A large numbers of endocrine cells are dispersed among the epithelial BYL719 cells of gut mucosa and react to changes in gut contents by releasing hormones that are, in general, targeted to other parts of the digestive system [1]. There are at least 14 different populations of enteric endocrine cells scattered throughout GI epithelia [2]. Enteric endocrine cells release various biologically active compounds such as gastrin, secretin, stomatostatin, cholecystokinin, chromogranins (Cgs) and serotonin (5-hydroxytryptamine: 5-HT) [3–5]. The hormones released from the enteric endocrine cells are important enteric mucosal signalling
molecules influencing gut physiology (motor and secretory function). Alteration of endocrine cell function, particularly in the context of 5-HT, has been shown to be associated in a number of GI diseases including inflammatory bowel disease (IBD), coeliac
disease, enteric infections, colon carcinoma and functional Selleck Alectinib disorders such as irritable bowel syndrome (IBS) [6–14]. The association between alteration in the production of gut hormones from enteric endocrine cells and various GI diseases emphasizes highly the significance of these hormones in intestinal homeostasis. Due to the strategic location of enteric endocrine cells in gut mucosa, interaction between immune and endocrine systems is very likely to play an important role in immune activation in relation to gut pathology and pathophysiology in various GI disorders, including IBD. This paper reviews information on the role of two major hormones of the GI tract, namely 5-HT and Cgs, in immune activation in the context of gut inflammation and highlights its implications in understanding the pathology and pathophysiology of inflammatory disorders of the gut. Enterochromaffin (EC) cells are the best-characterized GI endocrine cells, which are dispersed throughout the GI mucosa and are the main source of biogenic amine 5-HT in gut [5,15]. EC cells have specialized microvilli that project into the lumen, and contain enzymes and transporters
known to be present in the apical parts of the enterocytes [16]. EC cells function as sensors for the gut Selleckchem Decitabine contents and respond to luminal stimuli directly via these transporters and/or indirectly by mediators from the surrounding cells [16]. The GI tract contains about 95% of the body’s 5-HT, and EC cells are its main source [15,17]. 5-HT is also found in enteric neurones, but the 5-HT amount present in enteric neurones appears very small in comparison to that present in EC cells (approximately 90% of 5-HT in EC cells and 10% in enteric neurones) [17]. EC cells release 5-HT in a regulated and calcium-dependent manner in response to various mechanical and chemical stimuli, including bacterial toxins [3–5]. EC cells synthesize 5-HT from its precursor l-tryptophan. Tryptophan hydroxylase (TPH) catalyzes the rate-limiting step in the synthesis of 5-HT from tryptophan and has been detected prominently in EC cells [18].