Host-Directed Therapeutics for Tuberculosis: Can We Harness the Host?

Hawn, Thomas R.; Matheson, Alastair; Maley, Stephen N.; Vandal, Omar

doi:10.1128/mmbr.00032-13

Cited by 130 publications

(135 citation statements)

References 204 publications

(216 reference statements)

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“…ost-directed therapy (HDT) may offer expanded therapeutic options for improving tuberculosis (TB) treatment (1)(2)(3)(4)(5). Metformin (MetF), an AMP-activated protein kinase (AMPK)-activating drug for type 2 diabetes (DM), was reported to inhibit intracellular growth of mycobacteria by inducing reactive oxygen species and to enhance the efficacy of conventional anti-TB drugs in mouse models of acute and chronic TB; its use was associated with decreased TB severity and improved clinical outcomes in a retrospective analysis of 220 patients with DM and TB (6).…”

mentioning

confidence: 99%

Metformin Adjunctive Therapy Does Not Improve the Sterilizing Activity of the First-Line Antitubercular Regimen in Mice

Dutta

Pinn

Karakousis

2017

Antimicrob Agents Chemother

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Preliminary preclinical and observational studies suggest the potential utility of metformin as an adjunctive, host-directed agent for treatment of tuberculosis (TB). In this study, we sought to investigate the bactericidal and sterilizing activities of human-like exposures of metformin when given in combination with the firstline regimen against chronic tuberculosis in BALB/c mice. Mice receiving metformin adjunctive therapy had similar lung bacillary burdens with control mice during treatment, and the proportion of mice with microbiological relapse was similar between the two groups.KEYWORDS Mycobacterium tuberculosis, metformin, standard first-line regimen, BALB/c, bactericidal, sterilizing, host-directed therapy, relapse, cure, Denver regimen H ost-directed therapy (HDT) may offer expanded therapeutic options for improving tuberculosis (TB) treatment (1-5). Metformin (MetF), an AMP-activated protein kinase (AMPK)-activating drug for type 2 diabetes (DM), was reported to inhibit intracellular growth of mycobacteria by inducing reactive oxygen species and to enhance the efficacy of conventional anti-TB drugs in mouse models of acute and chronic TB; its use was associated with decreased TB severity and improved clinical outcomes in a retrospective analysis of 220 patients with DM and TB (6). In another retrospective study, Srujitha et al. showed that MetF use was associated with a 3.9-fold reduction in TB incidence among patients with DM (7). Based on these findings, we hypothesized that MetF adjunctive therapy would enhance the bactericidal and sterilizing activities of the standard first-line treatment (8, 9) against chronic TB infection in mice and shorten the duration of curative treatment as assessed by microbiological relapse.All animal-related procedures were approved by the Johns Hopkins University (JHU) School of Medicine Animal Care and Use Committee. A total of 170 female BALB/c mice aged 4 to 6 weeks (Charles River Labs, Wilmington, MA) were aerosol infected with Mycobacterium tuberculosis H37Rv (JHU) using the inhalation exposure system (GlasCol, Terre Haute, IN) calibrated to deliver ϳ10 2 CFU per mouse lung in two consecutive runs. After aerosol infection, the mice were randomized into the two treatment groups. Six weeks postinfection, the mice were treated daily (5 days/week) via esophageal cannulation with human-equivalent doses of rifampin (10 mg/kg), isoniazid (10 mg/kg), pyrazinamide (150 mg/kg), and ethambutol (100 mg/kg) (RHZE) with or without MetF (250 mg/kg) for up to 6 months (2, 10, 11). For the first 2 months of treatment, the mice received RHZE and, for the remaining 4 months, only rifampin and isoniazid (RH) to mirror the first-line regimen in humans. The rifampin dose preceded that of the other drugs by at least 1 h to prevent pharmacokinetic antagonism (12, 13). The dose of MetF (6) and is estimated (14) to be equivalent to 25 mg/kg in humans (15), which is well tolerated (15, 16). Groups of 5 mice were sacrificed on the day after infection, on the day of treatment initi...

