2018
DOI: 10.1016/j.trsl.2018.04.007
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The proteasome as a target to combat malaria: hits and misses

Abstract: The proteasome plays a vital role throughout the life cycle as Plasmodium parasites quickly adapt to a new host and undergo a series of morphologic changes during asexual replication and sexual differentiation. Plasmodium carries 3 different types of protease complexes: typical eukaryotic proteasome (26S) that resides in the cytoplasm and the nucleus, a prokaryotic proteasome homolog ClpQ that resides in the mitochondria, and a caseinolytic protease complex ClpP that resides in the apicoplast. In silico predic… Show more

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Cited by 32 publications
(24 citation statements)
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“…5A). Also, HS-Sensitive mutants shared an increased sensitivity to the proteasome inhibitor BTZ, consistent with laboratory observations connecting artemisinin MOA to the proteasome and clinical data that proteasome-inhibitors act synergistically with artemisinins 8, 19,20,21 . Overall, correlation of mutant phenotypic profiles across screens varied, with 16-45% having correlating phenotypes in at least one additional screen (Fig.…”
Section: Resultssupporting
confidence: 84%
“…5A). Also, HS-Sensitive mutants shared an increased sensitivity to the proteasome inhibitor BTZ, consistent with laboratory observations connecting artemisinin MOA to the proteasome and clinical data that proteasome-inhibitors act synergistically with artemisinins 8, 19,20,21 . Overall, correlation of mutant phenotypic profiles across screens varied, with 16-45% having correlating phenotypes in at least one additional screen (Fig.…”
Section: Resultssupporting
confidence: 84%
“…Another interesting clinical application of proteasome inhibition is in the treatment of malaria [232][233][234][235]. Malaria parasites contain their own form of the 26S proteasome in the cytoplasm and nucleus.…”
Section: Other Indications For Proteasome Inhibitorsmentioning
confidence: 99%
“…A bioassay that tested 20 antimalarial drugs with a sex-specific readout reported increased sensitivity of male gametocytes to thiostrepton [ 130 ]. These studies suggest growing evidence of mitochondrial metabolism and proteasome pathways as emerging drug targets that hold the key for the development of novel transmission-blocking chemotherapeutic interventions [ 162 , 163 , 164 ]. Additionally, natural products from plant and microbial origins are being extensively investigated for the discovery of new antimalarial compounds [ 165 ].…”
Section: Antimalarial Drug Therapies and Gametocytesmentioning
confidence: 99%