New test reveals which antibiotics truly kill bacteria

Scientists at the University of Basel have developed a novel testing method to determine whether antibiotics actually eliminate bacteria or merely halt their growth. This approach, called antimicrobial single-cell testing, tracks individual bacteria under a microscope to assess drug effectiveness more accurately. The findings, published in Nature Microbiology, highlight variations in bacterial tolerance to treatments for tuberculosis and other lung infections.

Antibiotic resistance poses a major global health challenge, with bacteria increasingly evading common drugs through genetic mutations. Even non-resistant bacteria can persist by entering a dormant state, where they cease multiplying but survive treatment, potentially reactivating infections later. This issue is particularly acute in prolonged therapies for tuberculosis and related lung conditions caused by Mycobacterium tuberculosis and Mycobacterium abscessus.

To address limitations in traditional lab tests, which focus on growth inhibition rather than outright killing, researchers led by Dr. Lucas Boeck from the University of Basel's Department of Biomedicine and University Hospital Basel introduced antimicrobial single-cell testing. This technique employs advanced microscopy to monitor millions of individual bacteria over several days under thousands of conditions. "We use it to film each individual bacterium over several days and observe whether and how quickly a drug actually kills it," Boeck explained.

In demonstrations, the team evaluated 65 drug combinations against Mycobacterium tuberculosis and analyzed samples from 400 patients with Mycobacterium abscessus infections. Results showed significant differences in efficacy between drug mixes and across bacterial strains, influenced by genetic factors that promote antibiotic tolerance. "The better bacteria tolerate an antibiotic, the lower the chances of therapeutic success are for the patients," Boeck noted. The method's predictions aligned closely with outcomes from clinical studies and animal models.

Currently used in research, this testing could extend to clinical settings and pharmaceutical development. It enables personalized antibiotic selection based on specific bacterial strains. "Our test method allows us to tailor antibiotic therapies specifically to the bacterial strains in individual patients," Boeck said. Furthermore, insights into bacterial survival mechanisms may inspire novel treatments. "Last but not least, the data can help researchers to better understand the survival strategies of pathogens and thus lay the foundation for new, more effective therapeutic approaches," he added.

The study underscores the need for precise tools in combating persistent infections, potentially improving patient outcomes and drug innovation.

Makala yanayohusiana

Illustration of Australian scientists developing antibodies targeting bacteria-specific sugar to treat drug-resistant infections in mice.
Picha iliyoundwa na AI

Australian team develops antibodies targeting a bacteria-only sugar, clearing drug-resistant infection in mice

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Australian researchers report they have engineered monoclonal antibodies that recognize pseudaminic acid—a sugar made by bacteria but not by humans—and used them to help eliminate multidrug-resistant Acinetobacter baumannii infections in mice, a step toward potential passive-immunotherapy treatments for hard-to-treat hospital infections.

As antibiotics increasingly fail, researchers at AIIMS Delhi are leading the battle against superbugs through early diagnosis, biomarker research, and rational antibiotic use. A recent case of a 50-year-old man with resistant bacterial meningitis underscores the urgency. The institute is running multiple projects to slow down antimicrobial resistance.

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Researchers from New England Biolabs and Yale University have developed the first fully synthetic system for engineering bacteriophages targeting Pseudomonas aeruginosa, a major antibiotic-resistant bacterium. Published in PNAS, the method uses digital DNA sequences to build viruses from scratch, bypassing traditional challenges in phage modification. This innovation aims to accelerate therapies against global antibiotic resistance threats.

Researchers at the University of California San Diego report they have developed a second-generation CRISPR-based “Pro-Active Genetics” system, called pPro-MobV, that is designed to spread between bacteria and disable antibiotic-resistance genes, including inside hard-to-treat biofilms.

Imeripotiwa na AI Imethibitishwa ukweli

Researchers at the University of California San Diego report that certain cancer cells survive targeted therapies by using low-level activation of a cell-death–linked enzyme, enabling them to endure treatment and later regrow tumors. Because this resistance mechanism does not depend on new genetic mutations, it appears early in treatment and may offer a new target to help prevent tumor relapse.

Researchers report that small doses of the antibiotic cephaloridine can prompt certain gut bacteria to increase production of colanic acid, a microbial polysaccharide previously tied to longer lifespan in laboratory animals. In experiments, treated roundworms lived longer and mice showed shifts in cholesterol or insulin measures associated with aging, with the team arguing the approach works by acting in the gut rather than throughout the body.

Imeripotiwa na AI Imethibitishwa ukweli

Researchers have identified indole metabolites from the human blood bacterium Paracoccus sanguinis that showed anti-aging activity in laboratory-grown human skin cells. The compounds reduced oxidative stress, inflammation and collagen-degrading activity in cell experiments, according to findings published in the Journal of Natural Products.

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