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confidence: 99%

Metformin Adjunctive Therapy Does Not Improve the Sterilizing Activity of the First-Line Antitubercular Regimen in Mice

Dutta

Pinn

Karakousis

2017

Antimicrob Agents Chemother

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“…A main strategy for adjunctive HDT of TB involves the modulation of inflammatory pathways to allow reactivation of dormant bacilli within granulomas, thereby enhancing the activity of antimycobacterial drugs (15,16). Given that the antiinflammatory properties of pirfenidone are retained during TB (Figure 1), we explored whether pirfenidone could be used for TB treatment shortening.…”

Section: Resultsmentioning

confidence: 99%

“…The many pitfalls of using antibiotics, including the inevitable rise of antibiotic resistance, have led to exploration of host-directed therapies (HDTs) as part of the anti-TB arsenal (15)(16)(17)(18). The main strategies used to date, which have involved the enhancement of host antimicrobial mechanisms and cytokine modulation to reduce inflammation and pathology, have yielded varying degrees of success (15,16). In instances where HDTs have been assessed as adjunctive therapies, these have not proved superior to standard TB treatment (19,20).…”

Section: Introductionmentioning

confidence: 99%

The antifibrotic drug pirfenidone promotes pulmonary cavitation and drug resistance in a mouse model of chronic tuberculosis

et al. 2016

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“…Identification of the immunogenetic factors associated with resistance may lead to novel strategies for immunomodulatory therapy. These strategies might include the use of small-molecule drugs that target host macrophage pathways or vaccines that induce T-cell responses which activate macrophages to kill M. tuberculosis (107).…”

Section: Is Reducing Tb Acquisition Risk By Vaccination Plausible?mentioning

confidence: 99%

Tuberculosis Vaccines and Prevention of Infection

Hawn

Day

Scriba

et al. 2014

Microbiol Mol Biol Rev

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137

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SUMMARY Tuberculosis (TB) is a leading cause of death worldwide despite the availability of effective chemotherapy for over 60 years. Although Mycobacterium bovis bacillus Calmette-Guérin (BCG) vaccination protects against active TB disease in some populations, its efficacy is suboptimal. Development of an effective TB vaccine is a top global priority that has been hampered by an incomplete understanding of protective immunity to TB. Thus far, preventing TB disease, rather than infection, has been the primary target for vaccine development. Several areas of research highlight the importance of including preinfection vaccines in the development pipeline. First, epidemiology and mathematical modeling studies indicate that a preinfection vaccine would have a high population-level impact for control of TB disease. Second, immunology studies support the rationale for targeting prevention of infection, with evidence that host responses may be more effective during acute infection than during chronic infection. Third, natural history studies indicate that resistance to TB infection occurs in a small percentage of the population. Fourth, case-control studies of BCG indicate that it may provide protection from infection. Fifth, prevention-of-infection trials would have smaller sample sizes and a shorter duration than disease prevention trials and would enable opportunities to search for correlates of immunity as well as serve as a criterion for selecting a vaccine product for testing in a larger TB disease prevention trial. Together, these points support expanding the focus of TB vaccine development efforts to include prevention of infection as a primary goal along with vaccines or other interventions that reduce the rate of transmission and reactivation.

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Host-Directed Therapeutics for Tuberculosis: Can We Harness the Host?

Cited by 130 publications

References 204 publications

Metformin Adjunctive Therapy Does Not Improve the Sterilizing Activity of the First-Line Antitubercular Regimen in Mice

Metformin Adjunctive Therapy Does Not Improve the Sterilizing Activity of the First-Line Antitubercular Regimen in Mice

The antifibrotic drug pirfenidone promotes pulmonary cavitation and drug resistance in a mouse model of chronic tuberculosis

Tuberculosis Vaccines and Prevention of Infection

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