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'Living medicine' created to treat drug-resistant infections

Experimental treatment dissolves antibiotic-resistant biofilms in mice

Date:
October 6, 2021
Source:
中心Genomic Regulation
Summary:
研究人员已经创造了“生活医学”胎面t antibiotic-resistant bacteria growing on the surfaces of medical implants. The researchers created the treatment by removing a common bacteria's ability to cause disease and repurposing it to attack harmful microbes instead. The findings are an important first step for the development of new treatments for these type of infections, which account for 80% of all infections acquired in hospital settings.
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Researchers at the Centre for Genomic Regulation (CRG) and Pulmobiotics S.L have created the first 'living medicine' to treat antibiotic-resistant bacteria growing on the surfaces of medical implants. The researchers created the treatment by removing a common bacteria's ability to cause disease and repurposing it to attack harmful microbes instead.

The experimental treatment was tested on infected cathetersin vitro,ex vivoandin vivo, successfully treating infections across all three testing methods. According to the authors, injecting the therapy under the skin of mice treated infections in 82% of the treated animals.

The findings are an important first step for the development of new treatments for infections affecting medical implants such as catheters, pacemakers and prosthetic joints. These are highly resistant to antibiotics and account for 80% of all infections acquired in hospital settings.

The study is published today in the journalMolecular Systems Biology. This work has been supported by the "la Caixa" Foundation through the CaixaResearch Health call, the European Research Council (ERC), the MycoSynVac project under the EU's Horizon 2020 research and innovation programme, the Generalitat de Catalunya and the Instituto de Salud Carlos III.

The new treatment specifically targets biofilms, colonies of bacterial cells that stick together on a surface. The surfaces of medical implants are ideal growing conditions for biofilms, where they form impenetrable structures that prevent antibiotics or the human immune system from destroying the bacteria embedded within. Biofilm-associated bacteria can be a thousand times more resistant to antibiotics than free-floating bacteria.

Staphylococcus aureusis one of the most common species of biofilm-associated bacteria.S. aureusinfections do not respond to conventional antibiotics, requiring patients to surgically remove any infected medical implants. Alternative therapies include the use of antibodies or enzymes, but these are broad-spectrum treatments that are highly toxic for normal tissues and cells, causing undesired side effects.

The authors of the study hypothesised that introducing living organisms that directly produce enzymes in the local vicinity of biofilms is a safer and cheaper way of treating infections. Bacteria are an ideal vector, as they have small genomes that can be modified using simple genetic manipulation.

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The researchers chose to engineerMycoplasma pneumoniae, a common species of bacteria that lacks a cell wall, making it easier to release the therapeutic molecules that fight infection while also assisting it in evading detection from the human immune system. Other advantages of usingM. pneumoniaeas a vector include its low risk of mutating new abilities, and its inability to transfer any of its modified genes to other microbes living nearby.

M. pneumoniaewas first modified so that it would not cause illness. Further tweaks made it produce two different enzymes that dissolve biofilms and attacks the cell walls of the bacteria embedded within. The researchers also modified the bacteria so that it secretes antimicrobial enzymes more efficiently.

The researchers first aim to use the modified bacteria to treat biofilms building around breathing tubes, asM. pneumoniaeis naturally adapted to the lung. "Our technology, based on synthetic biology and live biotherapeutics, has been designed to meet all safety and efficacy standards for application in the lung, with respiratory diseases being one of the first targets. Our next challenge is to address high-scale production and manufacturing, and we expect to start clinical trials in 2023," says María Lluch, co-corresponding author of the study and Chief Science Officer of Pulmobiotics.

The modified bacteria may also have long-term applications for other diseases. "Bacteria are ideal vehicles for 'living medicine' because they can carry any given therapeutic protein to treat the source of a disease. One of the great benefits of the technology is that once they reach their destination, bacterial vectors offer continuous and localised production of the therapeutic molecule. Like any vehicle, our bacteria can be modified with different payloads that target different diseases, with potentially more applications in the future," says ICREA Research Professor Luis Serrano, Director of the CRG and co-author of the study.

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Materialsprovided by中心Genomic Regulation.注意:内容可能被编辑风格d length.


Journal Reference:

  1. Victoria Garrido, Carlos Piñero-Lambea, Irene Rodriguez-Arce, Bernhard Paetzold, Tony Ferrar, Marc Weber, Eva Garcia-Ramallo, Carolina Gallo, María Collantes, Iván Peñuelas, Luis Serrano, María-Jesús Grilló, María Lluch-Senar.Engineering a genome-reduced bacterium to eliminate Staphylococcus aureus biofilms in vivo.Molecular Systems Biology, 2021 DOI:10.15252/msb.202010145

Cite This Page:

中心Genomic Regulation. "'Living medicine' created to treat drug-resistant infections: Experimental treatment dissolves antibiotic-resistant biofilms in mice." ScienceDaily. ScienceDaily, 6 October 2021. /releases/2021/10/211006095502.htm>.
中心Genomic Regulation. (2021, October 6). 'Living medicine' created to treat drug-resistant infections: Experimental treatment dissolves antibiotic-resistant biofilms in mice.ScienceDaily. Retrieved September 6, 2023 from www.koonmotors.com/releases/2021/10/211006095502.htm
中心Genomic Regulation. "'Living medicine' created to treat drug-resistant infections: Experimental treatment dissolves antibiotic-resistant biofilms in mice." ScienceDaily. www.koonmotors.com/releases/2021/10/211006095502.htm (accessed September 6, 2023).

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