Defective intestinal amino acid absorption in Ace2 null mice

Defective intestinal amino acid absorption in Ace2 null mice

Mutations in the main intestinal and kidney luminal neutral amino acid transporter B(0)AT1 (Slc6a19) lead to Hartnup disorder, a condition that is characterized by neutral aminoaciduria and in some cases pellagra-like symptoms. These latter symptoms caused by low-niacin are thought to result from de...

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Veröffentlicht in:American journal of physiology: Gastrointestinal and liver physiology 2012-09, Vol.303 (6), p.G686-G695
Hauptverfasser: Singer, Dustin, Camargo, Simone M R, Ramadan, Tamara, Schäfer, Matthias, Mariotta, Luca, Herzog, Brigitte, Huggel, Katja, Wolfer, David, Werner, Sabine, Penninger, Josef M, Verrey, François
Format: Artikel
Sprache:eng
Schlagworte:
Absorption - physiology
Amino Acid Transport Systems, Neutral - genetics
Amino Acid Transport Systems, Neutral - metabolism
Amino acids
Amino Acids - metabolism
Animal Nutritional Physiological Phenomena
Animals
Diet
Dietary Proteins - administration & dosage
Gene Expression Regulation - physiology
Genotype
Homeostasis
Intestines - metabolism
Male
Measurement
Mice
Mice, Knockout
Mutation
Niacin - metabolism
Peptidyl-Dipeptidase A - genetics
Peptidyl-Dipeptidase A - metabolism
Plasma
Proteins
Rodents
Time Factors
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Zusammenfassung:Mutations in the main intestinal and kidney luminal neutral amino acid transporter B(0)AT1 (Slc6a19) lead to Hartnup disorder, a condition that is characterized by neutral aminoaciduria and in some cases pellagra-like symptoms. These latter symptoms caused by low-niacin are thought to result from defective intestinal absorption of its precursor L-tryptophan. Since Ace2 is necessary for intestinal B(0)AT1 expression, we tested the impact of intestinal B(0)AT1 absence in ace2 null mice. Their weight gain following weaning was decreased, and Na(+)-dependent uptake of B(0)AT1 substrates measured in everted intestinal rings was defective. Additionally, high-affinity Na(+)-dependent transport of L-proline, presumably via SIT1 (Slc6a20), was absent, whereas glucose uptake via SGLT1 (Slc5a1) was not affected. Measurements of small intestine luminal amino acid content following gavage showed that more L-tryptophan than other B(0)AT1 substrates reach the ileum in wild-type mice, which is in line with its known lower apparent affinity. In ace2 null mice, the absorption defect was confirmed by a severalfold increase of L-tryptophan and of other neutral amino acids reaching the ileum lumen. Furthermore, plasma and muscle levels of glycine and L-tryptophan were significantly decreased in ace2 null mice, with other neutral amino acids displaying a similar trend. A low-protein/low-niacin diet challenge led to differential changes in plasma amino acid levels in both wild-type and ace2 null mice, but only in ace2 null mice to a stop in weight gain. Despite the combination of low-niacin with a low-protein diet, plasma niacin concentrations remained normal in ace2 null mice and no pellagra symptoms, such as photosensitive skin rash or ataxia, were observed. In summary, mice lacking Ace2-dependent intestinal amino acid transport display no total niacin deficiency nor clear pellagra symptoms, even under a low-protein and low-niacin diet, despite gross amino acid homeostasis alterations.
ISSN:0193-1857
1522-1547
DOI:10.1152/ajpgi.00140.2012