Submission Details

NAU-LAT-64bf4c5d
Molecule(s):
O=C1CC(NC(=O)C2CCOc3ccc(Cl)cc32)c2ccccc21

NAU-LAT-64bf4c5d-1
Duplicate of:
ALP-POS-8b8a49e1-2

O=C1CC(NC(=O)C2CCOc3ccc(Cl)cc32)c2ccccc21

Duplicate 3-aminopyridine-like Check Availability on Manifold View
O=C1CN(C(=O)C2CCOc3ccc(Cl)cc32)c2ccccc21

NAU-LAT-64bf4c5d-2

O=C1CN(C(=O)C2CCOc3ccc(Cl)cc32)c2ccccc21

O=C1CC(C(=O)NC2CCOc3ccc(Cl)cc32)c2ccccc21

NAU-LAT-64bf4c5d-3

O=C1CC(C(=O)NC2CCOc3ccc(Cl)cc32)c2ccccc21

3-aminopyridine-like Check Availability on Manifold View
O=C1CC(C(=O)N2CCOc3ccc(Cl)cc32)c2ccccc21

NAU-LAT-64bf4c5d-4

O=C1CC(C(=O)N2CCOc3ccc(Cl)cc32)c2ccccc21

O=C1CN(C(=O)NC2CCOc3ccc(Cl)cc32)c2ccccc21

NAU-LAT-64bf4c5d-5

O=C1CN(C(=O)NC2CCOc3ccc(Cl)cc32)c2ccccc21

3-aminopyridine-like Check Availability on Manifold View
O=C1CN(C(=O)OC2CCOc3ccc(Cl)cc32)c2ccccc21

NAU-LAT-64bf4c5d-6

O=C1CN(C(=O)OC2CCOc3ccc(Cl)cc32)c2ccccc21

Design Rationale:

Recently published screening of fragments (10.1002/anie.202109965) identified a fragment, which is similar in both structure and binding pose (PDB: 7P51) to the lead inhibitors on Moonshot project. Most importantly, the indanone moiety of the fragment almost identically overlaps with the isoquinoline moiety in lead structures, thus indanone might be used as a bioisosteric replacement. This change adds another stereocentre, but could improve logP, f(sp3), metabolism etc. Some simple structures are proposed to check this hypothesis.

Inspired By:
Discussion:

Contributor: Nauris Narvaiss, Latvian Institute of Organic synthesis - Fri, 29 Oct 2021 12:26:36 +0000