Treponema pallidum induces pro-inflammatory cytokine secretion in macrophages and macrophage-endothelial co-cultures
Sean Waugh, Akash Ranasinghe, Lisa A. Reynolds, Caroline E. Cameron

TL;DR
This study shows how the syphilis-causing bacterium Treponema pallidum triggers immune responses in macrophages and endothelial cells, leading to inflammation and disease symptoms.
Contribution
The study identifies specific cytokines secreted by macrophages and co-cultured endothelial cells in response to T. pallidum exposure.
Findings
T. pallidum exposure increases secretion of RANTES, IL-1β, MCP-1, GM-CSF, TNF, and IL-6 in macrophages.
Co-cultured endothelial cells show altered cytokine profiles compared to macrophage monocultures.
Reduced IL-8 secretion is observed in T. pallidum-exposed macrophages and co-cultures.
Abstract
Syphilis, caused by the extracellular bacterium Treponema pallidum ssp. pallidum, is a multi-stage and systemic infection that is lifelong in the absence of treatment. Two host cell types that frequently encounter T. pallidum during infection are endothelial cells and macrophages; treponemes disseminate through the vasculature and cross the blood–brain and placental barriers by traversing endothelial cell barriers, and macrophages are known to be critical for clearance of T. pallidum. Despite the importance of macrophages in treponemal clearance and endothelial cells in treponemal dissemination, a comprehensive understanding of the cytokines secreted by T. pallidum-exposed macrophages in the presence and absence of endothelial cells has not yet been achieved. To address this knowledge gap, we conducted time-course cytokine secretion profiling of macrophage-differentiated THP-1 cells…
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Taxonomy
TopicsSyphilis Diagnosis and Treatment · Sex work and related issues · Reproductive tract infections research
