Peer-reviewed veterinary case report
New drug RV1001 shows promise for treating lymphoma in dogs
By Heather L. Gardner et al.·Published in PLoS ONE·2018·View original on Semantic Scholar →
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Original publication title: Phase I/II evaluation of RV1001, a novel PI3Kδ inhibitor, in spontaneous canine lymphoma
- Species:
- dog
Plain-English summary
A group of dogs with lymphoma, a type of cancer affecting the immune system, were treated with a new medication called RV1001 to see how well it worked. Out of 21 dogs in the first phase of the study, 62% showed improvement, with some dogs experiencing complete or partial remission. In a follow-up phase with 35 dogs, the response rate increased to 77%. While some dogs experienced side effects like liver and stomach issues, these were manageable with dose adjustments. Overall, RV1001 showed promise as an effective treatment for dogs with lymphoma.
People also search for: dog lymphoma treatment · RV1001 for canine cancer · side effects of lymphoma medication in dogs
Abstract
Background RV1001 is a novel, potent, and selective PI3Kδ inhibitor. The purpose of this study was to evaluate the safety and efficacy of RV1001 in canine Non-Hodgkin lymphoma (NHL). Methods and results Inhibition of endogenous pAKT by RV1001 in primary canine NHL cells was determined by Western blotting. A phase I study of RV1001 was performed in 21 dogs with naïve and drug resistant T and B-cell NHL to assess safety, pharmacokinetic profile, and response to therapy. The objective response rate was 62% (complete response (CR) n = 3; partial response (PR) n = 10), and responses were observed in both naïve and chemotherapy-resistant B and T cell NHL. This study provided the recommended starting dose for a phase II, non-pivotal, exploratory, open label multi-centered clinical trial in 35 dogs with naïve and drug resistant T and B-cell NHL, to further define the efficacy and safety profile of RV1001. The objective response rate in the phase II study was 77% (CR n = 1; PR n = 26). Clinical toxicities were primarily hepatobiliary and gastrointestinal, and were responsive to dose modifications and/or temporary drug discontinuation. Hepatotoxicity was the primary dose limiting toxicity. Conclusions RV1001 exhibits good oral bioavailability, an acceptable safety profile, and biologic activity with associated inhibition of pAKT in dogs with B and T cell NHL. Data from these studies can be leveraged to help inform the design of future studies involving isoform-selective PI3K inhibitors in humans.
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Search related cases →Original publication on Semantic Scholar: https://www.semanticscholar.org/paper/29689086