Selinexor in Advanced, Metastatic Dedifferentiated Liposarcoma: A Multinational, Randomized, Double-Blind, Placebo-Controlled Trial

Authors

Mrinal M Gounder
Albiruni Abdul Razak
Neeta Somaiah
Sant Chawla
Javier Martin-Broto
Giovanni Grignani
Scott M Schuetze
Bruno Vincenzi
Andrew J Wagner
Bartosz Chmielowski
Robin L Jones
Richard F Riedel
Silvia Stacchiotti
Elizabeth T Loggers
Kristen N Ganjoo
Axel Le Cesne
Antoine Italiano
Xavier Garcia Del Muro
Melissa Burgess
Sophie Piperno-Neumann
Christopher Ryan
Mary F Mulcahy
Charles Forscher
Nicolas Penel
Scott Okuno
Anthony Elias
Lee Hartner
Tony Philip
Thierry Alcindor
Bernd Kasper
Peter Reichardt
Lore Lapeire
Jean-Yves Blay
Christine Chevreau
Claudia Maria Valverde Morales
Gary K Schwartz
James L Chen
Hari Deshpande
Elizabeth J Davis
Garth Nicholas
Stefan Gröschel
Helen Hatcher
Florence Duffaud
Antonio Casado Herráez
Roberto Diaz Beveridge
Giuseppe Badalamenti
Mikael Eriksson
Christian Meyer
Margaret von Mehren
Brian A Van Tine
Katharina Götze
Filomena Mazzeo
Alexander Yakobson
Aviad Zick
Alexander Lee
Anna Estival Gonzalez
Andrea Napolitano
Mark A Dickson
Dayana Michel
Changting Meng
Lingling Li
Jianjun Liu
Osnat Ben-Shahar
Dane R Van Domelen
Christopher J Walker
Hua Chang
Yosef Landesman
Jatin J Shah
Sharon Shacham
Michael G Kauffman
Steven Attia

Publication Date

8-1-2022

Journal

Journal of Clinical Oncology

Abstract

Purpose: Antitumor activity in preclinical models and a phase I study of patients with dedifferentiated liposarcoma (DD-LPS) was observed with selinexor. We evaluated the clinical benefit of selinexor in patients with previously treated DD-LPS whose sarcoma progressed on approved agents.

Methods: SEAL was a phase II-III, multicenter, randomized, double-blind, placebo-controlled study. Patients age 12 years or older with advanced DD-LPS who had received two-five lines of therapy were randomly assigned (2:1) to selinexor (60 mg) or placebo twice weekly in 6-week cycles (crossover permitted). The primary end point was progression-free survival (PFS). Patients who received at least one dose of study treatment were included for safety analysis (ClinicalTrials.gov identifier: NCT02606461).

Results: Two hundred eighty-five patients were enrolled (selinexor, n = 188; placebo, n = 97). PFS was significantly longer with selinexor versus placebo: hazard ratio (HR) 0.70 (95% CI, 0.52 to 0.95; one-sided P = .011; medians 2.8 v 2.1 months), as was time to next treatment: HR 0.50 (95% CI, 0.37 to 0.66; one-sided P < .0001; medians 5.8 v 3.2 months). With crossover, no difference was observed in overall survival. The most common treatment-emergent adverse events of any grade versus grade 3 or 4 with selinexor were nausea (151 [80.7%] v 11 [5.9]), decreased appetite (113 [60.4%] v 14 [7.5%]), and fatigue (96 [51.3%] v 12 [6.4%]). Four (2.1%) and three (3.1%) patients died in the selinexor and placebo arms, respectively. Exploratory RNA sequencing analysis identified that the absence of CALB1 expression was associated with longer PFS with selinexor compared with placebo (median 6.9 v 2.2 months; HR, 0.19; P = .001).

Conclusion: Patients with advanced, refractory DD-LPS showed improved PFS and time to next treatment with selinexor compared with placebo. Supportive care and dose reductions mitigated side effects of selinexor. Prospective validation of CALB1 expression as a predictive biomarker for selinexor in DD-LPS is warranted.

Keywords

Child, Double-Blind Method, Humans, Hydrazines, Liposarcoma, Triazoles

DOI

10.1200/JCO.21.01829

PMID

35394800

PMCID

PMC9467680

PubMedCentral® Posted Date

8-1-2022

PubMedCentral® Full Text Version

Post-print

Published Open-Access

yes