Access to new medications for the treatment of drug-resistant tuberculosis: Patient, provider and community perspectives

Lessem, Erica; Cox, Helen; Daniels, Colleen; Furin, Jennifer; McKenna, Lindsay; Mitnick, Carole D.; Mosidi, Thato; Reed, Caitlin; Seaworth, Barbara; Stillo, Jonathan; Tisile, Phumeza; Delft, Dalene von

doi:10.1016/j.ijid.2014.12.012

Cited by 36 publications

(35 citation statements)

References 11 publications

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“…Among them, linezolid has been clearly identified in two small randomized clinical trials [27,28] and different meta-analyses as the key drug for XDR-TB regimens [29,30], but frequent, and sometime severe side effects limit its use. Despite the Global Drug Facility is currently offering 600 mg pills at $8 (US), the market price unfortunately still limits its use in most developing countries [31].…”

Section: New Drugsmentioning

confidence: 99%

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The changing landscape in drug resistant-tuberculosis: an analysis of recent advances

Monedero¹,

Caminero²,

Bhavaraju

et al. 2016

Expert Review of Respiratory Medicine

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Section: New Drugsmentioning

confidence: 99%

“…Again price and injectable formulations reduce its availability for long treatments in most developing countries [31]. In any case, this group merits further evaluation, especially the new drugs with greater half-life allowing daily outpatient intake like ertapenem [35] or the new oral forms like faropenem [36].…”

Section: New Drugsmentioning

confidence: 99%

The changing landscape in drug resistant-tuberculosis: an analysis of recent advances

Monedero¹,

Caminero²,

Bhavaraju

et al. 2016

Expert Review of Respiratory Medicine

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“…This seems low in the face of the great need for novel anti-TB treatments [9]. What can be done to improve this figure?…”

Section: To the Editormentioning

confidence: 99%

Recruitment challenges for clinical trials with novel regimens for drug-resistant tuberculosis

et al. 2015

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“…amikacin, capreomycin, kanamycin) [19]. In addition, delamanid appears to offer a better tolerability profile, as these injectable agents may cause severe adverse events such as deafness, vestibular toxicity, electrolyte imbalances and renal impairment [19,23]. Delamanid-based therapy was generally well tolerated in clinical trials; however, its use may be limited by the potential risk of QT interval prolongation.…”

Section: What Is the Tolerability Profile Of Delamanid?mentioning

confidence: 99%

Delamanid in multidrug-resistant tuberculosis: a guide to its use in the EU

Lyseng‐Williamson

Blair

Scott

2015

Drugs Ther Perspect

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Oral delamanid (Deltyba Ò ) is a useful addition to the treatment options currently available to treat patients with multidrug-resistant tuberculosis (MDR-TB). In the EU, it is indicated for use as part of an appropriate combination regimen in adults with MDR-TB when an effective treatment regimen cannot otherwise be composed due to resistance or tolerability. It exhibits potent antitubercular activity against drug-susceptible and -resistant strains of Mycobacterium tuberculosis. In a 3-month randomized control trial (2 months treatment ? 1 month follow-up) in adults with MDR-TB, delamanid 100 mg twice daily ? an optimized background regimen (OBR) improved 2-month sputum culture conversion rates to a significantly greater extent than placebo ? OBR. In consecutive extension and follow-up studies, treatment with delamanid for C6 to 8 months was associated with higher rates of favourable outcomes and lower rates of unfavourable outcomes than treatment for B2 months. Delamanid was generally well tolerated in patients with MDR-TB. To reduce the potential risk of QT interval prolongation with delamanid, recommendations regarding monitoring and precautionary measures should be followed.Adis evaluation of delamanid as part of appropriate combination regimen in multidrug-resistant tuberculosis Improves sputum culture conversion rates when added to optimal background regimens Treatment for C6 to 8 months provides higher rates of favourable outcomes and lower rates of unfavourable outcomes (including mortality) than treatment for B2 months Not associated with clinically relevant pharmacokinetic drug interactions Generally well tolerated Associated with an increased risk of QT interval prolongation (use requires caution in at-risk patient populations)

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Access to new medications for the treatment of drug-resistant tuberculosis: Patient, provider and community perspectives

Cited by 36 publications

References 11 publications

The changing landscape in drug resistant-tuberculosis: an analysis of recent advances

The changing landscape in drug resistant-tuberculosis: an analysis of recent advances

Recruitment challenges for clinical trials with novel regimens for drug-resistant tuberculosis

Delamanid in multidrug-resistant tuberculosis: a guide to its use in the EU

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