A global perspective on pyrazinamide resistance: systematic review and meta-analysis
Abstract
Background
Pyrazinamide (PZA) is
crucial for tuberculosis (TB) treatment, given its unique
ability to eradicate persister bacilli. The worldwide burden of
PZA resistance remains poorly described.
Methods
Systematic PubMed, Science
Direct and Scopus searches for articles reporting phenotypic
(liquid culture drug susceptibility testing or pyrazinamidase
activity assays) and/or genotypic (polymerase chain reaction or
DNA sequencing) PZA resistance. Global and regional summary
estimates were obtained from random-effects meta-analysis,
stratified by presence or risk of multidrug resistant TB
(MDR-TB). Regional summary estimates were combined with regional
WHO TB incidence estimates to determine the annual burden of PZA
resistance. Information on single nucleotide polymorphisms
(SNPs) in the pncA gene was aggregated to obtain a global
summary.
Results
Pooled PZA resistance
prevalence estimate was 16.2% (95% CI 11.2-21.2) among all TB
cases, 41.3% (29.0-53.7) among patients at high MDR-TB risk, and
60.5% (52.3-68.6) among MDR-TB cases. The estimated global
burden is 1.4 million new PZA resistant TB cases annually, about
270,000 in MDR-TB patients. Among 1,815 phenotypically resistant
isolates, 608 unique SNPs occurred at 397 distinct positions
throughout the pncA gene.
Interpretation
PZA resistance is
ubiquitous, with an estimated one in six incident TB cases and
more than half of all MDR-TB cases resistant to PZA globally.
The diversity of SNPs across the pncA gene complicates the
development of rapid molecular diagnostics. These findings
caution against relying on PZA in current and future TB drug
regimens, especially in MDR-TB patients.
To read the article in full, click
here.
Source:
PLOS ONE
