AI Article Synopsis

  • Tuberculosis is a major global health threat, necessitating a deeper understanding of the factors that influence its outcomes, including host, environment, and bacterial characteristics.
  • Recent findings reveal six large genetic variations unique to Haarlem strains of Mycobacterium tuberculosis, including deletions and insertions, which may affect the strain's biology and potential drug targets.
  • These genetic markers can enhance the identification of Haarlem strains through rapid PCR testing, highlighting the need for a core set of genes that all TB strains share for better drug and vaccine development.

Article Abstract

Tuberculosis is the world's leading cause of death due to a single infectious agent, and efforts aimed at its control require a better understanding of host, environmental, and bacterial factors that govern disease outcome. Growing evidence indicates that certain Mycobacterium tuberculosis strains of distinct phylogeographic lineages elicit unique immunopathological events. However, identifying the genetic basis of these phenotypic peculiarities has proven difficult. Here we report the presence of six large sequence polymorphisms which, together with two single-nucleotide changes previously described by our group, consistently differentiate Haarlem strains from the remaining M. tuberculosis lineages. The six newly found Haarlem-specific genetic events are four deletions, which altogether involve more than 13 kb, and two intragenic insertions of the element IS6110. The absence of the genes involved in these polymorphisms could have an important physiological impact on Haarlem strains, i.e., by affecting key genes, such as Rv1354c and cyp121, which have been recently proposed as plausible drug targets. These lineage-specific polymorphisms can serve as genetic markers for the rapid PCR identification of Haarlem strains, providing a useful tool for strain surveillance and molecular epidemiology studies. Strain variability such as that described here underscores the need for the definition of a core set of essential genes in M. tuberculosis that are ubiquitously present in all circulating lineages, as a requirement in the development of effective antituberculosis drugs and vaccines.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC2953103PMC
http://dx.doi.org/10.1128/JCM.00157-10DOI Listing

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