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Good gut bacteria may help reduce risk for heart disease
COLUMBUS, Ohio - Scientists have discovered that one of the good gut bacteria has a benefit that has the potential to reduce the risk for heart disease.
The bacteria's activity in the intestines reduces production of a chemical that has been linked to the development of clogged arteries. After it's manufactured in the gut, the chemical enters the bloodstream and travels to the liver, where it is converted into its most harmful form.
The Ohio State University researchers have traced the bacteria's behavior to a family of proteins that they suspect could explain other ways that good gut organisms can contribute to human health. In essence, these microbes compete with bad bacteria for access to the same nutrients in the gut - and if the good bacteria win, they may prevent health problems that can result from how the body metabolizes food.
Much more work is ahead, but the scientists see potential for this microbe, Eubacterium limosum, to be used for therapeutic purposes in the future. Previous research has already shown the bacterium is "good" because it calms inflammation in the gut.
"Over the last decade, it has become apparent that bacteria in the human gut influence our health in many ways. The organism we studied affects health by preventing a problematic compound from becoming a worse one," said Joseph Krzycki, professor of microbiology at Ohio State and senior author of the study. "It's too soon to say whether this bacterium could have therapeutic value. But that's what we're working toward."
The research appears online and will be published in a future edition of the Journal of Biological Chemistry.
The chemical linked to the clogged arteries that characterize atherosclerosis is called trimethylamine, or TMA. It is produced during metabolism when some intestinal microbes - generally the bacteria considered unhelpful to humans - interact with certain nutrients from food. Among those nutrients is L-carnitine, a chemical compound found in meat and fish that is also used as a nutritional supplement to improve recovery after exercise.
Krzycki and his colleagues discovered that E. limosum interacts with L-carnitine in a different way in the gut, and that interaction eliminates L-carnitine's role in production of TMA (other nutrients also participate in TMA production in the gut).
The researchers attribute the bacteria's beneficial behavior to a protein called MtcB, an enzyme that cuts specific molecules off of compounds to help bacteria generate energy and survive. The process is called demethylation, and involves the removal of one methyl group - a carbon atom surrounded by three hydrogen atoms - to change a compound's structure or function.
"The bacterium does this for its own benefit, but it has the downstream effect of reducing the toxicity of TMA," Krzycki said. "Up until now, the only known gut microbial reactions with L-carnitine involved converting it into its bad form. We've discovered that a bacterium known to be beneficial could remove a methyl group and send the resulting product down another pathway without making any other harmful compounds in the process."
In these interactions, L-carnitine functions as a growth substrate - a compound consumed so the organism can live and grow, and also a target for enzyme activity. In the study, the researchers fed E. limosum cultures an assortment of potential substrates, including L-carnitine. Only when offered L-carnitine did the microbe synthesize the MtcB protein specifically to lop off L-carnitine's methyl group - in essence, MtcB is part of the bacteria's natural way to consume the nutrient.
Krzycki said finding this one significant health benefit in one species of gut bacteria suggests there is still a lot to learn about how gut bacteria can influence health outcomes associated with human metabolism.
"MtcB is part of a family of proteins with thousands of representatives that may use different compounds and change what nutrients bacteria consume in the gut," he said. "These proteins may behave very similarly chemically, but using different compounds obviously can create big changes as far as biology goes."
For more details click on the link: http://dx.doi.org/10.1074/jbc.RA120.012934
Hina Zahid Joined Medical Dialogue in 2017 with a passion to work as a Reporter. She coordinates with various national and international journals and association and covers all the stories related to Medical guidelines, Medical Journals, rare medical surgeries as well as all the updates in the medical field. Email:Â editorial@medicaldialogues.in. Contact no. 011-43720751
Dr Kamal Kant Kohli-MBBS, DTCD- a chest specialist with more than 30 years of practice and a flair for writing clinical articles, Dr Kamal Kant Kohli joined Medical Dialogues as a Chief Editor of Medical News. Besides writing articles, as an editor, he proofreads and verifies all the medical content published on Medical Dialogues including those coming from journals, studies,medical conferences,guidelines etc. Email: drkohli@medicaldialogues.in. Contact no. 011-43720751