Depletion of essential mycobacterial gene glmM reduces pathogen survival and induces host-protective immune responses against tuberculosis.
Meetu AgarwalAshima BhaskarBiplab SinghaSuparba MukhopadhyayIsha PahujaArchna SinghShivam ChaturvediNisheeth AgarwalVed Prakash DwivediVinay Kumar NandicooriPublished in: Communications biology (2024)
The limitations of TB treatment are the long duration and immune-dampening effects of anti-tuberculosis therapy. The Cell wall plays a crucial role in survival and virulence; hence, enzymes involved in its biosynthesis are good therapeutic targets. Here, we identify Mycobacterium tuberculosis (Mtb) GlmM, (GlmM Mtb ) engaged in the UDP-GlcNAc synthesis pathway as an essential enzyme. We generated a conditional knockdown strain, Rv-glmM kD using the CRISPR interference-mediated gene silencing approach. Depletion of GlmM Mtb affects the morphology and thickness of the cell wall. The Rv-glmM kD strain attenuated Mtb survival in vitro, in the host macrophages (ex vivo), and in a murine mice infection model (in vivo). Results suggest that the depletion of GlmM Mtb induces M1 macrophage polarization, prompting a pro-inflammatory cytokine response, apparent from the upregulation of activation markers, including IFNɣ and IL-17 that resists the growth of Mtb. These observations provide a rationale for exploring GlmM Mtb as a potential therapeutic target.
Keyphrases
- mycobacterium tuberculosis
- cell wall
- pulmonary tuberculosis
- immune response
- genome wide
- escherichia coli
- free survival
- pseudomonas aeruginosa
- signaling pathway
- staphylococcus aureus
- clinical trial
- magnetic resonance
- poor prognosis
- metabolic syndrome
- copy number
- cell proliferation
- climate change
- candida albicans
- adipose tissue
- genome editing
- mesenchymal stem cells
- combination therapy
- replacement therapy