Mycolactone: A Broad Spectrum Multitarget Antiviral Active in the Picomolar Range for COVID-19 Prevention and Cure
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International Journal of Molecular Sciences
Abstract
We have previously shown computationally that Mycolactone (MLN), a toxin produced
by Mycobacterium ulcerans, strongly binds to Munc18b and other proteins, presumably blocking
degranulation and exocytosis of blood platelets and mast cells. We investigated the effect of MLN
on endocytosis using similar approaches, and it bound strongly to the N-terminal of the clathrin
protein and a novel SARS-CoV-2 fusion protein. Experimentally, we found 100% inhibition up to
60 nM and 84% average inhibition at 30 nM in SARS-CoV-2 live viral assays. MLN was also 10×
more potent than remdesivir and molnupiravir. MLN’s toxicity against human alveolar cell line A549,
immortalized human fetal renal cell line HEK293, and human hepatoma cell line Huh7.1 were 17.12%,
40.30%, and 36.25%, respectively. The cytotoxicity IC50 breakpoint ratio versus anti-SARS-CoV-2
activity was more than 65-fold. The IC50 values against the alpha, delta, and Omicron variants were
all below 0.020 µM, and 134.6 nM of MLN had 100% inhibition in an entry and spread assays. MLN
is eclectic in its actions through its binding to Sec61, AT2R, and the novel fusion protein, making
it a good drug candidate for treating and preventing COVID-19 and other similarly transmitted
enveloped viruses and pathogens.
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Citation: Asiedu, S.O.; Gupta, Y.; Nicolaescu, V.; Gula, H.; Caulfield, T.R.; Durvasula, R.; Kempaiah, P.; Kwofie, S.K.; Wilson, M.D. Mycolactone: A Broad Spectrum Multitarget Antiviral Active in the Picomolar Range for COVID-19 Prevention and Cure. Int. J. Mol. Sci. 2023, 24, 7151. https://doi.org/ 10.3390/ijms24087151