AUTHOR=Abdou Elias , Jiménez de Bagüés María P. , Martínez-Abadía Ignacio , Ouahrani-Bettache Safia , Pantesco Véronique , Occhialini Alessandra , Al Dahouk Sascha , Köhler Stephan , Jubier-Maurin Véronique 

TITLE=RegA Plays a Key Role in Oxygen-Dependent Establishment of Persistence and in Isocitrate Lyase Activity, a Critical Determinant of In vivo Brucella suis Pathogenicity

JOURNAL=Frontiers in Cellular and Infection Microbiology

VOLUME=7

YEAR=2017

URL=https://www.frontiersin.org/journals/cellular-and-infection-microbiology/articles/10.3389/fcimb.2017.00186

DOI=10.3389/fcimb.2017.00186

ISSN=2235-2988

ABSTRACT=<p>For aerobic human pathogens, adaptation to hypoxia is a critical factor for the establishment of persistent infections, as oxygen availability is low inside the host. The two-component system RegB/A of <italic>Brucella suis</italic> plays a central role in the control of respiratory systems adapted to oxygen deficiency, and in persistence <italic>in vivo</italic>. Using an original “<italic>in vitro</italic> model of persistence” consisting in gradual oxygen depletion, we compared transcriptomes and proteomes of wild-type and Δ<italic>regA</italic> strains to identify the RegA-regulon potentially involved in the set-up of persistence. Consecutive to oxygen consumption resulting in growth arrest, 12% of the genes in <italic>B. suis</italic> were potentially controlled directly or indirectly by RegA, among which numerous transcriptional regulators were up-regulated. In contrast, genes or proteins involved in envelope biogenesis and in cellular division were repressed, suggesting a possible role for RegA in the set-up of a non-proliferative persistence state. Importantly, the greatest number of the RegA-repressed genes and proteins, including <italic>aceA</italic> encoding the functional IsoCitrate Lyase (ICL), were involved in energy production. A potential consequence of this RegA impact may be the slowing-down of the central metabolism as <italic>B. suis</italic> progressively enters into persistence. Moreover, ICL is an essential determinant of pathogenesis and long-term interactions with the host, as demonstrated by the strict dependence of <italic>B. suis</italic> on ICL activity for multiplication and persistence during <italic>in vivo</italic> infection. RegA regulates gene or protein expression of all functional groups, which is why RegA is a key regulator of <italic>B. suis</italic> in adaptation to oxygen depletion. This function may contribute to the constraint of bacterial growth, typical of chronic infection. Oxygen-dependent activation of two-component systems that control persistence regulons, shared by several aerobic human pathogens, has not been studied in <italic>Brucella</italic> sp. before. This work therefore contributes significantly to the unraveling of persistence mechanisms in this important zoonotic pathogen.</p>