Enteropathogenic Escherichia coli inhibits intestinal vitamin B1 (thiamin) uptake: studies with human-derived intestinal epithelial Caco-2 cells

doi:10.1152/ajpgi.00250.2009

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Am J Physiol Gastrointest Liver Physiol 297: G825-G833, 2009. First published July 23, 2009; doi:10.1152/ajpgi.00250.2009
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MUCOSAL BIOLOGY

Enteropathogenic Escherichia coli inhibits intestinal vitamin B1 (thiamin) uptake: studies with human-derived intestinal epithelial Caco-2 cells

Balasubramaniem Ashokkumar,¹^,2 Jeyan S. Kumar,² Gail A. Hecht,³ and Hamid M. Said¹^,2

¹Department of Medical Research, Veterans Administration Medical Center, Long Beach, California; ²Departments of Medicine and Physiology/Biophysics, University of California, Irvine, California; and ³Section of Digestive Diseases and Nutrition, Department of Medicine, University of Illinois, Chicago, Illinois

Submitted June 29, 2009 ; accepted in final form July 20, 2009

Infection with the gram-negative enteropathogenic Escherichiacoli (EPEC), a food-borne pathogen, represents a significantrisk to human health. Whereas diarrhea is a major consequenceof this infection, malnutrition also occurs especially in severeand prolonged cases, which may aggravate the health status ofthe infected hosts. Here we examined the effect of EPEC infectionon the intestinal uptake of the water-soluble vitamin B1 (thiamin)using an established human intestinal epithelial Caco-2 cellmodel. The results showed that infecting Caco-2 cells with wild-typeEPEC (but not with nonpathogenic E. coli, killed EPEC, or filteredsupernatant) leads to a significant (P < 0.01) inhibitionin thiamin uptake. Kinetic parameters of both the nanomolar(mediated by THTR-2) and the micromolar (mediated by THTR-1)saturable thiamin uptake processes were affected by EPEC infection.Cell surface expression of hTHTR-1 and -2 proteins, (determinedby the biotinylation method) showed a significantly (P <0.01) lower expression in EPEC-treated cells compared with controls.EPEC infection also affected the steady-state mRNA levels aswell as promoter activity of the SLC19A2 and SLC19A3 genes.Infecting Caco-2 cells with EPEC mutants that harbor mutationsin the escN gene (which encodes a putative ATPase for the EPECtype III secretion system, TTSS) or the espA, espB, or espDgenes (which encode structural components of the TTSS) did notaffect thiamin uptake. On the other hand, mutations in espFand espH genes (which encode effector proteins) exhibited partialinhibition in thiamin uptake. These results demonstrate forthe first time that EPEC infection of human intestinal epithelialcells leads to inhibition in thiamin uptake via effects on physiologicaland molecular parameters of hTHTR-1 and -2. Furthermore, theinhibition appears to be dependent on a functional TTSS of EPEC.

thiamin transport; hTHTR-1; hTHTR-2

Address for reprint requests and other correspondence: H. M. Said, UCI/VA Medical Program, VA Medical Center-151, Long Beach, CA 90822 (e-mail: hmsaid{at}uci.edu).