Neutrophil-mediated innate immune resistance to bacterial pneumonia is dependent on Tet2 function
Candice Quin, … , Michael J. Rauh, Dawn M.E. Bowdish
Candice Quin, … , Michael J. Rauh, Dawn M.E. Bowdish
Published April 4, 2024
Citation Information: J Clin Invest. 2024;134(11):e171002. https://doi.org/10.1172/JCI171002.
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Research Article Immunology Infectious disease Article has an altmetric score of 9

Neutrophil-mediated innate immune resistance to bacterial pneumonia is dependent on Tet2 function

Abstract

Individuals with clonal hematopoiesis of indeterminate potential (CHIP) are at increased risk of aging related health conditions and all-cause mortality, but whether CHIP affects risk of infection is much less clear. Using UK Biobank data, we revealed a positive association between CHIP and incident pneumonia in 438,421 individuals. We show that inflammation enhanced pneumonia risk, as CHIP carriers with a hypomorphic IL6 receptor polymorphism were protected. To better characterize the pathways of susceptibility, we challenged hematopoietic Tet Methylcytosine Dioxygenase 2–knockout (Tet2–/–) and floxed control mice (Tet2fl/fl) with Streptococcus pneumoniae. As with human CHIP carriers, Tet2–/– mice had hematopoietic abnormalities resulting in the expansion of inflammatory monocytes and neutrophils in peripheral blood. Yet, these cells were insufficient in defending against S. pneumoniae and resulted in increased pathology, impaired bacterial clearance, and higher mortality in Tet2–/– mice. We delineated the transcriptional landscape of Tet2–/– neutrophils and found that, while inflammation-related pathways were upregulated in Tet2–/– neutrophils, migration and motility pathways were compromised. Using live-imaging techniques, we demonstrated impairments in motility, pathogen uptake, and neutrophil extracellular trap (NET) formation by Tet2–/– neutrophils. Collectively, we show that CHIP is a risk factor for bacterial pneumonia related to innate immune impairments.

Authors

Candice Quin, Erica N. DeJong, Elina K. Cook, Yi Zhen Luo, Caitlyn Vlasschaert, Sanathan Sadh, Amy J.M. McNaughton, Marco M. Buttigieg, Jessica A. Breznik, Allison E. Kennedy, Kevin Zhao, Jeffrey Mewburn, Kimberly J. Dunham-Snary, Charles C.T. Hindmarch, Alexander G. Bick, Stephen L. Archer, Michael J. Rauh, Dawn M.E. Bowdish

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Figure 4

Pneumococcal pneumonia–induced sepsis and accompanying inflammatory responses are exacerbated in Tet2–/– mice.

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Pneumococcal pneumonia–induced sepsis and accompanying inflammatory resp...
(A) Experimental timeline of infection and concurrent survival (n = 13 Tet2–/–; n = 12 Tet2fl/fl). (B) Representative H&E-stained lung sections of mice at 10 days p.i. with S. pneumoniae. Original magnification 20-fold. (C) Histopathological analysis of lung H&E tissue sections [as shown in (B)] attained by 2 blinded scorers. (D) Counts and representative IHC staining of mononuclear phagocytes (F4/80+) and neutrophils (Ly6G+) on lung sections at 10 days p.i. Original magnification 200-fold. Tet–/– mice had increased numbers of mononuclear phagocytes in the lungs (Tet2fl/fl [27 ± 1]; Tet2–/– [35 ± 3.6]). In contrast, neutrophils were decreased (Tet2fl/fl [49 ± 2.3]; Tet2–/– [36 ± 4.2]). (E) Relative frequency, as a percentage of 100 cells counted via LeukoSpins, of neutrophils and monocytes in circulation 10 days p.i. showed an increase in neutrophils (Tet2fl/fl [20.9 ± 2.1]; Tet2–/– [46.9 ± 10.5]) and monocytes (Tet2fl/fl [4.9 ± 0.7]; Tet2–/– [7.6 ± 2.2]) in Tet2–/– mice. Representative images are shown. (F) Surface expression of CCR2 is decreased on peripheral blood neutrophils in Tet2–/– mice (Tet2fl/fl [4328 ± 449, n = 19]; Tet2–/– [2875 ± 407], n = 18), at steady-state. (G) Relative expression of CCL2 is lower in the lungs of Tet2–/– at steady-state (Tet2fl/fl [1.96 ± 0.35], n = 8; Tet2–/– [0.87 ± 0.17], n = 16). (H) Enumeration of CFUs in lungs and complete nasal turbinate (CNT) 10 days p.i. showed increased pathogen burden in the CNT of Tet2–/– mice (Tet2fl/fl [3.1 ± 0.1]; Tet2–/– [3.6 ± 0.22]). (I) Results from a simple linear regression between CFUs in the CNT at 10 days p.i. and whole blood inflammatory mediators showed a positive association between inflammation and pathogen burden, with a greater relationship in Tet2–/– mice. Shaded area represents 95% confidence intervals. * P < 0.05