The Tuberculosis Drug Candidate SQ109 and Its Analogs Have Multistage Activity Against

Overview

Journal ACS Infect Dis

Specialties Infectious Diseases
Microbiology
Pharmacology

Date 2024 Aug 14

PMID 39143042

Authors

Savannah J Watson

Mariette E van der Watt

Anjo Theron

Janette Reader

Sizwe Tshabalala

Erica Erlank

Lizette L Koekemoer

Mariska Naude

Marianna Stampolaki

Feyisola Adewole

Katie Sadowska

Pilar Perez-Lozano

Andreea L Turcu

Santiago Vazquez

Jihee Ko

Ben Mazurek

Davinder Singh

Satish R Malwal

Mathew Njoroge

Kelly Chibale

Oluseye K Onajole

Antonios Kolocouris

Eric Oldfield

Lyn-Marie Birkholtz

Affiliations

Soon will be listed here.

Abstract

Toward repositioning the antitubercular clinical candidate SQ109 as an antimalarial, analogs were investigated for structure-activity relationships for activity against asexual blood stages of the human malaria parasite pathogenic forms, as well as transmissible, sexual stage gametocytes. We show that equipotent activity (IC) in the 100-300 nM range could be attained for both asexual and sexual stages, with the activity of most compounds retained against a multidrug-resistant strain. The multistage activity profile relies on high lipophilicity ascribed to the adamantane headgroup, and antiplasmodial activity is critically dependent on the diamine linker. Frontrunner compounds showed conserved activity against genetically diverse southern African clinical isolates. We additionally validated that this series could block transmission to mosquitoes, marking these compounds as novel chemotypes with multistage antiplasmodial activity.

Citing Articles

Activity of Carbazole, Aminoguanidine and Diamine Anti-infectives against .

Singh D, Sleda M, Pandey A, Malwal S, Chen Y, Zhou R bioRxiv. 2025; .

PMID: 39990502 PMC: 11844542. DOI: 10.1101/2025.02.15.638445.

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