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Serotonin released from intestinal enterochromaffin cells mediates luminal non-cholecystokinin-stimulated pancreatic secretion in rats

被引:139
作者
Li, Y [1 ]
Hao, YB [1 ]
Zhu, JX [1 ]
Owyang, C [1 ]
机构
[1] Univ Michigan Hlth Syst, Dept Internal Med, Gastroenterol Res Unit, Ann Arbor, MI 48109 USA
来源
GASTROENTEROLOGY | 2000年 / 118卷 / 06期
关键词
D O I
10.1016/S0016-5085(00)70373-8
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
Background & Aims: Similar to cholecystokinin (CCK), non-CCK-dependent duodenal factors stimulate vagal mucosal afferent fibers to mediate pancreatic enzyme secretion via a common cholinergic pathway. We tested the hypothesis that Ei-hydroxytryptamine (5-HT) released from enterochromaffin (EC) cells plays an important role in the transduction of luminal information to the central nervous system via vagal afferent fibers to mediate pancreatic secretion. Methods: Pancreatic secretions were examined in conscious rats after intragastric administration of chopped rodent chow in the presence and absence of CCK or 5-HT3 and 5-HT2 antagonists. Pancreatic responses to intraduodenal administration of maltose, hyperosmolar NaCl, and light mucosal stroking were examined in rats pretreated with various pharmacological antagonists or after surgical or chemical ablation of vagal and 5-HT neural pathways. Results: Administration of L364,718 inhibited 54% of pancreatic protein secretion evoked by intragastric administration of rodent chow. L364,714 and ICS 205-930, a 5-HT3 antagonist, combined produced a 94% inhibition. Vagal afferent rootlet section eliminated pancreatic secretions evoked by intraduodenal stimuli, p-Chlorophenylalanine, a 5-HT synthesis inhibitor, but not 5,7-hydroxytryptamine, a 5-HT neurotoxin, also eliminated the pancreatic response to these luminal stimuli. The 5-HT3 antagonist markedly inhibited pancreatic secretion induced by maltose and hyperosmolar NaCl. 5-HT2 and 5-HT3 antagonists combined inhibited the pancreatic response to light stroking of the mucosa. Conclusions: Luminal factors such as osmolality, disaccharides, and mechanical stimulation stimulated pancreatic secretion via intestinal vagal mucosal afferent fibers. It is likely that 5-HT originating from intestinal EC cells activated 5-HT3 and 5-HT2 receptors on vagal afferent fibers to mediate luminal factor-stimulated pancreatic secretion.
引用
收藏
页码:1197 / 1207
页数:11
相关论文
共 65 条
[1]   INTERACTION OF THE CHOLINERGIC SYSTEM AND CHOLECYSTOKININ IN THE REGULATION OF ENDOGENOUS AND EXOGENOUS STIMULATION OF PANCREATIC-SECRETION IN HUMANS [J].
ADLER, G ;
BEGLINGER, C ;
BRAUN, U ;
REINSHAGEN, M ;
KOOP, I ;
SCHAFMAYER, A ;
ROVATI, L ;
ARNOLD, R .
GASTROENTEROLOGY, 1991, 100 (02) :537-543
[2]  
ALVAREZ EO, 1986, PHYSIOL BEHAV, V64, P340
[3]   THE ABDOMINAL VISCERAL INNERVATION AND THE EMETIC REFLEX - PATHWAYS, PHARMACOLOGY, AND PLASTICITY [J].
ANDREWS, PLR ;
DAVIS, CJ ;
BINGHAM, S ;
DAVIDSON, HIM ;
HAWTHORN, J ;
MASKELL, L .
CANADIAN JOURNAL OF PHYSIOLOGY AND PHARMACOLOGY, 1990, 68 (02) :325-345
[4]   DIHYDROXYTRYPTAMINES AS TOOLS TO STUDY THE NEUROBIOLOGY OF SEROTONIN [J].
BAUMGARTEN, HG ;
KLEMM, HP ;
SIEVERS, J ;
SCHLOSSBERGER, HG .
BRAIN RESEARCH BULLETIN, 1982, 9 (1-6) :131-150
[5]  
BJORKLUND A, 1975, J NEUROCHEM, V24, P833
[6]   EFFECTS OF 5-HYDROXYTRYPTAMINE ON DISCHARGE OF VAGAL MUCOSAL AFFERENT-FIBERS FROM THE UPPER GASTROINTESTINAL-TRACT OF THE FERRET [J].
BLACKSHAW, LA ;
GRUNDY, D .
JOURNAL OF THE AUTONOMIC NERVOUS SYSTEM, 1993, 45 (01) :41-50
[7]  
BRADFORD MM, 1976, ANAL BIOCHEM, V72, P248, DOI 10.1016/0003-2697(76)90527-3
[8]  
BULBRING E, 1959, J PHYSIOL-LONDON, V146, P18
[9]   PHYLOGENETIC STUDY OF SEROTONIN-IMMUNOREACTIVE STRUCTURES IN THE PANCREAS OF VARIOUS VERTEBRATES [J].
DING, WG ;
FUJIMURA, M ;
TOOYAMA, I ;
KIMURA, H .
CELL AND TISSUE RESEARCH, 1991, 263 (02) :237-243
[10]   P-CHLOROPHENYLALANINE-INDUCED SEROTONIN DEPLETION - REDUCTION IN EXPLORATORY LOCOMOTION BUT NO OBVIOUS SENSORY-MOTOR DEFICITS [J].
DRINGENBERG, HC ;
HARGREAVES, EL ;
BAKER, GB ;
COOLEY, RK ;
VANDERWOLF, CH .
BEHAVIOURAL BRAIN RESEARCH, 1995, 68 (02) :229-237
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