Alive Pathogenic and Saprophytic Leptospires Enter and Exit Human and Mouse Macrophages With No Intracellular Replication

Ignacio Santecchia; Delphine Bonhomme; Stylianos Papadopoulos; Pedro Escoll; Alexandre Giraud-Gatineau; Maryse Moya-Nilges; Frédérique Vernel-Pauillac; Ivo Gomperts Boneca; Catherine Werts

doi:10.3389/fcimb.2022.936931

Alive Pathogenic and Saprophytic Leptospires Enter and Exit Human and Mouse Macrophages With No Intracellular Replication

Front Cell Infect Microbiol. 2022 Jul 11:12:936931. doi: 10.3389/fcimb.2022.936931. eCollection 2022.

Authors

Ignacio Santecchia¹, Delphine Bonhomme¹, Stylianos Papadopoulos¹, Pedro Escoll², Alexandre Giraud-Gatineau³, Maryse Moya-Nilges⁴, Frédérique Vernel-Pauillac¹, Ivo Gomperts Boneca¹, Catherine Werts¹

Affiliations

¹ Institut Pasteur, Université Cité Paris, CNRS UMR6047, INSERM U1306, Unité de Biologie et Génétique de la Paroi Bactérienne, Paris, France.
² Institut Pasteur, Université Cité Paris, CNRS UMR6047, Unité Biologie des Bactéries Intracellulaires, Paris, France.
³ Institut Pasteur, Université Cité Paris, CNRS UMR6047, Unité de Biologie des Spirochètes, Paris, France.
⁴ Institut Pasteur, Université Cité Paris, Plateforme de Bio-imagerie Ultrastructurale, Paris, France.

Abstract

Leptospira interrogans are pathogenic bacteria responsible for leptospirosis, a zoonosis impacting 1 million people per year worldwide. Leptospires can infect all vertebrates, but not all hosts develop similar symptoms. Human and cattle may suffer from mild to acute illnesses and are therefore considered as sensitive to leptospirosis. In contrast, mice and rats remain asymptomatic upon infection, although they get chronically colonized in their kidneys. Upon infection, leptospires are stealth pathogens that partially escape the recognition by the host innate immune system. Although leptospires are mainly extracellular bacteria, it was suggested that they could also replicate within macrophages. However, contradictory data in the current literature led us to reevaluate these findings. Using a gentamicin-protection assay coupled to high-content (HC) microscopy, we observed that leptospires were internalized in vivo upon peritoneal infection of C57BL/6J mice. Additionally, three different serotypes of pathogenic L. interrogans and the saprophytic L. biflexa actively infected both human (PMA differentiated) THP1 and mouse RAW264.7 macrophage cell lines. Next, we assessed the intracellular fate of leptospires using bioluminescent strains, and we observed a drastic reduction in the leptospiral intracellular load between 3 h and 6 h post-infection, suggesting that leptospires do not replicate within these cells. Surprisingly, the classical macrophage microbicidal mechanisms (phagocytosis, autophagy, TLR-mediated ROS, and RNS production) were not responsible for the observed decrease. Finally, we demonstrated that the reduction in the intracellular load was associated with an increase of the bacteria in the supernatant, suggesting that leptospires exit both human and murine macrophages. Overall, our study reevaluated the intracellular fate of leptospires and favors an active entrance followed by a rapid exit, suggesting that leptospires do not have an intracellular lifestyle in macrophages.

Keywords: Leptospira biflexa; Leptospira interrogans; TLRs; high content confocal microscopy; intracellularity; macrophages.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Cattle
Humans
Leptospira interrogans*
Leptospira*
Leptospirosis* / microbiology
Macrophages / microbiology
Mice
Mice, Inbred C57BL
Rats