| Literature DB >> 33335659 |
Venkateshwar Rao Gummadi1, Anima Boruah2, Bharathi Raja Ainan1, Brahma Reddy Vare1, Srinivas Manda1, Hari Prakash Gondle1, Shiva Nagendra Kumar1, Subhendu Mukherjee1, Suraj T Gore1, Narasimha Rao Krishnamurthy1, Sivapriya Marappan1, Shilpa S Nayak1, Kavitha Nellore1, Wesley Roy Balasubramanian1, Archana Bhumireddy1, Sanjeev Giri1, Sreevalsam Gopinath1, Dodheri S Samiulla1, Girish Daginakatte1, Aravind Basavaraju1, Shekar Chelur1, Rajesh Eswarappa2, Charamanna Belliappa1, Hosahalli S Subramanya1, Robert N Booher3, Murali Ramachandra1, Susanta Samajdar1.
Abstract
Small molecule potent IRAK4 inhibitors from a novel bicyclic heterocycle class were designed and synthesized based on hits identified from Aurigene's compound library. The advanced lead compound, CA-4948, demonstrated good cellular activity in ABC DLBCL and AML cell lines. Inhibition of TLR signaling leading to decreased IL-6 levels was also observed in whole blood assays. CA-4948 demonstrated moderate to high selectivity in a panel of 329 kinases as well as exhibited desirable ADME and PK profiles including good oral bioavailability in mice, rat, and dog and showed >90% tumor growth inhibition in relevant tumor models with excellent correlation with in vivo PD modulation. CA-4948 was well tolerated in toxicity studies in both mouse and dog at efficacious exposure. The overall profile of CA-4948 prompted us to select it as a clinical candidate for evaluation in patients with relapsed or refractory hematologic malignancies including non-Hodgkin lymphoma and acute myeloid leukemia.Entities:
Year: 2020 PMID: 33335659 PMCID: PMC7734642 DOI: 10.1021/acsmedchemlett.0c00255
Source DB: PubMed Journal: ACS Med Chem Lett ISSN: 1948-5875 Impact factor: 4.345