While standard anti-TB drugs can cure most people of Mycobacterium tuberculosis infection, improper use of antibiotics has led to new strains of the bacterium resistant to the two most powerful medications, isoniazid and rifampicin.
"Multi-drug resistant TB is spreading rapidly in many parts of the world," said Vasu Nair, Georgia Research Alliance Eminent Scholar in Drug Discovery in the University of Georgia College of Pharmacy.
"There is a tremendous need for new therapies, and we think our laboratory has developed a strong candidate that disrupts fundamental steps in the bacterium's reproduction process," said Nair, lead author of the study in the journal Bioorganic and Medicinal Chemistry Letters.
This molecule is involved in processes that produce critical bacterial proteins that the organism needs to survive.
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The compound Nair and his colleagues developed works by binding to magnesium and specific amino acids found within the bacterium, interrupting the production of RNA.
"The compound we developed strongly inhibits the growth of the bacterium and renders it incapable of reproducing and spreading infection," Nair said.
"More importantly, the compound shows very low levels of cytotoxicity, which means that it is not harmful to the body," he said.
"All our tests were very favourable. The half-life is a little over 14 hours, and all traces of the drug are expected to be cleared through normal bodily functions," Nair said.
Nair and his colleagues said they were surprised to discover through preliminary experiments that the compound also exhibited strong anti-HIV properties, opening the door for dual therapeutic applications.
The risk for developing TB is between 26 and 31 times greater in people living with HIV than those without HIV infection, according to the World Health Organization (WHO).