(Journal Article): 150 mM HCO3- - How Does the Pancreas Do It? Clues from Computer Modelling of the Duct Cell
 
Sohma Y, Gray MA, Imai Y, Argent BE (Department of Physiology, Osaka Medical College. Takatsuki, Osaka, Japan. Department of Physiological Sciences, University Medical School. Newcastle upon Tyne, United Kingdom, b.e.argent@ncl.ac.uk )
 
IN: JOP. J Pancreas (Online) 2001; 02(4 Suppl.):198-202

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ABSTRACT: transmembrane conductance regulator (CFTR) is highly expressed in the pancreatic ductal epithelium and plays a key role in ductal HCO(3)(-) secretion. In humans, the pancreatic duct secretes near isotonic NaHCO(3). Experimental data suggests that HCO(3)(-) secretion occurs via apical Cl(-)/HCO(3)(-) exchangers working in parallel with Cl(-) channels (CFTR and calcium activated chloride channels, CaCC). Programming the currently available experimental data into our computer model (based on network thermodynamics) shows that while the anion exchanger/Cl(-) channel mechanism will produce a relatively large volume of a HCO(3)(-)-rich fluid, it can only raise the luminal HCO(3)(-) concentration up to about 70 mM. To achieve secretion of about 150 mM NaHCO(3) it is necessary to modulate the properties of the apical membrane transporters as the secreted fluid flows down the ductal system. On the basis of our computer simulations, we propose that HCO(3)(-) secretion occurs mainly via the exchanger in duct segments near the acini (luminal HCO(3)(-) concentration up to about 70 mM), but mainly via channels further down the ductal tree (raising luminal HCO(3)(-) to about 150 mM). We speculate that the switch between these two secretory mechanisms is controlled by a series of luminal signals (e.g. pH, HCO(3)(-) concentration) acting on the apical membrane transporters in the duct cell.

TYPE OF PUBLICATION: Round Table