التفاصيل البيبلوغرافية
| العنوان: |
The Discovery of Two Novel Classes of 5,5-Bicyclic Nucleoside-Derived PRMT5 Inhibitors for the Treatment of Cancer |
| المؤلفون: |
Ryan V. Quiroz (10359236), Michael H. Reutershan (2470597), Sebastian E. Schneider (2198083), David Sloman (10359430), Brian M. Lacey (2135143), Brooke M. Swalm (10359433), Charles S. Yeung (2302963), Craig Gibeau (1586212), Daniel S. Spellman (2649097), Danica A. Rankic (1858132), Dapeng Chen (528941), David Witter (10359239), Doug Linn (10359436), Erik Munsell (10359439), Guo Feng (413683), Haiyan Xu (148626), Jonathan M. E. Hughes (6912470), Jongwon Lim (163671), Josep Saurí (1523239), Kristin Geddes (10359442), Murray Wan (10359445), My Sam Mansueto (3384113), Nicole E. Follmer (10359448), Patrick S. Fier (1333728), Phieng Siliphaivanh (1822588), Pierre Daublain (1625986), Rachel L. Palte (8299626), Robert P. Hayes (9220508), Sandra Lee (273007), Shuhei Kawamura (1407448), Steven Silverman (10359451), Sulagna Sanyal (2918147), Timothy J. Henderson (2397364), Yingchun Ye (2032282), Yuanwei Gao (3951080), Benjamin Nicholson (2035678), Michelle R. Machacek (2639716) |
| سنة النشر: |
2021 |
| المجموعة: |
Smithsonian Institution: Digital Repository |
| مصطلحات موضوعية: |
Biochemistry, Medicine, Genetics, Molecular Biology, Pharmacology, Hematology, Infectious Diseases, Biological Sciences not elsewhere classified, Chemical Sciences not elsewhere classified, novel designs, Novel Classes, balancing bioavailability, structure-based drug designs, DNA repair, type II arginine methyltransferase, Additional efforts, optimization strategies, bicyclic nucleoside-derived classes, protein substrates, identification, dose projections, PRMT 5 activity, Cancer Protein arginine methyltrans., RNA, CYP 3A inhibition, strain energy calculations, compound docking, vivo activity, PRMT 5, PRMT 5 inhibitors |
| الوصف: |
Protein arginine methyltransferase 5 (PRMT5) is a type II arginine methyltransferase that catalyzes the post-translational symmetric dimethylation of protein substrates. PRMT5 plays a critical role in regulating biological processes including transcription, cell cycle progression, RNA splicing, and DNA repair. As such, dysregulation of PRMT5 activity is implicated in the development and progression of multiple cancers and is a target of growing clinical interest. Described herein are the structure-based drug designs, robust synthetic efforts, and lead optimization strategies toward the identification of two novel 5,5-fused bicyclic nucleoside-derived classes of potent and efficacious PRMT5 inhibitors. Utilization of compound docking and strain energy calculations inspired novel designs, and the development of flexible synthetic approaches enabled access to complex chemotypes with five contiguous stereocenters. Additional efforts in balancing bioavailability, solubility, potency, and CYP3A4 inhibition led to the identification of diverse lead compounds with favorable profiles, promising in vivo activity, and low human dose projections. |
| نوع الوثيقة: |
dataset |
| اللغة: |
unknown |
| Relation: |
https://figshare.com/articles/dataset/The_Discovery_of_Two_Novel_Classes_of_5_5-Bicyclic_Nucleoside-Derived_PRMT5_Inhibitors_for_the_Treatment_of_Cancer/14272909 |
| DOI: |
10.1021/acs.jmedchem.0c02083.s002 |
| الاتاحة: |
https://doi.org/10.1021/acs.jmedchem.0c02083.s002 |
| Rights: |
CC BY-NC 4.0 |
| رقم الانضمام: |
edsbas.7BB390EE |
| قاعدة البيانات: |
BASE |