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Dar bacterial product could trigger Parkinson’s-like brain damage

Gut Bacteria​ link to Parkinson’s Disease‍ Uncovered, Offering New treatment Pathways

SEOUL/LONDON⁢ – A groundbreaking new study⁣ has established a compelling link between a common ⁢gut bacterium and the advancement of ​parkinson’s-like brain damage.Researchers have identified imidazol propionate, a‌ substance⁣ produced by ‍ Streptococcus mutans, as a potential driver of the⁢ degeneration of dopamine-producing neurons – a hallmark of Parkinson’s disease. This discovery, published today in Nature Communications, could revolutionize our understanding and treatment of ⁤this debilitating ⁣neurological condition.

For⁢ years, scientists have observed a correlation between the gut microbiome – the vast community of ‌microorganisms residing in our digestive tract – and Parkinson’s ‍disease.⁣ However, pinpointing how specific ⁣gut bacteria might influence brain health ⁢has remained ‌a notable challenge. This new research provides‍ a crucial piece of the⁤ puzzle, identifying a direct chemical ​pathway connecting gut ‍microbial activity to neurodegeneration.

The international research team,led by Yunjong Lee of Sungkyunkwan University School of Medicine‍ and Ara Koh of the ⁤Pohang University of Science and Technology in South Korea,along with collaborators from China and Sweden,analyzed genetic data from 491 Parkinson’s patients and 234 healthy individuals. ⁣Their analysis revealed significantly higher levels of Streptococcus mutans in the‍ gut of those with Parkinson’s, alongside a more prevalent gene responsible for producing imidazol propionate – an‌ enzyme ⁢called Urocantreductase.

To establish a causal relationship, the ​team conducted experiments using germ-free mice,‍ raised⁤ in sterile environments. Colonizing these mice​ with live​ Streptococcus mutans ⁢resulted ‍in a‌ substantial loss of​ dopamine neurons in the midbrain,accompanied by brain inflammation and noticeable motor impairments,as measured by a pole ⁣climbing test. Importantly,mice colonized with heat-killed,inactive bacteria did not ⁤exhibit these ‌symptoms.

Further experiments confirmed that imidazol propionate, produced by the bacteria in the gut, ⁣can⁤ indeed cross the blood-brain barrier and⁤ accumulate in brain tissue.⁣ Researchers‌ then engineered a harmless strain of bacteria to produce the Urocantreductase enzyme,⁤ effectively creating a factory ⁢for imidazol ‌propionate. When introduced ⁣to germ-free mice, this modified bacteria triggered the same​ Parkinson’s-like symptoms observed with Streptococcus mutans colonization.

Delving into‍ the molecular mechanisms, the team discovered that imidazol propionate⁤ activates ‌the MTORC1 ​signaling⁤ pathway in brain cells. ​This pathway is⁣ known to play a role in cell growth,aging,and neurodegeneration. Activation of⁢ MTORC1 ⁣was specifically observed in dopamine-producing neurons in the brains of mice colonized with Streptococcus mutans.

treating mice with ⁣rapamycin, a drug known ‍to inhibit MTORC1, mitigated ⁣the⁢ damaging effects of the bacterial colonization,⁣ further solidifying the link between imidazol propionate, MTORC1 activation, and neurodegeneration.

“This ⁤research provides compelling evidence that a specific metabolite produced by a‍ common gut bacterium‌ can directly contribute to the development of‌ Parkinson’s-like symptoms,”​ explains Dr. lee. “It opens up ‍exciting new‌ avenues for ⁢potential ⁢therapeutic interventions, focusing on modulating the gut microbiome or directly‍ targeting the MTORC1 pathway.”

While further research is needed ‍to‌ fully understand the complex interplay ‍between the gut microbiome and Parkinson’s disease, this study represents⁣ a significant step forward in the fight​ against this⁢ devastating​ condition. The findings suggest that⁤ future treatments may involve dietary interventions, probiotics, or even targeted therapies designed to reduce the production of imidazol propionate ‍in the gut.

keywords: Parkinson’s Disease, Gut Microbiome, Streptococcus ​mutans,‌ Imidazol ​propionate, Neurodegeneration,⁤ Dopamine Neurons, MTORC1, ‍Brain Health, Neurological Disease, Research, Nature Communications.

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