VapC21 Toxin Contributes to Drug-Tolerance and Interacts With Non-cognate VapB32 Antitoxin in Mycobacterium tuberculosis

Sharma, Arun; Chattopadhyay, Gopinath; Chopra, Pankaj; Bhasin, Munmun; Thakur, Chandrani; Agarwal, Sakshi; Ahmed, Shahbaz; Chandra, Nagasuma; Varadarajan, Raghavan; Singh, Ramandeep

doi:10.3389/fmicb.2020.02037

Cited by 22 publications

(36 citation statements)

References 94 publications

(147 reference statements)

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“…Notably, the VapBC TA family is the most abundant type of TA system encoded by Mtb (60). Several studies have demonstrated that host-mediated stress, such as hypoxia and activated macrophages, induces transcriptional activation of multiple VapBC TA loci (61)(62)(63). Hudock et al identified the transcriptional profile from granuloma samples of active and latent TB patients; the expression of eight dosR regulon members (Rv0080, Rv0081, Rv1736c, Rv1737c, Rv2032, Rv2625c, and Rv2630) along with the induction of four pairs of toxin/antitoxin (vapBC19, vapBC21, vapBC33, and vapBC34) were observed within the granulomas of active and latent TB patients (61).…”

Section: Toxin-antitoxin (Ta) Systemmentioning

confidence: 99%

“…Hudock et al identified the transcriptional profile from granuloma samples of active and latent TB patients; the expression of eight dosR regulon members (Rv0080, Rv0081, Rv1736c, Rv1737c, Rv2032, Rv2625c, and Rv2630) along with the induction of four pairs of toxin/antitoxin (vapBC19, vapBC21, vapBC33, and vapBC34) were observed within the granulomas of active and latent TB patients (61). Sharma et al demonstrated that VapC21 overexpression hinders mycobacterial growth, and co-expression of antitoxin VapB21 reverses this effect (62). Moreover, VapC21 overexpression mutant and Mtb cultured in stress conditions, such as nutrient deprivation and hypoxia, exhibited similar transcriptional profiles (62).…”

Section: Toxin-antitoxin (Ta) Systemmentioning

confidence: 99%

“…Sharma et al. demonstrated that VapC21 overexpression hinders mycobacterial growth, and co-expression of antitoxin VapB21 reverses this effect ( 62 ). Moreover, VapC21 overexpression mutant and Mtb cultured in stress conditions, such as nutrient deprivation and hypoxia, exhibited similar transcriptional profiles ( 62 ).…”

Section: Mycobacterial Persisters Adapt To Stresses In the Host And Exhibit Antibiotic Tolerancementioning

confidence: 99%

“…demonstrated that VapC21 overexpression hinders mycobacterial growth, and co-expression of antitoxin VapB21 reverses this effect ( 62 ). Moreover, VapC21 overexpression mutant and Mtb cultured in stress conditions, such as nutrient deprivation and hypoxia, exhibited similar transcriptional profiles ( 62 ). Furthermore, VapC21 overexpression resulted in upregulated WhiB7 regulon, inducing antibiotic tolerance to aminoglycosides and EMB ( 62 ).…”

Section: Mycobacterial Persisters Adapt To Stresses In the Host And Exhibit Antibiotic Tolerancementioning

confidence: 99%

“…Moreover, VapC21 overexpression mutant and Mtb cultured in stress conditions, such as nutrient deprivation and hypoxia, exhibited similar transcriptional profiles ( 62 ). Furthermore, VapC21 overexpression resulted in upregulated WhiB7 regulon, inducing antibiotic tolerance to aminoglycosides and EMB ( 62 ). Talwar et al.…”

Section: Mycobacterial Persisters Adapt To Stresses In the Host And Exhibit Antibiotic Tolerancementioning

confidence: 99%

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Understanding the Reciprocal Interplay Between Antibiotics and Host Immune System: How Can We Improve the Anti-Mycobacterial Activity of Current Drugs to Better Control Tuberculosis?

