Differential cystine and dibasic amino acid handling after loss of function of the amino acid transporter b0,+AT (Slc7a9) in mice.

[cystinuria]

Cystinuria is an autosomal recessive disease caused by mutations in SLC 3 A 1 (rBAT ) and SLC 7 A 9 (b (0 ,+)AT ). Gene targeting of the catalytic subunit (Slc 7 a 9 ) in mice leads to excessive excretion of cystine , lysine , arginine , and ornithine . Here , we studied this non-type I cystinuria mouse model using gene expression analysis , Western blotting , clearance , and brush-border membrane vesicle (BBMV ) uptake experiments to further characterize the renal and intestinal consequences of losing Slc 7 a 9 function . The electrogenic and BBMV flux studies in the intestine suggested that arginine and ornithine are transported via other routes apart from system b (0 ,+). No remarkable gene expression changes were observed in other amino acid transporters and the peptide transporters in the intestine and kidney . Furthermore , the glomerular filtration rate (GFR ) was reduced by 30 % in knockout animals compared with wild-type animals . The fractional excretion of arginine was increased as expected (∼100 %), but fractional excretions of lysine (∼35 %), ornithine (∼16 %), and cystine (∼11 %) were less affected . Loss of function of b (0 ,+)AT reduced transport of cystine and arginine in renal BBMVs and completely abolished the exchanger activity of dibasic amino acids with neutral amino acids . In conclusion , loss of Slc 7 a 9 function decreases the GFR and increases the excretion of several amino acids to a lesser extent than expected with no clear regulation at the mRNA and protein level of alternative transporters and no increased renal epithelial uptake . These observations indicate that transporters located in distal segments of the kidney and /or metabolic pathways may partially compensate for Slc 7 a 9 loss of function .