PT  - JOURNAL ARTICLE
AU  - Scott M. Ocheltree
AU  - Hong Shen
AU  - Yongjun Hu
AU  - Jianming Xiang
AU  - Richard F. Keep
AU  - David E. Smith
TI  - Mechanisms of Cefadroxil Uptake in the Choroid Plexus: Studies in Wild-Type and PEPT2 Knockout Mice
AID  - 10.1124/jpet.103.060400
DP  - 2004 Feb 01
TA  - Journal of Pharmacology and Experimental Therapeutics
PG  - 462--467
VI  - 308
IP  - 2
4099  - http://jpet.aspetjournals.org/content/308/2/462.short
4100  - http://jpet.aspetjournals.org/content/308/2/462.full
SO  - J Pharmacol Exp Ther2004 Feb 01; 308
AB  - The choroid plexus uptake of [3H]cefadroxil was studied in peptide transporter 2 (PEPT2) wild-type and null mice as a function of temperature, transport inhibitors, pH, and saturability. At normal pH (7.4) and temperature (37°C), the uptake of 1 μM cefadroxil was reduced by 83% in PEPT2–/– mice as compared with PEPT2+/+ mice (p &amp;lt; 0.001). A further reduction was achieved in null animals by reducing the temperature to 4°C, or by adding saturating concentrations of unlabeled cefadroxil or p-aminohippurate (p &amp;lt; 0.05). Glycylsarcosine coadministration could inhibit the uptake of cefadroxil in PEPT2+/+ mice (p &amp;lt; 0.01) but not PEPT2–/– mice. Although a proton-stimulated uptake of cefadroxil was demonstrated in PEPT2+/+ mice (pH 6.5 versus pH 7.4; p &amp;lt; 0.01), no pH dependence was observed in PEPT2–/– mice. Kinetic parameters for cefadroxil (without p-aminohippurate) in wild-type mice were: Vmax = 5.4 pmol/mg/min, Km = 34 μM, and Kd = 0.0069 μl/mg/min; in the presence of p-aminohippurate, the parameters were: Vmax = 4.1 pmol/mg/min, Km = 27 μM, and Kd = 0.0064 μl/mg/min. In null animals, the kinetic parameters of cefadroxil (without p-aminohippurate) were: Vmax = 2.7 pmol/mg/min, Km = 110 μM, and Kd = 0.0084 μl/mg/min; in the presence of p-aminohippurate, only a Kd = 0.010 μl/mg/min was observed. Based on kinetic and inhibitor analyses, it was determined that (under linear conditions), 80 to 85% of cefadroxil&#039;s uptake in choroid plexus is mediated by PEPT2, 10 to 15% by organic anion transporter(s), and 5% by nonspecific mechanisms. These findings demonstrate that PEPT2 is the primary transporter responsible for cefadroxil uptake in the choroid plexus. Moreover, the data suggest a role for PEPT2 in the clearance of peptidomimetics from cerebrospinal fluid. The American Society for Pharmacology and Experimental Therapeutics