New and repurposed drugs to treat multidrug- and extensively drug-resistant tuberculosis

Silva, Denise Rossato; Dalcolmo, Margareth; Tiberi, Simon; Arbex, Marcos Abdo; Munoz-Torrico, Marcela; Duarte, Raquel; D’Ambrosio, Lia; Visca, Dina; Rendon, Adrian; Gaga, Mina; Zumla, Alimuddin; Migliori, Giovanni Battista

doi:10.1590/S1806-37562017000000436

Acessibilidade / Reportar erro

Brasil

Jornal Brasileiro de Pneumologia

Español English

Brasil

Español English

sumário « anterior atual seguinte »

Sumário

REVIEW ARTICLE • J. bras. pneumol. 44 (02) • Mar-Apr 2018 • https://doi.org/10.1590/S1806-37562017000000436 copy

New and repurposed drugs to treat multidrug- and extensively drug-resistant tuberculosis

Authorship SCIMAGO INSTITUTIONS RANKINGS

ABSTRACT

Multidrug-resistant and extensively drug-resistant tuberculosis (MDR-TB and XDR-TB, respectively) continue to represent a challenge for clinicians and public health authorities. Unfortunately, although there have been encouraging reports of higher success rates, the overall rate of favorable outcomes of M/XDR-TB treatment is only 54%, or much lower when the spectrum of drug resistance is beyond that of XDR-TB. Treating M/XDR-TB continues to be a difficult task, because of the high incidence of adverse events, the long duration of treatment, the high cost of the regimens used, and the drain on health care resources. Various trials and studies have recently been undertaken (some already published and others ongoing), all aimed at improving outcomes of M/XDR-TB treatment by changing the overall approach, shortening treatment duration, and developing a universal regimen. The objective of this review was to summarize what has been achieved to date, as far as new and repurposed drugs are concerned, with a special focus on delamanid, bedaquiline, pretomanid, clofazimine, carbapenems, and linezolid. After more than 40 years of neglect, greater attention has recently been paid to the need for new drugs to fight the “white plague”, and promising results are being reported.

Keywords:
Tuberculosis/therapy; Tuberculosis, multidrug-resistant; Extensively drug-resistant tuberculosis; Antitubercular agents

Class	Drug(s)	Target	Phase	Notes
Diarylquinoline	Bedaquiline	ATP synthase	3	Conditional marketing approval
Imidazopyridine amide	Q203	Targets the cytochrome b subunit of the cytochrome bc1 complex, essential for the respiratory electron chain, also depletes intracellular ATP	1	Phase 1b safety studies completed in the United States
				Phase 1 dose-escalation study underway (NCT02858973)
		Activity similar to that of bedaquiline		Phase 1 dose-escalation study underway (NCT02858973)
		Activity similar to that of bedaquiline		Early bactericidal activity study expected to have started before the end of 2017
Nitroimidazole	Delamanid	Inhibit cell wall synthesis and cell respiration	3	Conditional marketing approval
Nitroimidazole	Pretomanid	Inhibit cell wall synthesis and cell respiration	3	Awaiting regulatory approval
Oxazolidinone	Sutezolid	Protein synthesis 23s ribosome	2a	Significant reduction in counts of colony-forming units in an early bactericidal activity study
	Sutezolid		2a	Phase 1a completed only recently (NCT03199313), due to licensing problems
	Delpazolid (LCB01-0371)		2	A phase 2 safety and early bactericidal activity study of the drug expected to be completed in late 2017
1,2-ethylenediamine	SQ109	Inhibit cell wall synthesis (MmpL3)	2-3	May be synergic with bedaquiline
1,2-ethylenediamine	SQ109	Inhibit cell wall synthesis (MmpL3)	2-3	Two SQ109-containing arms in a PanACEA trial testing high-dose rifampin stopped early because pre-specified efficacy thresholds were not met
Benzothiazinone	PBTZ169	DprE1 inhibitors (inhibit cell wall synthesis)	2	Synergies with bedaquiline and clofazimine
	OPC-167832		1	Co-developed as a companion drug for delamanid in view of a pan-tuberculosis regimen
	TBA-7371		1	Phase 1a trial has begun (NCT03199339)
Riminophenazine	TBI-166	Outer membrane, bacterial respiratory chain and ion transporters	1	Improved analogue of clofazimine
Riminophenazine	TBI-166		1	Phase 1 to commence in China in October of 2017
Oxaborole	GSK 070, GSK 3036656	Protein synthesis (leucyl-tRNA synthetase)	1	Phase 1 completed (NCT03075410)

Sociedade Brasileira de Pneumologia e Tisiologia SCS Quadra 1, Bl. K salas 203/204, 70398-900 - Brasília - DF - Brasil, Fone/Fax: 0800 61 6218 ramal 211, (55 61)3245-1030/6218 ramal 211 - São Paulo - SP - Brazil
E-mail: jbp@sbpt.org.br

Acompanhe os números deste periódico no seu leitor de RSS

[1] Correspondence to: Giovanni Battista Migliori. WHO Collaborating Centre for TB and Lung Diseases, Maugeri Care and Research Institute, Tradate, Italia. Via Roncaccio 16, 21049, Tradate, Italy. Tel +39. 0331. 829404; Fax +39. 0331. 829402. E-mail: giovannibattista.migliori@icsmaugeri.it

Group A	Fluoroquinolones	Levofloxacin*
		Moxifloxacin*
		Gatifloxacin*^,†
Group B	Aminoglycosides	Amikacin*
		Capreomycin
		Kanamycin
		(Streptomycin)^‡
Group C	Other core second-line agents	Ethionamide/prothionamide
		Cycloserine/terizidone
		Linezolid*
		Clofazimine*
Group D	Add-on agents (non-core MDR-TB regimen)	D1
		Pyrazinamide
		Ethambutol
		High-dose isoniazid
		D2
		Bedaquiline^§
		Delamanid^§
		D3
		Para-aminosalicylic acid
		Imipenem plus cilastatin (requires clavulanate)*
		Meropenem (requires clavulanate)*
		Amoxicillin plus clavulanate*
		Thioacetazone*^,║