Antileishmanial Chemotherapy through Clemastine Fumarate
Mediated Inhibition of the Leishmania Inositol Phosphorylceramide
Synthase
Posted on 2020-12-09 - 02:14
Current
chemotherapeutics for leishmaniasis have multiple deficiencies,
and there is a need for new safe, efficacious, and affordable medicines.
This study describes a successful drug repurposing approach that identifies
the over-the-counter antihistamine, clemastine fumarate, as a potential
antileishmanial drug candidate. The screening for inhibitors of the
sphingolipid synthase (inositol phosphorylceramide synthase, IPCS)
afforded, following secondary screening against Leishmania
major (Lmj) promastigotes, 16 active compounds. Further refinement
through the dose response against LmjIPCS and intramacrophage L. major amastigotes identified clemastine fumarate
with good activity and selectivity with respect to the host macrophage.
On target engagement was supported by diminished sensitivity in a
sphingolipid-deficient L. major mutant (ΔLmjLCB2) and altered phospholipid and sphingolipid profiles
upon treatment with clemastine fumarate. The drug also induced an
enhanced host cell response to infection indicative of polypharmacology.
The activity was sustained across a panel of Old and New World Leishmania species, displaying an in vivo activity equivalent to the currently used drug, glucantime, in a
mouse model of L. amazonensis infection. Overall,
these data validate IPCS as an antileishmanial drug target and indicate
that clemastine fumarate is a candidate for repurposing for the treatment
of leishmaniasis.
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Mina, John G.
M.; Charlton, Rebecca L.; Alpizar-Sosa, Edubiel; Escrivani, Douglas O.; Brown, Christopher; Alqaisi, Amjed; et al. (2020). Antileishmanial Chemotherapy through Clemastine Fumarate
Mediated Inhibition of the Leishmania Inositol Phosphorylceramide
Synthase. ACS Publications. Collection. https://doi.org/10.1021/acsinfecdis.0c00546