gram-negative obligate intracellular bacterium Rickettsia parkeri is an emerging tick-borne human pathogen. Recently, R. parkeri Sca2 and RickA have been implicated in adherence and actin-based motility in vertebrate host cell infection models; however, the rickettsia-derived factors essential to tick infection are unknown. Using R. parkeri mutants lacking functional Sca2 or RickA to compare actin polymerization, replication, and cell-to-cell spread in vitro, similar phenotypes in tick and mammalian cells were observed. Specifically, actin polymerization in cultured tick cells is controlled by the two separate proteins in a time-dependent manner. To assess the role of Sca2 and RickA in dissemination in the tick host, Rickettsia-free Amblyomma maculatum, the natural vector of R. parkeri, was exposed to wild-type, R. parkeri rickA::tn, or R. parkeri sca2::tn bacteria, and individual tick tissues, including salivary glands, midguts, ovaries, and hemolymph, were analyzed at 12 h and after continued bloodmeal acquisition for 3 or 7 days postexposure. Initially, ticks exposed to wild-type R. parkeri had the highest rickettsial load across all organs; however, rickettsial loads decreased and wild-type rickettsiae were cleared from the ovaries at 7 days postexposure. In contrast, ticks exposed to R. parkeri rickA::tn or R. parkeri sca2::tn had comparatively lower rickettsial loads, but bacteria persisted in all organs for 7 days. These data suggest that while RickA and Sca2 function in actin polymerization in tick cells, the absence of these proteins did not change dissemination patterns within the tick vector. American Society for Microbiology 2018-05-22 /pmc/articles/PMC5964526/ /pubmed/29581194 http://dx.doi.org/10.1128/IAI.00123-18 Text en Copyright © 2018 Harris et al. https://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Bacterial Infections
Harris, Emma K.
Jirakanwisal, Krit
Verhoeve, Victoria I.
Fongsaran, Chanida
Suwanbongkot, Chanakan
Welch, Matthew D.
Macaluso, Kevin R.
Role of Sca2 and RickA in the Dissemination of Rickettsia parkeri in Amblyomma maculatum
title Role of Sca2 and RickA in the Dissemination of Rickettsia parkeri in Amblyomma maculatum
title_full Role of Sca2 and RickA in the Dissemination of Rickettsia parkeri in Amblyomma maculatum
title_fullStr Role of Sca2 and RickA in the Dissemination of Rickettsia parkeri in Amblyomma maculatum
title_full_unstemmed Role of Sca2 and RickA in the Dissemination of Rickettsia parkeri in Amblyomma maculatum
title_short Role of Sca2 and RickA in the Dissemination of Rickettsia parkeri in Amblyomma maculatum
title_sort role of sca2 and ricka in the dissemination of rickettsia parkeri in amblyomma maculatum
topic Bacterial Infections
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5964526/
https://www.ncbi.nlm.nih.gov/pubmed/29581194
http://dx.doi.org/10.1128/IAI.00123-18
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