Linkage of s100a10 (p11) to enteric 5-HT4-mediated serotonergic signaling roles in GI motility, enteric nervous system development, and co-morbid dysfunction of gut and brain

s100a10 (p11) 与肠道 5-HT4 介导的血清素信号在胃肠道运动、肠神经系统发育以及肠道和大脑共病功能障碍中的作用的联系

• 批准号: 10090228
• 负责人: Kara Gross Margolis
• 金额: $ 45.86万
• 依托单位: COLUMBIA UNIVERSITY HEALTH SCIENCES
• 依托单位国家: 美国
• 财政年份: 2021
• 资助国家: 美国
• 起止时间: 2021-02-01 至 2025-01-31
• 项目状态: 未结题
• 来源: https://reporter.nih.gov/project-details/10090228
• 关键词: 5-Hydroxytryptophan; Affect; Age-Months; Agonist; Anabolism; Anxiety; Biotinylation; Brain; Bypass; Cell Surface Receptors; Cell membrane; Cell surface; Clinical; Co-Immunoprecipitations; Comprehension; Constipation; Data; Defect; Development; Disease; Economic Burden; Educational workshop; Enteral; Enteric Nervous System; Environmental Exposure; Enzymes; Epithelial; Epithelial Cells; Exhibits; Failure; Functional Gastrointestinal Disorders; Functional disorder; Gastrointestinal Motility; Gastrointestinal tract structure; Genetic; Genetic Transcription; High Prevalence; Human; Immunofluorescence Immunologic; Impairment; Individual; Intestinal Mucosa; Intestines; Irritable Bowel Syndrome; Knowledge; Lead; Lesion; Life; Mediating; Membrane; Mental Depression; Molecular; Mood Disorders; Moods; Mucous Membrane; Mus; Neuraxis; Neurons; Pathogenesis; Patients; Phenotype; Play; Prevalence; Quality of life; Role; Serotonergic System; Serotonin; Serotonin Receptors 5-HT4; Signal Transduction; Signaling Molecule; Site; Suggestion; Symptoms; TPH2; Testing; Transgenic Mice; Treatment Failure; United States National Institutes of Health; Variant; affective disturbance; analog; brain dysfunction; comorbidity; cost; depression model; depressive behavior; depressive symptoms; design; effective therapy; gastrointestinal; gastrointestinal function; genetic variant; improved; in vivo; motility disorder; mouse model; nervous system development; neurogenesis; neuron development; novel; novel therapeutics; pre-clinical; receptor; serotonin receptor; suicide victim; trafficking

Project Summary Although functional gastrointestinal (GI) disorders (FGIDs) are the most common causes of bowel dysfunction worldwide, many patients are inadequately treated because current therapies are frequently ineffective. The inadequacy of therapy is largely due to an incomplete comprehension of underlying mechanisms that are critical for the design of new treatments. Up to half of individuals with FGIDs also suffer from mood disorders. Evidence supports the idea that the GI tract is vulnerable to genetic perturbations that can exert lasting effects on GI function and mood. It is thus conceivable that a co-morbid FGID and psychiatric condition result from abnormalities occurring as the result of a genetic variant. Discovery of the pathophysiology underlying FGIDs and psychiatric co-morbidities is likely to enhance understanding of their relationship and thus lead to novel therapies for both. Serotonin (5-HT), which is a major determinant of enteric and central nervous system (ENS and CNS) development and also modulates FGID-related symptoms (GI motility) as well as mood, may be an important developmental modulator of FGID pathogenesis. It is 5-HT stimulation of the 5-HT4 receptor, however, that has the most well-studied prokinetic, anti-nociceptive, anti- depressive, and anti-anxiety effects and has thus been targeted to treat both GI dysmotility and mood dysfunction. Curiously, however, >50% of patients with FGIDs are relatively unresponsive to them. The reason for 5-HT4 treatment failure is unknown, making this a critical treatment obstacle. Our preliminary data strongly suggest that failure to respond to a 5-HT4 agonist is due to a defect in 5-HT4 trafficking. Although defects in enteric 5-HT4 trafficking have never previously been explored, such abnormalities have been described in the CNS; p11 is a critical adaptor molecule involved in this transport of 5-HT4 receptors to cell surfaces, where the receptors become available to mediate 5-HT signaling. P11 also plays a role in depression (p11KO mice exhibit depressive behaviors and CNS p11 transcription is impaired in mouse models of depression and human suicide victims). We have found that in the ENS, as in the CNS, gut p11 is co- expressed with 5-HT4 receptors where they co-immunoprecipitate, suggesting that p11 interacts with 5-HT4 in the gut and, further, that p11 affects 5-HT4 receptor-mediated actions on ENS development and GI motility. Our hypotheses are thus that p11 facilitation of trafficking of 5-HT4 receptors to cell surfaces is essential for 5-HT4- modulation of ENS development and function and that p11 dysfunction thus underlies comorbid FGID and depression. In this application we will explore: (1) How critical the p11-5-HT4 interaction is for effective GI motility utilizing a comprehensive array of in vivo and ex vivo studies ± the selective 5-HT4 agonist, prucalopride, in WT and p11KO mice; (2) If effects of p11 on mood (depression / anxiety), ENS development, and GI motility depend on mucosal or enteric neuronal p11, using novel transgenic mice that selectively lack p11 in the enteric epithelium or ENS and; (3) If enteric 5-HT4 trafficking and function are p11-dependent.