Phagosomal RNA sensing through TLR8 controls susceptibility to tuberculosis

Charlotte Maserumule ; Charlotte Passemar ORCID logo ; Olivia SH Oh ; Kriztina Hegyi ; Karen Brown ; Aaron Weimann ; Adam Dinan ; Sonia Davila ; Catherine Klapholz ; Josephine Bryant ; +16 more... Deepshikha Verma ; Jacob Gadwa ; Shivankari Krishnananthasivam ; Kridakorn Vongtongsalee ; Edward Kendall ; Andres Trelles ; Martin L Hibberd ORCID logo ; Joaquín Sanz ; Jorge Bertol ; Lucia Vázquez-Iniesta ; Kaliappan Andi ; S Siva Kumar ; Diane Ordway ; Rafael Prados-Rosales ; Paul A MacAry ; R Andres Floto ; (2025) Phagosomal RNA sensing through TLR8 controls susceptibility to tuberculosis. Cell Reports, 44 (5). p. 115657. ISSN 2211-1247 DOI: 10.1016/j.celrep.2025.115657
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Genetic determinants of susceptibility to Mycobacterium tuberculosis (Mtb) remain poorly understood but could provide insights into critical pathways involved in infection, informing host-directed therapies and enabling risk stratification at individual and population levels. Through a genome-wide forward genetic screen, we identify Toll-like receptor 8 (TLR8) as a key regulator of intracellular killing of Mtb. Pharmacological TLR8 activation enhances the killing of phylogenetically diverse clinical isolates of drug-susceptible and multidrug-resistant Mtb by macrophages and during in vivo infection in mice. TLR8 is activated by phagosomal mycobacterial RNA released by extracellular membrane vesicles and enhances xenophagy-dependent Mtb killing. We find that the TLR8 variant M1V, common in Far Eastern populations, enhances intracellular killing of Mtb through preferential signal-dependent trafficking to phagosomes. TLR8 signaling may, therefore, both regulate susceptibility to tuberculosis and provide novel drug targets.


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