Literature DB >> 9808697

Noncompetitive inhibition of glycylsarcosine transport by quinapril in rabbit renal brush border membrane vesicles: effect on high-affinity peptide transporter.

W Akarawut1, C J Lin, D E Smith.   

Abstract

Angiotensin converting enzyme (ACE) inhibitors are important therapeutic agents for treating patients with hypertension and cardiovascular diseases. Although most ACE inhibitors are cleared by the kidney via glomerular filtration and tubular secretion, little is known about their reabsorption potential. In particular, it is believed that while certain ACE inhibitors are transported by the intestinal peptide transporter (PepT1), these same compounds do not interact with the renal peptide transporter (PepT2). In the present study, we examined the interaction of quinapril with the high-affinity peptide transporter, PepT2. Studies were performed in rabbit renal brush border membrane vesicles in which the uptake of [14C]glycylsarcosine (GlySar), at low substrate concentrations, was examined in the absence and presence of quinapril (and other ACE inhibitors). We found that quinapril was capable of cis-inhibiting the uptake of GlySar and in a concentration-dependent manner. While the Ki for quinapril ( approximately 1 mM) was several-fold higher than the Km for GlySar ( approximately 160 microM), the interaction was unique in that inhibition of PepT2 was of a noncompetitive type. Overall, the data suggest that quinapril is a low-affinity inhibitor of the renal peptide transporter and that it binds to a site distinct from that of the GlySar binding site.

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Year:  1998        PMID: 9808697

Source DB:  PubMed          Journal:  J Pharmacol Exp Ther        ISSN: 0022-3565            Impact factor:   4.030


  9 in total

1.  Effects of glibenclamide on glycylsarcosine transport by the rat peptide transporters PEPT1 and PEPT2.

Authors:  K Sawada; T Terada; H Saito; Y Hashimoto; K Inui
Journal:  Br J Pharmacol       Date:  1999-11       Impact factor: 8.739

2.  Glycylsarcosine uptake in rabbit renal brush border membrane vesicles isolated from outer cortex or outer medulla: evidence for heterogeneous distribution of oligopeptide transporters.

Authors:  C J Lin; D E Smith
Journal:  AAPS PharmSci       Date:  1999

3.  Competitive inhibition of glycylsarcosine transport by enalapril in rabbit renal brush border membrane vesicles: interaction of ACE inhibitors with high-affinity H+/peptide symporter.

Authors:  C J Lin; W Akarawut; D E Smith
Journal:  Pharm Res       Date:  1999-05       Impact factor: 4.200

4.  Differential recognition of ACE inhibitors in Xenopus laevis oocytes expressing rat PEPT1 and PEPT2.

Authors:  T Zhu; X Z Chen; A Steel; M A Hediger; D E Smith
Journal:  Pharm Res       Date:  2000-05       Impact factor: 4.200

5.  Abnormal expression of the peptide transporter PepT1 in the colon of massive bowel resection rat: a potential route for colonic mucosa damage by transport of fMLP.

Authors:  Bin Shi; Desheng Song; Hua Xue; Jinhai Li; Ning Li; Jieshou Li
Journal:  Dig Dis Sci       Date:  2006-09-29       Impact factor: 3.199

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Authors:  Vidula Kolhatkar; James E Polli
Journal:  Pharm Res       Date:  2010-08-14       Impact factor: 4.200

7.  Targeted disruption of peptide transporter Pept1 gene in mice significantly reduces dipeptide absorption in intestine.

Authors:  Yongun Hu; David E Smith; Ke Ma; Dilara Jappar; Winston Thomas; Kathleen M Hillgren
Journal:  Mol Pharm       Date:  2008 Nov-Dec       Impact factor: 4.939

8.  Novel inhibitors of human organic cation/carnitine transporter (hOCTN2) via computational modeling and in vitro testing.

Authors:  Lei Diao; Sean Ekins; James E Polli
Journal:  Pharm Res       Date:  2009-05-13       Impact factor: 4.200

9.  Theoretical analysis of headache recurrence in patients administered triptans for migraine based on receptor occupancy.

Authors:  Kentaro Tokuoka; Risa Takayanagi; Mioko Toyabe; Masayuki Watanabe; Yasuhisa Kitagawa; Yasuhiko Yamada
Journal:  J Headache Pain       Date:  2015-08-05       Impact factor: 7.277

  9 in total

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