Surrey Scientists Target Gene Pathways in TB Zombie Cells, Offering Hope to Cut Treatment Time for 1.3M Annual Deaths

Scientists at the University of Surrey have discovered how to target tuberculosis (TB) bacteria that hide from antibiotics. This finding could lead to better treatments for a disease that kills 1.3 million people every year.

TB remains deadly not just because of drug resistance, but because some bacteria can survive treatment by becoming dormant – earning them the nickname “zombie cells.” These cells essentially play dead during antibiotic treatment, then reawaken once treatment stops, causing infection to return.

“Tuberculosis really is the forgotten pandemic,” says Dr. Suzie Hingley-Wilson from the University of Surrey. “It killed 1.3 million people last year, mostly from completely drug-sensitive strains. The problem isn’t always resistance—it’s persisters.”

The Surrey research team exposed over 500,000 genetically modified TB bacteria to common antibiotics – rifampicin and streptomycin. By studying which bacteria survived, they identified specific genes that help these zombie cells stay alive during treatment.

Their key discovery challenges what scientists previously believed. Rather than using the same survival tactics against all antibiotics, TB bacteria use different genetic pathways depending on which drug they face.

“What we found is that persister survival depends on the antibiotic used,” explains Dr. Hingley-Wilson. “The mechanisms aren’t shared as previously thought; they’re drug-specific.”

The researchers found these critical genes perform various roles: some strengthen the bacterial cell wall, others prevent bacterial self-destruction, and some maintain the cell’s metabolism. When these genes were disrupted, far fewer bacteria survived antibiotic treatment.

Professor Johnjoe McFadden, who led the study, believes this could transform how we treat TB. “The mechanisms involved in persistence are probably the biggest mysteries in microbiology. Their solution could revolutionize treatment.”

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Current TB treatment requires months of multiple antibiotics. Many patients struggle to complete such long treatments, which contributes to the rise of drug resistance. If new drugs could target these persistence mechanisms, treatment times could potentially be shortened dramatically.

The World Health Organization has identified antimicrobial resistance as one of the top 10 global health threats. Finding new ways to kill bacteria becomes increasingly urgent as more bacteria evolve to resist our current antibiotics.

This research represents a shift from previous approaches. While scientists have long focused on bacterial resistance – genetic mutations that allow bacteria to disable antibiotics – persisters don’t mutate. They temporarily enter a dormant state that antibiotics can’t affect.

The next research phase will focus on developing new drugs that mimic these gene functions. This could lead to treatments that specifically target and eliminate TB persister cells, potentially saving millions of lives.

For patients, this breakthrough could mean shorter treatments – possibly weeks instead of months – making TB treatment more manageable and effective. This could significantly reduce TB’s global impact and slow the spread of antimicrobial resistance.

While developing approved treatments will take time, this discovery provides a clear direction for TB drug development. By targeting the genetic weaknesses of persister cells, future treatments may finally overcome one of TB’s most effective survival strategies.

The research offers new hope for effective treatments against a disease that has plagued humanity for centuries. By understanding how to eliminate even the most stubborn TB cells, scientists are one step closer to controlling this deadly infection.

The research was published in Scientific Reports and marks a significant advance in fighting one of the world’s most dangerous infectious diseases.