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Multicenter Study
. 2025 Apr 24;145(17):1858-1869.
doi: 10.1182/blood.2024026211.

Glucarpidase for treatment of high-dose methotrexate toxicity

Shruti Gupta  1   2   3 Sarah A Kaunfer  1 Kevin L Chen  4 Julie-Alexia Dias  4 Anitha Vijayan  5   6 Arun Rajasekaran  7 Jason M Prosek  8 Huong L Truong  9   10 Anthony Wood  11   12 Claude Bassil  13 Amanda D Renaghan  14 Chintan V Shah  15 Jingjing Zhang  16 Ilya Glezerman  17   18 Christopher Carlos  19 Katherine Kelly  20 Christopher J Passero  21 Jan Drappatz  22 Ala Abudayyeh  23 Daniel Sanghoon Shin  24 C John Sperati  25 Bradley J Yelvington  26 Swetha R Kanduri  27 Javier A Neyra  7   28 Daniel Edmonston  29 Anushree C Shirali  30 Anip Bansal  31 Abdallah Geara  32 Zain Mithani  33 Susan L Ziolkowski  34 Arash Rashidi  35 Jonathan Jakubowski  5 Ashwini Pujari  7 David A Bond  36 Emily Dotson  37 Sarah Wall  36 John Patton  36 Jason N Barreto  9 Sandra M Herrmann  38 Mohammad S Sheikh  38 Rachid Baz  12 Jamie Lee  12 Nicholas Lucchesi  14 Michael Kolman  15   39 Muhammad Ahsan Rasheed  16 Afsheen Afzal  17   18 Dasol Kang  17   18 Amrita Mahesh  19 Raymond K Hsu  19 Anthony Nicolaysen  40 Kibrewessen Tefera  40 Claire Schretlen  25   41 Ryan M Miller  26 Juan Carlos Velez  27 Alexander H Flannery  42 Abinet M Aklilu  29   43 Shuchi Anand  34 Soniya Chandrasekhara  44 Vicki Donley  35 Ashka Patel  45 Jian Ni  46 Shobana Krishnamurthy  1 Rafia Ali  1 Osman A Yilmam  1 Sophia L Wells  1 Jessica L Ortega  1 Olivia L Green-Lingren  1 Rebecca K Leaf  3   47 Meghan E Sise  3   48 Lakshmi Nayak  3   49   50 Ann S LaCasce  3   50 Nelson Leung  38 David E Leaf  1   3
Affiliations
Multicenter Study

Glucarpidase for treatment of high-dose methotrexate toxicity

Shruti Gupta et al. Blood. .

Abstract

High-dose methotrexate (MTX) results in high rates of acute kidney injury (AKI), neutropenia, and hepatotoxicity. Glucarpidase is a recombinant enzyme that cleaves MTX, but clinical data supporting its use are scarce. We examined the association between glucarpidase administration and outcomes in adults with MTX-AKI from 28 cancer centers across the United States using a sequential target trial emulation framework. The primary end point was kidney recovery at hospital discharge, defined as survival to discharge with serum creatinine <1.5-fold baseline and without dialysis dependence. Key secondary end points were time to kidney recovery, neutropenia, and transaminitis on day 7, and time to death. Using multivariable logistic and Cox regression models, we compared outcomes in patients who received glucarpidase within 4 days following MTX initiation with those in patients who did not. Among 708 patients with MTX-AKI, 209 (29.5%) received glucarpidase. Overall, 183 (25.8%) had a primary end point event. Glucarpidase receipt was associated with a 2.70-fold higher adjusted odds of kidney recovery (95% confidence interval [CI], 1.69-4.31) compared with no glucarpidase receipt. Patients treated with glucarpidase also had faster time to kidney recovery (adjusted hazard ratio [aHR], 1.88; 95% CI, 1.18-3.33) and lower risks of grade ≥2 neutropenia (adjusted odds ratio [aOR], 0.50; 95% CI, 0.28-0.91) and grade ≥2 transaminitis (aOR, 0.50; 95% CI, 0.28-0.91) on day 7. There was no difference in time to death (aHR, 0.76; 95% CI, 0.49-1.18). These data suggest glucarpidase may improve both renal and extrarenal outcomes in patients with MTX-AKI.

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