Early Resistance of Non-virulent Mycobacterial Infection in C57BL/6 Mice Is Associated With Rapid Up-Regulation of Antimicrobial Cathelicidin <i>Camp</i>.
Adam. Lucille L; López-González. Moisés M; Björk. Albin A; Pålsson. Sandra S; Poux. Candice C; Wahren-Herlenius. Marie M; Fernández. Carmen C; Spetz. Anna-Lena AL
Key Findings
- C57BL/6 mice cleared non‑virulent mycobacterial infection faster than BALB/c mice.
- Early clearance was linked to a rapid increase in the cathelicidin peptide CRAMP (human LL‑37) in the lungs.
- The fast‑clearing mice did not show the large neutrophil and myeloid cell influx seen in the slower‑clearing strain.
Practical Outcomes
- For biohackers, the study hints that strategies to raise LL‑37 levels (e.g., vitamin D supplementation, certain probiotics, or topical LL‑37 analogs) might enhance early innate defense against bacterial lung infections. However, the evidence is limited to mice and a non‑virulent strain, so any human protocol would be experimental and should be approached cautiously.
Summary
In a mouse study, the strain that cleared a harmless TB‑like infection fastest showed a big jump in the natural antimicrobial peptide LL‑37 (called CRAMP in mice) right after exposure, without needing a flood of immune cells. The other mouse strain relied on lots of inflammatory cells and cytokines instead. This suggests that boosting LL‑37 could help the body fight certain infections early, without causing excess inflammation.
Abstract
Early clearance of tuberculosis is the successful eradication of inhaled bacteria before the development of an adaptive immune response. We previously showed, by utilizing a non-virulent mycobacteria infection model, that C57BL/6 mice are more efficient than BALB/c in their control of bacterial growth in the lungs during the first weeks of the infection. Here, we assessed early (within 1-3 days) innate immune events locally in the lungs to identify factors that may contribute to the control of non-virulent mycobacterial burden. We confirmed that C57BL/6 mice are more resistant to infection compared with BALB/c after intranasal inoculation with mycobacterium. Transcriptomic analyses revealed a remarkably silent signature in C57BL/6 mice despite effective control of bacterial growth. In contrast, BALB/c mice up-regulated genes associated with neutrophil and myeloid cell chemotaxis and migration. Flow cytometry analyses corroborated the transcriptomic analyses and demonstrated influx of both neutrophil and myeloid cell populations in BALB/c mice, while these did not increase in C57BL/6 mice. We further detected increased release of TNF-α from BALB/c lung cells but limited release from C57BL/6-derived cells. However, C57BL/6 mice showed a marked early up-regulation of the <i>Camp</i> gene, encoding the cathelicidin CRAMP peptide, post-mycobacterial exposure. CRAMP (LL-37 in human) expression in the lungs was confirmed using immunofluorescence staining. Altogether, these findings show that C57BL/6 mice can clear the mycobacterial infection early and that this early control is associated with high CRAMP expression in the lungs without concomitant influx of immune cells. The role of CRAMP/LL-37 during mycobacterial infection may be relevant for novel protective strategies, and warrants further studies of human cohorts.
Study Information
pubmed
2018
2018-09-03T00:00:00.000Z
10.3389/fimmu.2018.01939
8
43