MMV367

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Ligands
MMV367

GtoPdb Ligand ID: 13673

Synonyms: GSK3772701 | GSK701 | MMV1582367

Comment: MMV367 is an antimalarial clinical candidate, selected from a new class of pyrrolidinamide-containing compounds identified from a phenotypic screen. The chemical structure was first disclosed during the 265th National Meeting of the American Chemical Society (Boston, 2018) [4] and is one of the structures claimed in patent WO2019145360A1 [2].

The Malaria tab on this ligand page provides additional curator comments of relevance to the Guide to MALARIA PHARMACOLOGY.

2D Structure

Physico-chemical Properties

Hydrogen bond acceptors	8
Hydrogen bond donors	1
Rotatable bonds	8
Topological polar surface area	90.09
Molecular weight	411.43
XLogP	0.34
No. Lipinski's rules broken	0

Generated using the Chemistry Development Kit (CDK) (Willighagen EL et al. Journal of Cheminformatics vol. 9:33. 2017, doi:10.1186/s13321-017-0220-4; https://cdk.github.io/)

SMILES / InChI / InChIKey

Canonical SMILES	C1=C(C=CC(=C1)F)[C@H]2CCN(C2)C(=O)C3=CC=C(C=C3)OC[C@@H](CN4N=CN=N4)O
Isomeric SMILES	C1CN(C[C@H]1C2=CC=C(C=C2)F)C(=O)C3=CC=C(C=C3)OC[C@@H](CN4N=CN=N4)O
InChI	InChI=1S/C21H22FN5O3/c22-18-5-1-15(2-6-18)17-9-10-26(11-17)21(29)16-3-7-20(8-4-16)30-13-19(28)12-27-24-14-23-25-27/h1-8,14,17,19,28H,9-13H2/t17-,19+/m0/s1
InChI Key	RMWYAYFMEWWLSK-PKOBYXMFSA-N

Generated using the Chemistry Development Kit (CDK) (Willighagen EL et al. Journal of Cheminformatics vol. 9:33. 2017, doi:10.1186/s13321-017-0220-4; https://cdk.github.io/)

References
1. Bopp S, Pasaje CFA, Summers RL, Magistrado-Coxen P, Schindler KA, Corpas-Lopez V, Yeo T, Mok S, Dey S, Smick S et al.. (2023) Potent acyl-CoA synthetase 10 inhibitors kill Plasmodium falciparum by disrupting triglyceride formation. Nat Commun, 14 (1): 1455. [PMID:36927839]
2. Castellote I, León ML, Hernando JI. (2019) Novel compounds for the treatment of parasitic infections. Patent number: WO2019145360A1. Assignee: Glaxosmithkline Intellectual Property Development Limited. Priority date: 23/01/2019. Publication date: 01/08/2019.
3. Kanai M, Hagenah LM, Ashley EA, Chibale K, Fidock DA. (2022) Keystone Malaria Symposium 2022: a vibrant discussion of progress made and challenges ahead from drug discovery to treatment. Trends Parasitol, 38 (9): 711-718. [PMID:35864072]
4. Rami H, Castellote I, Gamo FJ, Haselden J, Calderon Romo F. Discovery of pyrrolidinamides, a novel chemical class for malaria treatment: First time disclosure of the orally bioavailable clinical candidate GSK701. Accessed on 20/01/2025. Modified on 20/01/2025. 265th National Meeting of the American Chemical Society, Boston, MA, USA, American Chemical Society; 2018, https://www.morressier.com/o/event/5fc6413703137aa525805a17/article/5fc642112d78d1fec46581d0

References

1. Bopp S, Pasaje CFA, Summers RL, Magistrado-Coxen P, Schindler KA, Corpas-Lopez V, Yeo T, Mok S, Dey S, Smick S et al.. (2023)
Potent acyl-CoA synthetase 10 inhibitors kill Plasmodium falciparum by disrupting triglyceride formation.
Nat Commun, 14 (1): 1455. [PMID:36927839]

2. Castellote I, León ML, Hernando JI. (2019)
Novel compounds for the treatment of parasitic infections.
Patent number: WO2019145360A1. Assignee: Glaxosmithkline Intellectual Property Development Limited. Priority date: 23/01/2019. Publication date: 01/08/2019.

3. Kanai M, Hagenah LM, Ashley EA, Chibale K, Fidock DA. (2022)
Keystone Malaria Symposium 2022: a vibrant discussion of progress made and challenges ahead from drug discovery to treatment.
Trends Parasitol, 38 (9): 711-718. [PMID:35864072]

4. Rami H, Castellote I, Gamo FJ, Haselden J, Calderon Romo F.
Discovery of pyrrolidinamides, a novel chemical class for malaria treatment: First time disclosure of the orally bioavailable clinical candidate GSK701.
Accessed on 20/01/2025. Modified on 20/01/2025. 265th National Meeting of the American Chemical Society, Boston, MA, USA, American Chemical Society; 2018, https://www.morressier.com/o/event/5fc6413703137aa525805a17/article/5fc642112d78d1fec46581d0