Inhibiting DosRST As a New Approach to Tuberculosis Therapy

Zheng, Huiqing; Abramovitch, Robert B.

doi:10.4155/fmc-2019-0263

Cited by 21 publications

(19 citation statements)

References 94 publications

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“…Furthermore, it has been established that the DosR regulon is required for Mtb to establish an NRP state and survive during hypoxia [ 42 ], which supports the idea that CtpF is an interesting attenuation target to design novel vaccines, and may even be a new target for anti-TB compounds [ 38 , 70 ].…”

Section: Discussionmentioning

confidence: 85%

“…As stated above, the expression of ctpF is controlled by DosR [ 44 ], which is involved in maintaining low bacterial growth under unfavorable conditions (such as in granulomas), entering into a dormant state and maintaining it for a long time within the host [ 41 , 42 , 43 , 44 , 45 , 56 ]. Therefore, we used qRT-PCR to compare the absolute transcription levels of ctpF in a model of progressive pulmonary TB and latent TB infection in BALB/c mice ( Figure 6 ).…”

Section: Resultsmentioning

confidence: 99%

“…It had been previously established that CtpF is a membrane transporter involved in calcium pumping outside mycobacterial cells, and in the response to oxidative/nitrosative stress [ 40 ]. Moreover, ctpF is the only Mtb P-type ATPase gene regulated by the global latency regulator (DosR), which is involved in the adaptation of bacilli to anaerobic environments, acidic pH, starvation and high nitric oxide (NO) intermediates inside macrophages and granulomas; thus, ctpF promotes a non-replicating persistence (NRP) or dormancy state [ 41 , 42 , 43 , 44 , 45 ]. Therefore, the fact that ctpF is part of the DosR regulon and its expression is activated in response to redox stress (a condition faced by the tubercle bacillus in the phagosomal environment) suggests that the role of this transporter is critical during Mtb infection.…”

Section: Introductionmentioning

confidence: 99%

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The ctpF Gene Encoding a Calcium P-Type ATPase of the Plasma Membrane Contributes to Full Virulence of Mycobacterium tuberculosis

Maya-Hoyos

Mata-Espinosa

López-Torres

et al. 2022

IJMS

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Identification of alternative attenuation targets of Mycobacterium tuberculosis (Mtb) is pivotal for designing new candidates for live attenuated anti-tuberculosis (TB) vaccines. In this context, the CtpF P-type ATPase of Mtb is an interesting target; specifically, this plasma membrane enzyme is involved in calcium transporting and response to oxidative stress. We found that a mutant of MtbH37Rv lacking ctpF expression (MtbΔctpF) displayed impaired proliferation in mouse alveolar macrophages (MH-S) during in vitro infection. Further, the levels of tumor necrosis factor and interferon-gamma in MH-S cells infected with MtbΔctpF were similar to those of cells infected with the parental strain, suggesting preservation of the immunogenic capacity. In addition, BALB/c mice infected with Mtb∆ctpF showed median survival times of 84 days, while mice infected with MtbH37Rv survived 59 days, suggesting reduced virulence of the mutant strain. Interestingly, the expression levels of ctpF in a mouse model of latent TB were significantly higher than in a mouse model of progressive TB, indicating that ctpF is involved in Mtb persistence in the dormancy state. Finally, the possibility of complementary mechanisms that counteract deficiencies in Ca2+ transport mediated by P-type ATPases is suggested. Altogether, our results demonstrate that CtpF could be a potential target for Mtb attenuation.

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Section: Discussionmentioning

confidence: 85%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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The ctpF Gene Encoding a Calcium P-Type ATPase of the Plasma Membrane Contributes to Full Virulence of Mycobacterium tuberculosis

Maya-Hoyos

Mata-Espinosa

López-Torres

et al. 2022

IJMS

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“…Oxygen levels in cells are detected through more or less complex biochemical sensors, depending on the organism [ 156 ]. In the case of M.tb , its presence or absence is determined by DevS and DosT, two oxygen heme-based sensors, which function like a two-component system along with DevR, a response regulator [ 157 ]. By sensing variations in the levels of oxygen in the surrounding media, these promote a series of metabolic changes in the bacillus, initiating the process of latency.…”

