4.7 Article

Simvastatin increases the in vivo activity of the first-line tuberculosis regimen

Journal

JOURNAL OF ANTIMICROBIAL CHEMOTHERAPY
Volume 69, Issue 9, Pages 2453-2457

Publisher

OXFORD UNIV PRESS
DOI: 10.1093/jac/dku166

Keywords

TB; statins; lipids; mice

Funding

  1. [R01 HL106788]
  2. [R01 AI083125]
  3. [R01 HL106786]

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Background: The need to develop new, improved treatments for tuberculosis (TB) remains urgent, and the repurposing of existing drugs represents a possible shortcut to market. Recently, there has been significant interest in host-directed adjuvant therapy to enhance bacillary killing. HMG-CoA reductase inhibitors (statins), which are among the most commonly prescribed drugs, have immunomodulatory properties and improve the clinical outcomes of bacterial infections. Methods: We studied the tuberculocidal activity of simvastatin alone and in combination with first-line anti-TB drugs in J774 macrophages and during chronic TB infection. Results: Exposure to 5 mu M simvastatin significantly increased the tuberculocidal activity of isoniazid in J774 macrophages at Day 3 after infection versus isoniazid alone (P=0.02). Similarly, relative to the standard oral regimen of rifampicin (10 mg/kg), isoniazid (10 mg/kg) and pyrazinamide (150 mg/kg) given five times weekly, the addition of 25 mg/kg simvastatin enhanced bacillary killing, reducing the number of lung cfu by an additional 1 log(10) at Day 28 (P<0.01) and by a further 1.25 log(10) at Day 56 (P<0.01). Conclusions: The potential additive activity of simvastatin to first-line TB treatment holds promise. However, further studies to identify the optimal statin and dosing are required. In addition the ability of combination treatment with statins to accelerate the time required to achieve a stable cure remains to be explored.

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