Stereochemical Differences in Fluorocyclopropyl Amides Enable Tuning of Btk Inhibition and Off-Target Activity | Zendy

James J. Crawford | Zendy; Wendy Lee | Zendy; Adam R. Johnson | Zendy; Kelly J. Delatorre | Zendy; Jacob Chen | Zendy; Charles Eigenbrot | Zendy; Julia D. Heidmann | Zendy; Satoko Kakiuchi-Kiyota | Zendy; Arna Katewa | Zendy; James R. Kiefer | Zendy; Lichuan Liu | Zendy; Joseph W. Lubach | Zendy; Dinah Misner | Zendy; Hans E. Purkey | Zendy; Karin Reif | Zendy; Jennifer Vogt | Zendy; Harvey Wong | Zendy; Christine Yu | Zendy; Wendy B. Young | Zendy

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Stereochemical Differences in Fluorocyclopropyl Amides Enable Tuning of Btk Inhibition and Off-Target Activity

Author(s) -

James J. Crawford,

Wendy Lee,

Adam R. Johnson,

Kelly J. Delatorre,

Jacob Chen,

Charles Eigenbrot,

Julia D. Heidmann,

Satoko Kakiuchi-Kiyota,

Arna Katewa,

James R. Kiefer,

Lichuan Liu,

Joseph W. Lubach,

Dinah Misner,

Hans E. Purkey,

Karin Reif,

Jennifer Vogt,

Harvey Wong,

Christine Yu,

Wendy B. Young

Publication year - 2020

Publication title -

acs medicinal chemistry letters

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 1.065

H-Index - 66

ISSN - 1948-5875

DOI - 10.1021/acsmedchemlett.0c00249

Subject(s) - bruton's tyrosine kinase , rheumatoid arthritis , ibrutinib , tyrosine kinase , medicine , pharmacology , amide , chemistry , cancer research , immunology , biochemistry , chronic lymphocytic leukemia , leukemia , receptor

Bruton's tyrosine kinase (Btk) is thought to play a pathogenic role in chronic immune diseases such as rheumatoid arthritis and lupus. While covalent, irreversible Btk inhibitors are approved for treatment of hematologic malignancies, they are not approved for autoimmune indications. In efforts to develop additional series of reversible Btk inhibitors for chronic immune diseases, we sought to differentiate from our clinical stage inhibitor fenebrutinib using cyclopropyl amide isosteres of the 2-aminopyridyl group to occupy the flat, lipophilic H2 pocket. While drug-like properties were retained-and in some cases improved-a safety liability in the form of hERG inhibition was observed. When a fluorocyclopropyl amide was incorporated, Btk and off-target activity was found to be stereodependent and a lead compound was identified in the form of the ( R , R )- stereoisomer.

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