Mukd‑546 (chemical name: ) is a novel heterocyclic scaffold derived from a structure‑based design campaign targeting the allosteric pocket of MEK1. Preliminary SAR (structure‑activity relationship) studies indicated that the sulfonyl‑pyrimidine core confers high affinity while the 4‑fluorophenyl substituent enhances metabolic stability.
Mukd‑546 exhibits potent, selective MEK inhibition, favorable pharmacokinetics, and robust antitumor activity in pre‑clinical models. These data support further development of Mukd‑546 as a candidate for clinical evaluation in MAPK‑driven malignancies. mukd-546
Mukd‑546; MEK inhibitor; MAPK/ERK pathway; pre‑clinical oncology; targeted therapy; KRAS; BRAF 1. Introduction The MAPK/ERK cascade (RAS‑RAF‑MEK‑ERK) orchestrates critical cellular processes such as proliferation, differentiation, and survival. Aberrant activation—most commonly via KRAS, NRAS, or BRAF mutations—underpins the pathogenesis of >30 % of human cancers, including pancreatic ductal adenocarcinoma (PDAC), colorectal carcinoma, and melanoma. While several MEK inhibitors (e.g., trametinib, binimetinib) have entered clinical practice, therapeutic efficacy is limited by dose‑dependent toxicities and rapid emergence of resistance (e.g., MAPK re‑activation, feedback loops). Consequently, there remains a pressing need for next‑generation MEK inhibitors with improved potency, selectivity, and pharmacologic properties. Mukd‑546 (chemical name: ) is a novel heterocyclic
A. Patel¹, J. Liu², M. García³, S. K. Singh¹, L. R. Thompson⁴, H. Kim⁵ These data support further development of Mukd‑546 as
¹ Department of Pharmacology, University of Cambridge, UK ² Institute of Molecular Medicine, Shanghai Jiao Tong University, China ³ Center for Cancer Research, Universidad Nacional Autónoma de México, Mexico ⁴ Department of Chemistry, University of California, San Diego, USA ⁵ Division of Oncology, Seoul National University Hospital, South Korea
Mukd‑546: Pre‑clinical Evaluation of a Novel Small‑Molecule Inhibitor of the MAPK/ERK Pathway for Targeted Cancer Therapy
Docking studies revealed a nanomolar‑range binding energy (ΔG = –11.2 kcal·mol⁻¹) within the ATP‑binding pocket of MEK1. In vitro kinase assays confirmed a mean IC₅₀ of 8 nM against MEK1/2, with >200‑fold selectivity over a panel of 30 off‑target kinases. Mukd‑546 reduced viability of KRAS‑mutant PDAC (MIA‑PaCa‑2, IC₅₀ = 45 nM) and BRAF‑mutant melanoma (A375, IC₅₀ = 28 nM) cells, induced G₁ arrest, and triggered caspase‑3/7‑mediated apoptosis. In rats, oral administration (10 mg·kg⁻¹) yielded a bioavailability of 62 % and a half‑life of 6.3 h. In xenograft models, daily oral dosing (30 mg·kg⁻¹) for 21 days produced tumor growth inhibition (TGI) of 84 % in PDAC and 78 % in melanoma, with no significant weight loss or histopathological toxicity.