A series of 5-aryl-2-amino-
i
midazo
t
hia
d
iazole (ITD) derivatives
were identified by a phenotype-based high-throughput screening using
a blood stage
Plasmodium falciparum
(
Pf
) growth inhibition assay. A lead optimization program focused on
improving antiplasmodium potency, selectivity against human kinases,
and absorption, distribution, metabolism, excretion, and toxicity
properties and extended pharmacological profiles culminated in the
identification of
INE963
(
1
), which demonstrates
potent cellular activity against
Pf
3D7 (EC
50
= 0.006 μM) and achieves “artemisinin-like”
kill kinetics
in vitro
with a parasite clearance
time of <24 h. A single dose of 30 mg/kg is fully curative in the
Pf
-humanized severe combined immunodeficient mouse model.
INE963
(
1
) also exhibits a high barrier to resistance
in drug selection studies and a long half-life (
T
1/2
) across species. These properties suggest the significant
potential for
INE963
(
1
) to provide a curative
therapy for uncomplicated malaria with short dosing regimens. For
these reasons,
INE963
(
1
) was progressed
through GLP toxicology studies and is now undergoing Ph1 clinical
trials.
Abstract. The study of plagiarism and its detection is a highly popular field of research that has witnessed increased attention over recent years. In this paper we describe the range of problems that exist within academe in the area of 'unfair means', which encompasses a wider range of issues of attribution, ownership and originality. Unfair means offers a variety of problems that may benefit from the development of computational methods, thereby requiring appropriate evaluation resources. This may provide further areas of focus for large-scale evaluation activities, such as PAN, and researchers in the field more generally.
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