Section: Targeting Nonreplicating Mtbmentioning

confidence: 99%

Addressing Latent Tuberculosis: New Advances in Mimicking the Disease, Discovering Key Targets, and Designing Hit Compounds

Campaniço

Harjivan

Warner

et al. 2020

IJMS

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Despite being discovered and isolated more than one hundred years ago, tuberculosis (TB) remains a global public health concern arch. Our inability to eradicate this bacillus is strongly related with the growing resistance, low compliance to current drugs, and the capacity of the bacteria to coexist in a state of asymptomatic latency. This last state can be sustained for years or even decades, waiting for a breach in the immune system to become active again. Furthermore, most current therapies are not efficacious against this state, failing to completely clear the infection. Over the years, a series of experimental methods have been developed to mimic the latent state, currently used in drug discovery, both in vitro and in vivo. Most of these methods focus in one specific latency inducing factor, with only a few taking into consideration the complexity of the granuloma and the genomic and proteomic consequences of each physiological factor. A series of targets specifically involved in latency have been studied over the years with promising scaffolds being discovered and explored. Taking in account that solving the latency problem is one of the keys to eradicate the disease, herein we compile current therapies and diagnosis techniques, methods to mimic latency and new targets and compounds in the pipeline of drug discovery.

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“…This latter TCS (given different names in different species (YycFG, WalRK, VicRK)), has attracted particular attention with regard to novel chemicals agents that inhibit its activities, and although the essentiality of such TCSs often resides with the RR component, many inhibitor studies have focused on the membrane-located SHK components (see [ 61 ] for a recent listing of some examples). Several additional recent reviews of inhibitors of SHK and/or RR components have been published [ 17 , 18 , 21 , 23 , 25 , 62 , 63 , 64 , 65 , 66 ].…”

Section: Introductionmentioning

confidence: 99%

Membrane Sensor Histidine Kinases: Insights from Structural, Ligand and Inhibitor Studies of Full-Length Proteins and Signalling Domains for Antibiotic Discovery

Phillips‐Jones

2021

Molecules

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There is an urgent need to find new antibacterial agents to combat bacterial infections, including agents that inhibit novel, hitherto unexploited targets in bacterial cells. Amongst novel targets are two-component signal transduction systems (TCSs) which are the main mechanism by which bacteria sense and respond to environmental changes. TCSs typically comprise a membrane-embedded sensory protein (the sensor histidine kinase, SHK) and a partner response regulator protein. Amongst promising targets within SHKs are those involved in environmental signal detection (useful for targeting specific SHKs) and the common themes of signal transmission across the membrane and propagation to catalytic domains (for targeting multiple SHKs). However, the nature of environmental signals for the vast majority of SHKs is still lacking, and there is a paucity of structural information based on full-length membrane-bound SHKs with and without ligand. Reasons for this lack of knowledge lie in the technical challenges associated with investigations of these relatively hydrophobic membrane proteins and the inherent flexibility of these multidomain proteins that reduces the chances of successful crystallisation for structural determination by X-ray crystallography. However, in recent years there has been an explosion of information published on (a) methodology for producing active forms of full-length detergent-, liposome- and nanodisc-solubilised membrane SHKs and their use in structural studies and identification of signalling ligands and inhibitors; and (b) mechanisms of signal sensing and transduction across the membrane obtained using sensory and transmembrane domains in isolation, which reveal some commonalities as well as unique features. Here we review the most recent advances in these areas and highlight those of potential use in future strategies for antibiotic discovery. This Review is part of a Special Issue entitled “Interactions of Bacterial Molecules with Their Ligands and Other Chemical Agents” edited by Mary K. Phillips-Jones.

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Inhibiting DosRST As a New Approach to Tuberculosis Therapy

Cited by 21 publications

References 94 publications

The ctpF Gene Encoding a Calcium P-Type ATPase of the Plasma Membrane Contributes to Full Virulence of Mycobacterium tuberculosis

The ctpF Gene Encoding a Calcium P-Type ATPase of the Plasma Membrane Contributes to Full Virulence of Mycobacterium tuberculosis

Addressing Latent Tuberculosis: New Advances in Mimicking the Disease, Discovering Key Targets, and Designing Hit Compounds

Membrane Sensor Histidine Kinases: Insights from Structural, Ligand and Inhibitor Studies of Full-Length Proteins and Signalling Domains for Antibiotic Discovery

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