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Rana R. McKay, MD @DrRanaMcKay @UCSDHealth #ASCO20 Optimized management of nivolumab (Nivo) and ipilimumab (Ipi) in advanced renal cell carcinoma (RCC): A response-based phase II study (O…

Rana R. McKay, MD UC SD Health discusses ASCO 2020 abstract entitled Optimized management of nivolumab (Nivo) and ipilimumab (Ipi) in advanced renal cell carcinoma (RCC): A response-based phase II study (OMNIVORE)

Context:
For advanced RCC, Nivo + Ipi is a proven first-line treatment (tx). We hypothesized that not all patients (pts) would need to have CTLA-4 blockade applied. In addition, Nivo’s optimum maintenance time in response pts is not known. In this phase II response-adaptive trial, we investigate the sequential addition of 2 doses of Ipi in response pts (NCT03203473) to induce response in Nivo non-responders (NR) and duration of Nivo.

Approaches:
We have enrolled pts with advanced RCC without previous exposure to the checkpoint inhibitor. All pts received Nivo alone within 6 months (mos) of tx, with subsequent arm allocation based on RECISTv1.1 response. Nivo was discontinued and observed (Arm A) pts with a reported partial response (PR) or full response (CR) within 6 months (mos). Arm A pts reinitiated Nivo if progressive disease (PD) developed; when PD continued or recurred, Ipi was applied to Nivo. Pts with a stable disease (SD) or PD have obtained 2 doses of Ipi (Arm B) after no more than 6 mos of Nivo alone. The primary endpoints were the 1-year (yr) PR / CR proportion after Nivo discontinuation (Arm A) and the proportion of Nivo NR converting to PR / CR after Ipi (Arm B) addition.

Reviews:
83 pts initiated tx, of which 99% had ECOG 0-1, 96% clear cell RCC, 51% tx-naïve and 69% intermediate / poor IMDC risk. There was a median follow-up of 17.0 mos. The arm was not allocated 15 pts [7 withdrawals for PD, 7 withdrawals for toxicity, 1 only on tx with unconfirmed PR (uPR)]. At 6 mos, Nivo induction resulted in a verified PR at 11% of pts (n=9/83): 12% (n=5/42) tx-naïve, 10% (4/41) prior tx, 8% (n=1/13) favorable risk, 11% (n=8/70) intermediate / poor risk (Table). Arm A was assigned 11 pts (13 percent: 9 PR, 1 uPR, 1 SD), of which 5 (45 percent, 90 percent CI 20-73 percent) remained off Nivo at 1 year old. 2 pts converted to a PR (4 percent, 90 percent CI 1-11 percent) of 57 pts (69 percent) allocated to Arm B, both of which had previous tx and PD as the best response to Nivo alone. Adverse events associated with grade 3-4 treatment (TrAE) occurred in 7 percent (n=6/83) on Nivo induction and in 23 percent (n=13/57) on Arm B (Nivo + Ipi).

Conclusions Therein:
At present, due to the lack of CR and low PR / CR conversion rate (4 percent), we do not suggest a Nivo strategy followed by response-based Ipi addition. Although a subset of pts treated with Nivo alone can sustain a lasting response off tx at 1-yr, it is currently not recommendable to discontinue early Nivo in the absence of toxicity. Research into biomarkers to direct tx continues. Details on clinical trials: NCT03203473.

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