et al. 2021

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Tuberculosis (TB), caused by Mycobacterium tuberculosis (Mtb) infection, remains a global health threat despite recent advances and insights into host-pathogen interactions and the identification of diverse pathways that may be novel therapeutic targets for TB treatment. In addition, the emergence and spread of multidrug-resistant Mtb strains led to a low success rate of TB treatments. Thus, novel strategies involving the host immune system that boost the effectiveness of existing antibiotics have been recently suggested to better control TB. However, the lack of comprehensive understanding of the immunomodulatory effects of anti-TB drugs, including first-line drugs and newly introduced antibiotics, on bystander and effector immune cells curtailed the development of effective therapeutic strategies to combat Mtb infection. In this review, we focus on the influence of host immune-mediated stresses, such as lysosomal activation, metabolic changes, oxidative stress, mitochondrial damage, and immune mediators, on the activities of anti-TB drugs. In addition, we discuss how anti-TB drugs facilitate the generation of Mtb populations that are resistant to host immune response or disrupt host immunity. Thus, further understanding the interplay between anti-TB drugs and host immune responses may enhance effective host antimicrobial activities and prevent Mtb tolerance to antibiotic and immune attacks. Finally, this review highlights novel adjunctive therapeutic approaches against Mtb infection for better disease outcomes, shorter treatment duration, and improved treatment efficacy based on reciprocal interactions between current TB antibiotics and host immune cells.

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Section: Toxin-antitoxin (Ta) Systemmentioning

confidence: 99%

Section: Toxin-antitoxin (Ta) Systemmentioning

confidence: 99%

Section: Mycobacterial Persisters Adapt To Stresses In the Host And Exhibit Antibiotic Tolerancementioning

confidence: 99%

Section: Mycobacterial Persisters Adapt To Stresses In the Host And Exhibit Antibiotic Tolerancementioning

confidence: 99%

Section: Mycobacterial Persisters Adapt To Stresses In the Host And Exhibit Antibiotic Tolerancementioning

confidence: 99%

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Understanding the Reciprocal Interplay Between Antibiotics and Host Immune System: How Can We Improve the Anti-Mycobacterial Activity of Current Drugs to Better Control Tuberculosis?

et al. 2021

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Ter‐Seq: A high‐throughput method to stabilize transient ternary complexes and measure associated kinetics

et al. 2022

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Regulation of biological processes by proteins often involves the formation of transient, multimeric complexes whose characterization is mechanistically important but challenging. The bacterial toxin CcdB binds and poisons DNA Gyrase. The corresponding antitoxin CcdA extracts CcdB from its complex with Gyrase through the formation of a transient ternary complex, thus rejuvenating Gyrase. We describe a high throughput methodology called Ter-Seq to stabilize probable ternary complexes and measure associated kinetics using the CcdA-CcdB-GyrA14 ternary complex as a model system. The method involves screening a yeast surface display (YSD) saturation mutagenesis library of one partner (CcdB) for mutants that show enhanced ternary complex formation. We also isolated CcdB mutants that were either resistant or sensitive to rejuvenation, and used surface plasmon resonance (SPR) with purified proteins to validate the kinetics measured using the surface display. Positions, where CcdB mutations lead to slower rejuvenation rates, are largely involved in CcdA-binding, though there were several notable exceptions suggesting allostery. Mutations at these positions reduce the affinity towards CcdA, thereby slowing down the rejuvenation process. Mutations at GyrA14-interacting positions significantly enhanced rejuvenation rates, either due to reduced affinity or complete loss of CcdB binding to GyrA14. We examined the effect of different parameters (CcdA affinity, GyrA14 affinity, surface accessibilities, evolutionary conservation) on the rate of rejuvenation. Finally, we further validated the Ter-Seq results by monitoring the kinetics of ternary complex formation for individual CcdB mutants in solution by fluorescence resonance energy transfer (FRET) studies.

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Are all VapC toxins of Mycobacterium tuberculosis endowed with enigmatic RNase activity?

Zarin,

Alam,

Hasnain

et al. 2024

J Biosci

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VapC21 Toxin Contributes to Drug-Tolerance and Interacts With Non-cognate VapB32 Antitoxin in Mycobacterium tuberculosis

Cited by 22 publications

References 94 publications

Understanding the Reciprocal Interplay Between Antibiotics and Host Immune System: How Can We Improve the Anti-Mycobacterial Activity of Current Drugs to Better Control Tuberculosis?

Understanding the Reciprocal Interplay Between Antibiotics and Host Immune System: How Can We Improve the Anti-Mycobacterial Activity of Current Drugs to Better Control Tuberculosis?

Ter‐Seq: A high‐throughput method to stabilize transient ternary complexes and measure associated kinetics

Are all VapC toxins of Mycobacterium tuberculosis endowed with enigmatic RNase activity?

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