Four-Month Moxifloxacin-Based Regimens for Drug-Sensitive Tuberculosis

Gillespie, Stephen H.; Crook, Angela M.; McHugh, Timothy D.; Mendel, Carl M.; Meredith, Sarah; Murray, Stephen R.; Pappas, Frances; Phillips, Patrick P. J.; Nunn, Andrew

doi:10.1056/nejmoa1407426

Cited by 557 publications

(624 citation statements)

References 23 publications

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“…In 2014, three trials were reported that relate to treatment shortening based on the substitution of a fluoroquinolone [9][10][11].…”

Section: Early-phase Clinical Studies Of Moxifloxacinmentioning

confidence: 99%

“…The important approach to TB drug development that can yield results rapidly is to repurpose drugs that also have activity against TB. Moxifloxacin is an example of this process and will be the focus of this review, which is timely as the results of three phase III clinical trials utilising a fluoroquinolone as a key component in the treatment of susceptible infection have been reported recently [9][10][11] and novel moxifloxacin regimens for the treatment of MDR disease are in progress [12]. Moxifloxacin also has an important role in the management of patients who are unable to tolerate a …”

Section: Introductionmentioning

confidence: 99%

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The role of moxifloxacin in tuberculosis therapy

Gillespie

2016

Eur Respir Rev

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Tuberculosis (TB) remains a global threat with more than 9 million new infections. Treatment remains difficult and there has been no change in the duration of the standard regimen since the early 1980s. Moreover, many patients are unable to tolerate this treatment and discontinue therapy, increasing the risk of resistance. There is a growing tide of multidrug resistance and few effective antibiotics to tackle the problem. Since the turn of the millennium there has been a surge in interest in developing new therapies for TB and a number of new drugs have been developed. In this review the repurposing of moxifloxacin, an 8-methoxy-fluoroquinolone, for TB treatment is discussed. The evidence that underpins the development of this agent is reviewed. The results of the recently completed phase III trials are summarised and the reasons for the unexpected outcome are explored. Finally, the design of new trials that incorporate moxifloxacin, and that address both susceptible disease and multidrug resistance, is described. @ERSpublications A review of the role of moxifloxacin in tuberculosis therapy http://ow.ly/WaAyC

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“…In 2014, three trials were reported that relate to treatment shortening based on the substitution of a fluoroquinolone [9][10][11].…”

Section: Early-phase Clinical Studies Of Moxifloxacinmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

The role of moxifloxacin in tuberculosis therapy

Gillespie

2016

Eur Respir Rev

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“…It is known that the majority of relapses occur within six months of stopping treatment in clinical trials of DS-TB (18,19) and results from REMoxTB (20), RIFAQUIN(21) and OFLOTUB (22) have confirmed this. Some groups are therefore designing clinical trials in DS-TB with the primary endpoint 12 months after randomisation (i.e.…”

Section: Duration and Frequency Of Follow-upmentioning

confidence: 87%

Methodological considerations in clinical trials for new MDR-TB treatment regimens

Phillips

2016

int j tuberc lung dis

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(108 words)In stark contrast to the treatment of drug-sensitive TB, the evidence base underpinning global guidelines for the treatment of MDR-TB is very poor. This, with the lack of experience from previous trials and the nature of the disease, means that there are a number of methodological aspects that are particular to trials of new regimens for MDR-TB. These aspects include the weight of evidence required to change policy and practice, the flexibility to make adaptations to an ongoing trial, the choice of patient population, the importance of the internal control, the duration and frequency of follow-up, and particular safety monitoring for novel combinations of new and repurposed drugs.

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“…The disappointing results from all recent Phase III trials of TB drugs [2][3][4][5] clearly demonstrate that a shift in paradigm is needed in TB drug development. Insufficient efficacy is the main cause for failures in clinical drug development [6,7].…”

Section: Shift In the Tb Drug Development Paradigm: Reality Or Fiction?mentioning

confidence: 99%