December 2023
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152 Reads
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2 Citations
Nature Microbiology
Oxidative stress triggers ferroptosis, a form of cellular necrosis characterized by iron-dependent lipid peroxidation, and has been implicated in Mycobacterium tuberculosis (Mtb) pathogenesis. We investigated whether Bach1, a transcription factor that represses multiple antioxidant genes, regulates host resistance to Mtb. We found that BACH1 expression is associated clinically with active pulmonary tuberculosis. Bach1 deletion in Mtb-infected mice increased glutathione levels and Gpx4 expression that inhibit lipid peroxidation. Bach1−/− macrophages exhibited increased resistance to Mtb-induced cell death, while Mtb-infected Bach1-deficient mice displayed reduced bacterial loads, pulmonary necrosis and lipid peroxidation concurrent with increased survival. Single-cell RNA-seq analysis of lungs from Mtb-infected Bach1−/− mice revealed an enrichment of genes associated with ferroptosis suppression. Bach1 depletion in Mtb-infected B6.Sst1S mice that display human-like necrotic lung pathology also markedly reduced necrosis and increased host resistance. These findings identify Bach1 as a key regulator of cellular and tissue necrosis and host resistance in Mtb infection.
![Alterations in global expression of Gpx4 regulate host resistance to Mtb infection. (A–H) Gpx4fl/fl (used as control animals) and cre-ERT2⁺Gpx4fl/fl mice treated with tamoxifen were infected by aerosol inoculation with ∼100 bacilli of Mtb (H37Rv). Results are representative of two separate experiments performed for each analysis. (A) Scheme of tamoxifen administration. Tamoxifen (2 mg/animal) was given to mice daily via i.p. injections for 5 d. Animals were then rested for 7 d before Mtb infection. (B–H) At 28 d p.i., mice were euthanized and lungs and spleens were harvested. Pulmonary (B) and splenic (C) bacterial loads in Mtb-infected mice. (D) Representative H&E and ZN images of lungs isolated from Gpx4fl/fl (upper panel) and cre-ERT2⁺Gpx4fl/fl mice (lower panel; scale bars [lower magnification], 500 μm). Each image is representative of tissue sections from five individual mice per experiment. Extensive necrotic lesions (dashed line and asterisk) with intrabronchial accumulation of necrotic cellular material along with elevated numbers of AFB were present in the lungs of cre-ERT2⁺Gpx4fl/fl mice. On the lower ZN panel, wide-spread necrosis with numerous Mtb was evident in the lungs of cre-ERT2⁺Gpx4fl/fl mice (scale bars, 20 μm). (E and F) Parenchymal enlargement (E) and TB lesion (F) areas as measured in the lung sections. (G) Number of AFB per cell in lung sections assessed by microscopy. (H) Lipid peroxidation in live CD11b⁺ cell subset in the lungs analyzed by flow cytometry. (I–O) C57BL/6 (WT) and Gpx4-overexpressing (GPX4TG) mice were infected by intrapharyngeal inoculation with ∼1,000–1,500 bacilli of Mtb (H37Rv) as a model of severe TB and the animals sacrificed at 28 d p.i. (I and J) Bacterial burdens in the lungs (I) and spleens (J). Data shown are representative of one of five separate experiments performed. (K) Lung necrosis evaluated by SytoxGreen DNA staining. (L) Mean fluorescence intensity (MFI) of SytoxGreen staining per area of whole lung samples (n = 8–10). Data are representative of one of three separate experiments performed (scale bars, 800 μm). (M) Heatmap visualization of 10 cytokines measured by multiplex in lung homogenates from WT and GPX4TG mice. Data shown are pooled from three independent experiments. (N and O) Cell numbers (N) and lipid peroxidation levels (LAA; O) in AMs (CD45⁺/DUMP⁻/Ly6G⁻/CD24⁻/low/IA-IE⁺/CD45ivneg/CD64⁺/CD11b−/low/CD11c⁺/Siglec-F⁺) and IMs (CD45⁺/DUMP⁻/Ly6G⁻/CD24−/low/IA-IE⁺/CD45ivneg/CD64⁺/CD11bhi/CD11c−/low/Siglec-F⁻) analyzed by flow cytometry. The data shown are pooled results from two independent experiments. The data shown in A–O represent the means ± SEM of samples. (B, C, E–J, and L–O) Statistical significance was assessed by the Mann–Whitney test and significant differences are indicated with asterisks (*, P < 0.05; **, P < 0.01; ***, P < 0.001; ****, P < 0.0001).](https://www.researchgate.net/publication/363346218/figure/fig3/AS:11431281083431908@1662570057268/Alterations-in-global-expression-of-Gpx4-regulate-host-resistance-to-Mtb-infection-A-H_Q320.jpg)
![Deficiency of Gpx4 expression in the hematopoietic compartment enhances host susceptibility to Mtb infection. (A) Gpx4 expression in different hematopoietic cell types was analyzed by flow cytometry in the lungs of uninfected WT mice. (B–K) Gpx4fl/fl and CD45creGpx4fl/fl mice were infected via aerosol with ∼100–200 bacilli of virulent Mtb H37Rv strain. (C–K) Mice were euthanized at 50–55 d p.i. and lungs and spleens were harvested and analyzed. (B) Survival curves of Mtb-infected Gpx4fl/fl and CD45creGpx4fl/fl mice. Statistical significance was assessed by Mantel–Cox test. (C and D) Bacterial loads in the lungs (C) and spleens (D) were determined. (E) Representative H&E (left panel) and ZN (right panel) images of lungs from Gpx4fl/fl (upper panel) and CD45creGpx4fl/fl mice (bottom panel; scale bars [lower magnification], 500 μm). Each image is a composite of sections from four to five individual mice in each group per experiment (three independent experiments; scale bars [higher magnification), 20 μm; 50 μm [bottom left panel]). Massive necrotic tissue damage (asterisk) was observed in the lungs of CD45creGpx4fl/fl mice together with the presence of higher numbers of Mtb (red). Fewer and more isolated AFB (red arrow) were found in the lungs of Mtb-infected Gpx4fl/fl animals. (F) Heatmap visualization of 10 cytokines measured in lung homogenates from Gpx4fl/fl and CD45creGpx4fl/fl mice. Data shown are pooled from four independent experiments (each column represents an individual animal). (G–K) Flow cytometric analysis was performed on single-cell suspension from lungs of Mtb-infected Gpx4fl/fl and CD45creGpx4fl/fl mice. (G) Sample FACS plot of parenchymal macrophages. (H and I) Summary data of frequency and cell numbers of AM (H) and IM (I). (J) Frequency and numbers of Ly6G⁺ cells in the lung. (K) Lipid peroxidation (LAA staining) in different myeloid cells in the lungs. Pooled results of three independent experiments are shown (n = 12 each group). The data shown in A–O represent the means ± SEM of samples. (B–D and F–K) Statistical significance was assessed by the Mann–Whitney test and significant differences are indicated with asterisks (*, P < 0.05; **, P < 0.01; ***, P < 0.001; ****, P < 0.0001).](https://www.researchgate.net/publication/363346218/figure/fig4/AS:11431281083406531@1662570059151/Deficiency-of-Gpx4-expression-in-the-hematopoietic-compartment-enhances-host_Q320.jpg)
