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• W2955540332 abstract "The gut-brain axis is of crucial importance for controlling glucose homeostasis. Alteration of this axis promotes the type 2 diabetes (T2D) phenotype (hyperglycaemia, insulin resistance). Recently, a new concept has emerged to demonstrate the crucial role of the enteric nervous system in the control of glycaemia via the hypothalamus. In diabetic patients and mice, modification of enteric neurons activity in the proximal part of the intestine generates a duodenal hyper-contractility that generates an aberrant message from the gut to the brain. In turn, the hypothalamus sends an aberrant efferent message that provokes a state of insulin resistance, which is characteristic of a T2D state. Targeting the enteric nervous system of the duodenum is now recognized as an innovative strategy for treatment of diabetes. By acting in the intestine, bioactive gut molecules that we called “enterosynes” can modulate the function of a specific type of neurons of the enteric nervous system to decrease the contraction of intestinal smooth muscle cells. Here, we focus on the origins of enterosynes (hormones, neurotransmitters, nutrients, microbiota, and immune factors), which could be considered therapeutic factors, and we describe their modes of action on enteric neurons. This unsuspected action of enterosynes is proposed for the treatment of T2D, but it could be applied for other therapeutic solutions that implicate communication between the gut and brain." @default.
• W2955540332 created "2019-07-12" @default.
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• W2955540332 date "2019-07-02" @default.
• W2955540332 modified "2023-10-14" @default.
• W2955540332 title "Targeting the Enteric Nervous System to Treat Metabolic Disorders? “Enterosynes” as Therapeutic Gut Factors" @default.
• W2955540332 cites W1518824992 @default.
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• W2955540332 cites W1612135120 @default.
• W2955540332 cites W1793035576 @default.
• W2955540332 cites W1963557346 @default.
• W2955540332 cites W1973706539 @default.
• W2955540332 cites W1974890544 @default.
• W2955540332 cites W1981367331 @default.
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• W2955540332 cites W1987771620 @default.
• W2955540332 cites W1988783094 @default.
• W2955540332 cites W1994305667 @default.
• W2955540332 cites W1997203862 @default.
• W2955540332 cites W1998714747 @default.
• W2955540332 cites W2001857679 @default.
• W2955540332 cites W2002297978 @default.
• W2955540332 cites W2009815277 @default.
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• W2955540332 cites W2031541332 @default.
• W2955540332 cites W2032030580 @default.
• W2955540332 cites W2032123628 @default.
• W2955540332 cites W2034475269 @default.
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• W2955540332 doi "https://doi.org/10.1159/000500602" @default.
• W2955540332 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/31280267" @default.
• W2955540332 hasPublicationYear "2019" @default.
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