Perspectives for personalized therapy for patients with multidrug‐resistant tuberculosis

Lange, Christoph; Alghamdi, Wael; Al‐Shaer, Mohammad H.; Brighenti, Susanna; Diacon, Andreas H.; DiNardo, Andrew; Grobbel, Hans-Peter; Gröschel, Matthias I.; Groote-Bidlingmaier, Florian von; Hauptmann, Matthias; Heyckendorf, Jan; Köhler, Niklas; Köhl, Thomas; Merker, Matthias; Niemann, Stefan; Peloquin, Charles A.; Reimann, Maja; Schaible, Ulrich E.; Schaub, Dagmar; Schleusener, Viola; Thye, Thorsten; Schӧn, Thomas

doi:10.1111/joim.12780

Cited by 34 publications

(36 citation statements)

References 232 publications

(267 reference statements)

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“…There are approximately 500,000 new MDR-TB cases per year and the treatment success rates for MDR-TB is currently 55% compared to 85% for drug-susceptible TB [1]. MDR-TB treatment is associated with costly therapy by second-line drugs for longer periods, sometimes up to two years, which is accompanied with more complex side-effects [10]. In addition, extensively drug-resistant-TB (XDR-TB) is the most severe form that has a global treatment success rate of 30%, leading to high mortality and morbidity, especially in TB/HIV co-infected patients [11].…”

Section: Introductionmentioning

confidence: 99%

Host-Directed Therapy as a Novel Treatment Strategy to Overcome Tuberculosis: Targeting Immune Modulation

et al. 2020

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Tuberculosis (TB) is one of the leading causes of mortality and morbidity, particularly in developing countries, presenting a major threat to the public health. The currently recommended long term treatment regimen with multiple antibiotics is associated with poor patient compliance, which in turn, may contribute to the emergence of multi-drug resistant TB (MDR-TB). The low global treatment efficacy of MDR-TB has highlighted the necessity to develop novel treatment options. Host-directed therapy (HDT) together with current standard anti-TB treatments, has gained considerable interest, as HDT targets novel host immune mechanisms. These immune mechanisms would otherwise bypass the antibiotic bactericidal targets to kill Mycobacterium tuberculosis (Mtb), which may be mutated to cause antibiotic resistance. Additionally, host-directed therapies against TB have been shown to be associated with reduced lung pathology and improved disease outcome, most likely via the modulation of host immune responses. This review will provide an update of host-directed therapies and their mechanism(s) of action against Mycobacterium tuberculosis.

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Section: Introductionmentioning

confidence: 99%

Host-Directed Therapy as a Novel Treatment Strategy to Overcome Tuberculosis: Targeting Immune Modulation

et al. 2020

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“…For some antituberculosis drugs, dose adjustments are indicated in patients with renal or hepatic impairment. Therapeutic drug concentration monitoring may have a role in some settings and is reviewed elsewhere as part of the approach to personalized therapy for DR-TB [28,29]. These topics are not included in this review.…”

Section: Introductionmentioning

confidence: 99%

Current research toward optimizing dosing of first-line antituberculosis treatment

McIlleron

Chirehwa

2018

Expert Review of Anti-infective Therapy

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Introduction: Drug concentrations in tuberculosis patients on standard regimens vary widely with clinically important consequences.Areas covered: We review the available literature identifying factors correlated with pharmacokinetic variability of antituberculosis drugs. Based on population pharmacokinetic models and the weight, height, and sex distributions in a large data base of African tuberculosis patients, we propose simplified weight-based doses of the available fixed dose combination(FDC) for adults with drug susceptible tuberculosis. Emerging studies will support optimized weight-based dosing for children. Other sources of important pharmacokinetic variability include genetic variants, drug-drug interactions, formulation quality, and methods of preparation and administration.Expert commentary: Optimized weight band-based dosing will result in more equitable distribution of drug exposures by weight. The use of high doses of isoniazid in patients with drug-resistant tuberculosis would be safer and more effective if a feasible test was developed to allow stratified dosing according to acetylator type. There is an urgent need for more suitable formulations of many second-line drugs for children. The adoption of new technologies and efficient FDC design may allow further advances for patients and treatment programs. Lastly, current efforts to ensure adequate quality of antituberculosis drug products are not preventing the use of substandard products to treat patients with tuberculosis.

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“…As this is a major pitfall detection of resistance mutations by gDST can elucidate whether isolates with MIC below but close to the critical concentration are wild-type or not i.e. the gDST result may overrule pDST (59,92).…”

Section: Breakpoints Used For Tb Drugsmentioning

confidence: 99%

“…Furthermore, opinions vary regarding the utility and cost-benefit of TDM (139)(140)(141). Despite knowledge gaps, experts in the field promote the use of TDM for TB and guidelines and reviews have also acknowledged this, but not routinely for all patients (92,108,141,142). Presently, therapeutic drug monitoring is mainly used in high-resource settings in case of therapy failure, MDR/XDR-TB or severe adverse drug reactions.…”

Section: The Role Of Therapeutic Drug Monitoring In Tuberculosis Treamentioning

confidence: 99%

“…Until a universal reference method for pDST has been established and breakpoints properly revised, it is advisable in difficult cases with complicated resistance to use pDST in combination with gDST because of the influence of the inherent technical variability of pDST. Further, a reliable standardised pDST is needed to draw the map of genotype-phenotype correlations by gathering data on the phenotypic profiles of the different drug resistance mutations, as well as for resistance screening of new drugs entering the market (92). Hopefully in the future, WGS will have the ability to relate all resistance mutations of TB drugs to phenotypic susceptibility, enabling early design of an adequate treatment regimen and correct dose prescriptions.…”

Section: Consequences Of Poorly Defined Breakpointsmentioning

confidence: 99%

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Towards individualised treatment of tuberculosis

Niward

2019

Linköping University Medical Dissertations

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Each year, around 10 million of individuals develop active tuberculosis (TB). Worldwide, TB is the leading cause of death from an infectious agent surpassing both malaria and HIV. Current treatment regimens are long and therefore encompass a risk of nonadherence and development of acquired drug-resistance, reflected in the increase of multidrug-resistant (MDR) and extensively drug-resistant (XDR) TB. Indeed, this calls for prudent use of existing TB drugs and improvement of TB treatment strategies. The aim of this thesis was to investigate the current drug susceptibility testing (DST) breakpoints for Mycobacterium tuberculosis (M. tuberculosis), the pharmacokinetics and pharmacodynamics (PK/PD) of TB treatment and to explore the role of therapeutic drug monitoring (TDM) for optimising TB treatment. LIST OF SCIENTIFIC PAPERS This thesis is based on the following publications, referred to in the text by their Roman numerals.

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Perspectives for personalized therapy for patients with multidrug‐resistant tuberculosis

Cited by 34 publications

References 232 publications

Host-Directed Therapy as a Novel Treatment Strategy to Overcome Tuberculosis: Targeting Immune Modulation

Host-Directed Therapy as a Novel Treatment Strategy to Overcome Tuberculosis: Targeting Immune Modulation

Current research toward optimizing dosing of first-line antituberculosis treatment

Towards individualised treatment of tuberculosis

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