AUTHOR=Fukaya Yutaka , Kimura Toshimi , Hamada Yukihiro , Yoshimura Kenichi , Hiraga Hiroaki , Yuza Yuki , Ogawa Atsushi , Hara Junichi , Koh Katsuyoshi , Kikuta Atsushi , Koga Yuhki , Kawamoto Hiroshi 

TITLE=Development of a population pharmacokinetics and pharmacodynamics model of glucarpidase rescue treatment after high-dose methotrexate therapy

JOURNAL=Frontiers in Oncology

VOLUME=13

YEAR=2023

URL=https://www.frontiersin.org/journals/oncology/articles/10.3389/fonc.2023.1003633

DOI=10.3389/fonc.2023.1003633

ISSN=2234-943X

ABSTRACT=<sec><title>Introduction</title><p>Glucarpidase (CPG2) reduces the lethal toxicity of methotrexate (MTX) by rapid degradation.</p></sec><sec><title>Methods</title><p>In this study, a CPG2 population pharmacokinetics (popPK) analysis in healthy volunteers (phase 1 study) and a popPK-pharmacodynamics (popPK-PD) analysis in patients (phase 2 study, <italic>n</italic> = 15) who received 50 U/kg of CPG2 rescue for delayed MTX excretion were conducted. In the phase 2 study, the first CPG2 treatment at a dose of 50 U/kg was intravenously administered for 5 min within 12 h after the first confirmation of delayed MTX excretion. The second dose of CPG2, with a plasma MTX concentration &gt;1 μmol/L, was administered to the patient more than 46 h after the start of CPG2 administration.</p></sec><sec><title>Results</title><p>The population mean PK parameters (95% CI) of MTX, obtained from the final model <italic>post hoc</italic>, were estimated as follows: <italic>CLr<sub>MTX</sub></italic> = 2.424 L/h (95% CI: 1.755–3.093), <italic>Vc<sub>MTX</sub></italic> = 12.6 L (95% CI: 10.8–14.3), <italic>Vp<sub>MTX</sub></italic> = 2.15 L (95% CI: 1.60–2.70), and <italic>α</italic> = 8.131 x 10<sup>5</sup> (4.864 x 10<sup>5</sup>-11.398 x 10<sup>5</sup>). The final model, including covariates, was <italic>CLr<sub>MTX</sub></italic> (L/h): 3.248 x <italic>Body Weight</italic>/<italic>Serum creatinine/</italic>60 (CV 33.5%), <italic>Vc<sub>MTX</sub></italic> (L): 0.386 x <italic>Body Weight/body surface area</italic> (CV 29.1%), <italic>Vp<sub>MTX</sub></italic> (L):3.052 x <italic>Body Weight</italic>/60 (CV 90.6%), and <italic>α</italic> (L/h): 6.545 x 10<sup>5</sup> (CV 79.8%).</p></sec><sec><title>Discussion</title><p>These results suggest that the pre-CPG2 dose and 24 h after CPG2 dosing were the most important sampling points in the Bayesian estimation of plasma MTX concentration prediction at 48 h. These CPG2-MTX popPK analysis and Bayesian estimation of rebound in plasma MTX concentrations are clinically important to estimate &gt;1.0 μmol/L 48 h after the first CPG2 dosing.</p></sec><sec><title>Clinical trial registration</title><p><uri xlink:href="https://dbcentre3.jmacct.med.or.jp/JMACTR/App/JMACTRS06/JMACTRS06.aspx?seqno=2363" xmlns:xlink="http://www.w3.org/1999/xlink">https://dbcentre3.jmacct.med.or.jp/JMACTR/App/JMACTRS06/JMACTRS06.aspx?seqno=2363</uri>, identifier JMA-IIA00078 and <uri xlink:href="https://dbcentre3.jmacct.med.or.jp/JMACTR/App/JMACTRS06/JMACTRS06.aspx?seqno=2782" xmlns:xlink="http://www.w3.org/1999/xlink">https://dbcentre3.jmacct.med.or.jp/JMACTR/App/JMACTRS06/JMACTRS06.aspx?seqno=2782</uri>, identifier JMA-IIA00097.</p></sec>