Abstract 2607: Antitumor activity of the selective RAF inhibitor HM95573 in solid tumors and hematologic malignancies

Lee, Young-Mi; Bae, Inhyu; Mo, Namgoong Gwang; Lee, Jae Ho; Kim, Suhyeon; Song, Ji Yeon; Lee, Kyu Hang; Song, Taehun; Ahn, Young Gil; Kim, Young Hoon; Suh, Kwee Hyun

doi:10.1158/1538-7445.am2015-2607

Cited by 2 publications

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“…22 is under phase I clinical evaluation in patients with solid malignancies − Lastly, a compound from Novartis, 24 (LXH254), is an equipotent BRAF monomer–dimer inhibitor currently in clinical phase I development . The chemical structures of 23 and 24 have not been disclosed.…”

Section: Progress In Raf Kinase Inhibitor Developmentmentioning

confidence: 99%

Current Insights of BRAF Inhibitors in Cancer

2018

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Oncogenic BRAF kinase deregulates the ERK signaling pathway in a large number of human tumors. FDA-approved BRAF inhibitors for BRAFV600E/K tumors have provided impressive clinical responses extending survival of melanoma patients. However, these drugs display paradoxical activation in normal tissue with BRAFWT due to RAF transactivation and priming, acquired drug resistance, and limited clinical effectiveness in non-V600 BRAF-dependent tumors, underscoring the urgent need to develop improved BRAF inhibitors. This review provides an overview of recent structural and biochemical insights into the mechanisms of BRAF regulation by BRAF inhibitors that are linked to their clinical activity, clinical liabilities, and medicinal chemistry properties. The effectiveness and challenges of structurally diverse next generation RAF inhibitors currently in preclinical and clinical development are discussed, along with mechanistic insights for developing more effective RAF inhibitors targeting different oncogenic BRAF conformations.

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Section: Progress In Raf Kinase Inhibitor Developmentmentioning

confidence: 99%