Data from Clinical Activity of Ripretinib in Patients with Advanced Gastrointestinal Stromal Tumor Harboring Heterogeneous <i>KIT/PDGFRA</i> Mutations in the Phase III INVICTUS Study — Sebastian Bauer (2023) | RDL Network
Data from Clinical Activity of Ripretinib in Patients with Advanced Gastrointestinal Stromal Tumor Harboring Heterogeneous <i>KIT/PDGFRA</i> Mutations in the Phase III INVICTUS Study
Preprint 2023 en
Authors
SB
Sebastian Bauer
MH
Michael C. Heinrich
SG
Suzanne George
Abstract
1 min read
<div>AbstractPurpose:<p>Most patients with gastrointestinal stromal tumor (GIST) have activating mutations in <i>KIT/PDGFRA</i> and are initially responsive to tyrosine kinase inhibitors (TKI). The acquisition of secondary mutations leads to refractory/relapsed disease. This study reports the results of an analysis from the phase III INVICTUS study (NCT03353753) characterizing the genomic heterogeneity of tumors from patients with advanced GIST and evaluating ripretinib efficacy across <i>KIT/PDGFRA</i> mutation subgroups.</p>Patients and Methods:<p>Tumor tissue and liquid biopsy samples that captured circulating tumor DNA were collected prior to study enrollment and sequenced using next-generation sequencing. Subgroups were determined by <i>KIT/PDGFRA</i> mutations and correlation of clinical outcomes and <i>KIT/PDGFRA</i> mutational status was assessed.</p>Results:<p>Overall, 129 patients enrolled (ripretinib 150 mg once daily, <i>n</i> = 85; placebo, <i>n</i> = 44). The most common primary mutation subgroup detected by combined tissue and liquid biopsies were in <i>KIT</i> exon 11 (ripretinib, 61.2%; placebo, 77.3%) and <i>KIT</i> exon 9 (ripretinib, 18.8%; placebo, 15.9%). Patients receiving ripretinib demonstrated progression-free survival (PFS) benefit versus placebo regardless of mutation status (HR 0.16) and in all assessed subgroups in Kaplan–Meier PFS analysis (exon 11, <i>P</i> < 0.0001; exon 9, <i>P</i> = 0.0023; exon 13, <i>P</i> < 0.0001; exon 17, <i>P</i> < 0.0001). Among patients with wild-type <i>KIT/PDGFRA</i> by tumor tissue, PFS ranged from 2 to 23 months for ripretinib versus 0.9 to 10.1 months for placebo.</p>Conclusions:<p>Ripretinib provided clinically meaningful activity across mutation subgroups in patients with advanced GIST, demonstrating that ripretinib inhibits a broad range of <i>KIT/PDGFRA</i> mutations in patients with advanced GIST who were previously treated with three or more TKIs.</p></div>
Sebastian Bauer, Michael C. Heinrich, Suzanne George, John Zalcberg, César Serrano, Hans Gelderblom, Robin L. Jones, Steven Attia, Gina Z. D’Amato, Ping Chi, Peter Reichardt, Julie Meade, Ying Su, Rodrigo Ruiz‐Soto, Jean Yves Blay, Margaret von Mehren, Patrick Schöffski
Sebastian Bauer, Michael C. Heinrich, Suzanne George, John Zalcberg, César Serrano, Hans Gelderblom, Robin L. Jones, Steven Attia, Gina Z. D’Amato, Ping Chi, Peter Reichardt, Julie Meade, Ying Su, Rodrigo Ruiz‐Soto, Jean Yves Blay, Margaret von Mehren, Patrick Schöffski
Suzanne George, Jean Yves Blay, Ping Chi, Robin L. Jones, César Serrano, Neeta Somaiah, Hans Gelderblom, John Zalcberg, William M. Reichmann, Kam Sprott, P. H. Cox, Matthew L. Sherman, Rodrigo Ruiz‐Soto, Michael C. Heinrich, Sebastian Bauer
Jonathan C. Trent, Robin L. Jones, Suzanne George, Hans Gelderblom, Patrick Schöffski, Margaret von Mehren, John Zalcberg, Yoon‐Koo Kang, Albiruni Ryan Abdul Razak, Steven Attia, Axel Le Cesne, William M. Reichmann, Kam Sprott, Haroun Achour, Matthew L. Sherman, Rodrigo Ruiz‐Soto, Jean Yves Blay, Michael C. Heinrich, Sebastian Bauer
Salvatore Romeo, Maria Dêbiec‐Rychter, M. van Glabbeke, Heidi Van Paassen, Paola Comite, Ronald van Eijk, Jan Oosting, Jaap Verweij, Philippe Terrier, Ulrike Schneider, Raf Sciot, Jean Yves Blay, Pancras C.W. Hogendoorn
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