Dana-Farber Cancer Institute and Harvard Medical School, Boston, MA
Toni K. Choueiri , Daniel Yick Chin Heng , Jae-Lyun Lee , Mathilde Cancel , Remy B Verheijen , Anders Mellemgaard , Lone Ottesen , Melanie M. Frigault , Anne L'Hernault , Zsolt Szijgyarto , Sabina Signoretti , Laurence Albiges
Background: PRCC is the most common type of non-clear cell RCC, accounting for 10–15% of renal malignancies. As a subset of PRCC cases are MET-driven, MET inhibition may be an appropriate targeted treatment approach. In a single-arm Phase II study, savolitinib (AZD6094, HMPL‐504, volitinib), a highly selective MET-tyrosine kinase inhibitor, demonstrated antitumor activity in pts with MET-driven PRCC (Choueiri et al. JCO 2017). The Phase III SAVOIR study (NCT03091192) further assessed savolitinib vs standard of care sunitinib in pts with MET-driven PRCC. Methods: In this open-label (sponsor blinded), randomized study, pts with centrally confirmed MET-driven (MET and/or HGF amplification, chromosome 7 gain and/or MET kinase domain mutations), metastatic PRCC were randomized to savolitinib 600 mg once daily (QD), or sunitinib 50 mg QD 4 weeks on / 2 weeks off. Primary objective was progression-free survival (PFS; RECIST 1.1 by blinded independent central review). Secondary objectives included overall survival (OS), objective response rate (ORR), and safety and tolerability. Results: After external data on predicted PFS with sunitinib in pts with MET-driven disease became available, study enrollment was closed. At data cutoff (Aug 2019), only 60 of the planned 180 pts were randomized (savolitinib n = 33; sunitinib n = 27). Most had chromosome 7 gain (savolitinib 91%; sunitinib 96%) and no prior therapy (savolitinib 85%; sunitinib 93%). PFS, OS, and ORR were numerically improved with savolitinib vs sunitinib (Table). CTCAE grade ≥3 adverse events (AEs) were reported in 42% and 81% of pts; dose modifications were related to AEs in 30% and 74% of pts with savolitinib and sunitinib respectively. After discontinuation, 36% of all savolitinib and 19% of all sunitinib pts received subsequent anticancer therapy. Conclusions: Although pt numbers and follow-up were limited, savolitinib demonstrated encouraging efficacy and an improved safety profile vs sunitinib, with fewer grade ≥3 AEs and fewer dose modifications required. Sunitinib performance was poorer than expected based on external retrospective data. Further investigation of savolitinib as a treatment option for MET-driven PRCC is warranted. Clinical trial information: NCT03091192.
Savolitinib (n = 33) | Sunitinib (n = 27) | |
---|---|---|
PFS events, n (%) | 17 (52) | 20 (74) |
Median PFS (95% CI), mo | 7.0 (2.8, NR) | 5.6 (4.1, 6.9) |
HR (95% CI) | 0.71 (0.37, 1.36); p = 0.313 | |
Deaths, n (%) | 9 (27) | 13 (48) |
Median OS (95% CI), mo | NR (11.9, NR) | 13.2 (7.6, NR) |
HR (95% CI) | 0.51 (0.21, 1.17); p = 0.110 | |
ORR n (%) [95% CI] All partial responses | 9 (27) [13.3, 45.5] | 2 (7) [0.9, 24.3] |
NR, not reached
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Abstract Disclosures
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First Author: John Raymond Zalcberg
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First Author: Toni K. Choueiri
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