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Researchers discover that anti-malaria drugs can fight pulmonary disease

Date:
March 21, 2022
Source:
Colorado State University
Summary:
A research team has discovered that drugs used to treat malaria are also effective at treating a pulmonary disease similar to tuberculosis.
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A research team at Colorado State University has discovered that drugs used to treat malaria are also effective at treating a pulmonary disease similar to tuberculosis.

Their findings were featured on the cover of the Feb. 23 issue ofScience Translational Medicine.

The study is a significant development in the fight against infections caused by non-tuberculous mycobacteria, or NTM, which are now more common than tuberculosis in the United States and often attack people who have a weakened immune system or preexisting conditions like chronic obstructive pulmonary disease or cystic fibrosis.

“目前抗生素availabl很少e to treat NTM infections, and some patients fail to respond to any treatment," said Professor Mary Jackson of CSU's Department of Microbiology, Immunology and Pathology, one of the lead authors. "The perspective that antimalarial drugs that already have undergone advanced clinical trials may become part of the arsenal of drugs available to fight these infections could have an immediate impact in the clinic."

The research, which was led by Jackson and lead author Juan Manuel Belardinelli, a research scientist in CSU's Department of Microbiology, Immunology and Pathology, targeted an NTM known asMycobacterium abscessus. Few drugs are effective against this mycobacterium, and the ones that are tend to be toxic and cause bad side effects, Jackson said.

Targeting disease's defense mechanism

Jackson and Belardinelli worked with other members of CSU's Mycobacteria Research Laboratories to target one of the key defense mechanisms that this mycobacterium deploys to fight off our immune system and antibiotics.

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The researchers believe that the bacterium is capable of sensing and responding to threats in its environment, such as lowered oxygen levels, oxidative stress and acidic pH, which are our body's natural ways of fighting disease. It does so by activating, among other things, a regulator known as DosRS which controls many essential functions in the bacterium such as its respiration, ability to form biofilms and ability to enter a dormant state when the conditions are not favorable to bacterial multiplication.

They found that in mice, two existing antimalarial drugs were able to prevent DosRS from responding to stresses, meaning that the bacterium struggled to fight off antibiotics and the immune system's natural disease response.

"It blocked the regulator and kept it from doing its job," Jackson explained. "One of the things the treatment did, in particular, was to lower the bacterium's ability to form biofilms, thereby reducing its ability to resist killing by antibiotics."

The treatment alone was just as effective at dropping bacterial loads in the lungs as the combination of antibiotics currently used to treat the disease.

The lead authors are now working with doctors at National Jewish Health to administer the drug that proved most effective -- OZ439 -- to humans, particularly those with cystic fibrosis.

"Treatment ofM. abscessusis especially challenging because a minimum of three to four antibiotics are needed in combination, and there are few available options," said Dr. Jerry Nick, a pulmonologist at National Jewish Health. "The repurposing of antibiotics developed for other infections for use in the treatment ofM. abscessushas proven to be the most successful route to increasing available therapies for this serious disease. This report is especially exciting because these compounds were both effective against the infection and also increased the effectiveness of other antibiotics. The repurposing strategy reduces the time needed to test these compounds in clinical trials, as often there is a proven track record of safety and clinical experience."

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Materialsprovided byColorado State University.注意:内容可能被编辑风格d length.


Journal Reference:

  1. Juan Manuel Belardinelli, Deepshikha Verma, Wei Li, Charlotte Avanzi, Crystal J. Wiersma, John T. Williams, Benjamin K. Johnson, Matthew Zimmerman, Nicholas Whittel, Bhanupriya Angala, Han Wang, Victoria Jones, Véronique Dartois, Vinicius C. N. de Moura, Mercedes Gonzalez-Juarrero, Camron Pearce, Alan R. Schenkel, Kenneth C. Malcolm, Jerry A. Nick, Susan A. Charman, Timothy N. C. Wells, Brendan K. Podell, Jonathan L. Vennerstrom, Diane J. Ordway, Robert B. Abramovitch, Mary Jackson.Therapeutic efficacy of antimalarial drugs targeting DosRS signaling in Mycobacterium abscessus.Science Translational Medicine, 2022; 14 (633) DOI:10.1126/scitranslmed.abj3860

Cite This Page:

科罗拉多州立大学。“研究人员发现that anti-malaria drugs can fight pulmonary disease." ScienceDaily. ScienceDaily, 21 March 2022. /releases/2022/03/220321162717.htm>.
科罗拉多州立大学。(2022, March 21). Researchers discover that anti-malaria drugs can fight pulmonary disease.ScienceDaily. Retrieved September 6, 2023 from www.koonmotors.com/releases/2022/03/220321162717.htm
科罗拉多州立大学。“研究人员发现that anti-malaria drugs can fight pulmonary disease." ScienceDaily. www.koonmotors.com/releases/2022/03/220321162717.htm (accessed September 6, 2023).

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