Transintestinal Acetate Transport in a Herbivorous Teleost: Anion Exchange at the Basolateral Membrane

نویسنده

  • G. A. AHEARN
چکیده

Purified basolateral membrane vesicles were prepared from the intestinal epithelium of the tilapia Oreochromis mossambicus, a herbivorous teleost. Characteristics of volatile fatty acid (VFA) transport were investigated using [H]acetate as a representative anion. No significant change in [H]acetate influx was observed in the presence of a cation gradient (K or Na) compared to the influx observed in the absence of a cation gradient, indicating the lack of cationdependent coupling for acetate transport. The time course of [H]acetate uptake into vesicles preloaded with acetate or bicarbonate was enhanced compared to [H]acetate uptake into vesicles preloaded with gluconate. A series of transstimulation and cis-inhibition studies involving both organic and inorganic anions indicated the presence of a highly specific anion-exchange carrier which readily exchanged [H]acetate with the volatile fatty acids (formate, acetate, propionate and butyrate) and bicarbonate. Kinetic analysis of [H]acetate influx as a function of external acetate concentration yielded a biphasic uptake curve which was interpreted as carrier-mediated transfer (/max=21.77±2.05nmolmg~ 1 protein 10s"; /Cm=12.70±2.95mmoir ) plus apparent diffusion (P=0.17±0.02nmol mg" protein 10s" mmol" acetate). [H]Acetate uptake was also a hyperbolic function of internal bicarbonate concentration, displaying a relatively low HCO3~ half-saturation constant (X'm=0.41mmoll~ ). Intact intestinal sheets mounted in Ussing chambers demonstrated net absorptive fluxes of [H] acetate when serosal acetate concentration was maintained at l.Ommoll" and the mucosal acetate concentration was varied from 1.32 to lO.Ommoll". At mucosal acetate concentrations lower than 1.32mmoll~, a net secretion of VFAs was observed. Transepithelial transport of [H]acetate was significantly inhibited by the presence of acetazolamide. A transintestinal transport model for volatile fatty acids is proposed in which specific anion antiporters, located on the brush-border and basolateral poles of the cell, exchange luminal VFAs for serosal and intracellular bicarbonate, resulting in net transepithelial uptake of VFAs. This process is driven by a downhill lumen-to-blood VFA concentration gradient and the intracellular generation of bicarbonate by carbonic anhydrase.

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تاریخ انتشار 2005