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How immunotherapy may be effective for fighting tuberculosis

Date:
March 14, 2019
Source:
University of Notre Dame
Summary:
New research suggests that structures released by infected cells in tuberculosis may be used in tandem with antibiotics to boost the body's immune system, helping fight off the disease.
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FULL STORY

In part because of its resistance to many antibiotics, tuberculosis kills approximately 1.7 million people worldwide each year. But new research from the University of Notre Dame suggests that structures released by the infected cells may be used in tandem with antibiotics to boost the body's immune system, helping fight off the disease.

The paper, published inEMBO Reportsby Jeffrey Schorey, the George B. Craig Jr. Professor, and Yong Cheng, research assistant professor, both in the Department of Biological Sciences, describes how the structures, called extracellular vesicles (EVs), containMycobacterium tuberculosisRNA and transfer it to other cells. This starts a built-in weapon system against the disease in the form of an immune response.

Though extracellular vesicles containing RNA from viruses had been discovered years ago, Schorey and his collaborators recently discovered RNA from bacteria --Mycobacterium tuberculosis-- in EVs. This discovery led to experiments described in theEMBO Reportspaper to determine how the bacteria's RNA was affecting the "target" cell, including cells infected byM. tuberculosis.

A key research discovery hinges on macrophages, which are cells of the immune system. These cells, when treated with EVs released from M. tuberculosis-infected cells, can control the infection better than macrophages not previously exposed to the EVs, Schorey and Cheng determined. "It had never before been shown that bacterial RNA in EVs can activate this sensing pathway, one that has primarily been thought to be involved in viral sensing," Schorey said. The authors then show that EV-treated macrophages produce compounds like reactive oxygen species that can promote the killing of theM. tuberculosisonce it infects the macrophage.

The discovery is important because it can lead to future therapies for treatment of tuberculosis. Preliminary data in the paper suggest that antibiotics might work better when combined with an immunotherapy based on using these EVs. The data from the mouse model showed that more of the bacterial-infected cells were killed with the combination of therapies than either antibiotics or EVs alone, Schorey noted.

The next steps for future research are to try this approach with other laboratory models, with the goal that they also show the benefit of combining EVs, as immunotherapy treatments, with antibiotics to treat drug-resistant tuberculosis.

Worldwide, more than 10 million people develop active tuberculosis each year. Furthermore, over two billion people are infected with the bacteria. This results in a reservoir of infected people who may develop disease if their immune systems are compromised.

Schorey is affiliated with Advanced Diagnostics and Therapeutics, the Eck Institute for Global Health and the Center for Rare and Neglected Diseases at Notre Dame. The research was funded by the National Institute of Allergy and Infectious Diseases.

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Story Source:

Materialsprovided byUniversity of Notre Dame. Original written by Deanna Csomo McCool.注意:内容可能被编辑风格d length.


Journal Reference:

  1. Yong Cheng, Jeffery S Schorey.Extracellular vesicles deliver Mycobacterium RNA to promote host immunity and bacterial killing.EMBO reports, 2019; 20 (3): e46613 DOI:10.15252/embr.201846613

Cite This Page:

University of Notre Dame. "How immunotherapy may be effective for fighting tuberculosis." ScienceDaily. ScienceDaily, 14 March 2019. /releases/2019/03/190314123119.htm>.
University of Notre Dame. (2019, March 14). How immunotherapy may be effective for fighting tuberculosis.ScienceDaily. Retrieved October 18, 2023 from www.koonmotors.com/releases/2019/03/190314123119.htm
University of Notre Dame. "How immunotherapy may be effective for fighting tuberculosis." ScienceDaily. www.koonmotors.com/releases/2019/03/190314123119.htm (accessed October 18, 2023).

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