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Am J Physiol Regul Integr Comp Physiol (November 12, 2008). doi:10.1152/ajpregu.90632.2008
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Submitted on July 27, 2008
Revised on November 3, 2008
Accepted on November 6, 2008

Central cholinergic mechanisms mediated swallowing, renal excretion, and c-fos expression in the ovine fetus near term

Lijun Shi1, Caiping Mao2, Fanxing Zeng1, Liyan Zhu2, and Zhice Xu3*

1 Department of Human Sport Science
2 Perinatal Research Laboratory
3 Center for Perinatal Biology

* To whom correspondence should be addressed. E-mail: zxu{at}llu.edu.

Fetal swallowing and renal metabolism contribute importantly to amniotic and body fluid homeostasis. To determine central cholinergic modulation of swallowing activity and renal excretion associated with neural activity we examined the effects of intracerebroventricular (i.c.v.) injection of carbachol, a cholinergic agonist, in ovine fetuses at 0.9 gestation. Fetuses were chronically prepared with thyrohyoid, nuchal and thoracic esophagus, and diaphragm electromyogram electrodes, lateral ventricle and vascular catheters. Electrodes were also implanted on the parietal dura for determination of fetal electrocorticogram (ECoG). After 5 days of recovery, fetal swallowing, ECoG, and urine output were monitored during basal period and the experimental period following i.c.v. injection of 0.9% NaCl as the control (n=5) or carbachol (3µg/kg, n=5). Central carbachol did not significantly change fetal low voltage (LV) and high voltage (HV) ECoG temporal distributions. However, swallowing activity during LV ECoG was elevated significantly after i.c.v. carbachol. Associated with the swallowing activation, FOS immunoreactivity in the putative dipsogenic center, subfornical organ, was enhanced significantly. The fetal urine flow rate and renal Na+, K+, and Cl- excretion were markedly increased following i.c.v. carbachol, and sustained at the high level for at least 2 hours. The results indicate that the central cholinergic mechanism is established and functional in regulation of fetal behavior and renal excretion at least at 0.9 gestation, which plays an important role in maintenance of fetal body fluid homeostasis.







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