Preclinical Evaluation of Repurposed Antimalarial Artemisinins for the Treatment of Malignant Peripheral Nerve Sheath Tumors
Heather M. Duensing, Jalen M. Dixon, Owen R. Hunter, Nicolina C. Graves, Nickalus C. Smith, Andersen J. Tomes, Cale D. Fahrenholtz

TL;DR
This study explores using antimalarial artemisinins to treat MPNSTs by exploiting their ability to increase oxidative stress in tumor cells.
Contribution
The study demonstrates that artemisinin derivatives selectively kill MPNST cells through oxidative stress.
Findings
DHA and ARS are selectively cytotoxic to MPNST cells compared to normal Schwann cells.
DHA-induced cytotoxicity is mediated through oxidative stress and lipid peroxidation.
N-acetyl-cysteine can prevent DHA-mediated cytotoxicity in MPNST cells.
Abstract
Malignant peripheral nerve sheath tumors (MPNSTs) are a rare type of soft tissue sarcoma associated with poor prognoses. The standard of care for non-resectable tumors consists of surgical excision followed by radiation and chemotherapy. MPNSTs are most common in patients with neurofibromatosis type 1 but can also occur sporadically. Regardless of origin, MPNSTs most often rely on signaling pathways that increase basal oxidative stress. This provides the basis for developing therapeutics with mechanisms that can potentiate oxidative stress to selectively eradicate tumor cells at doses that are tolerable for normal cells. Artemisinin derivatives are a mainstay of malaria therapy worldwide, with a well-established safety profile. Artemisinin’s antimalarial effects are due to an endoperoxide bridge in its chemical structure that induces oxidative stress. We found that artesunate (ARS) and…
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Taxonomy
TopicsMultiple Myeloma Research and Treatments · Research on Leishmaniasis Studies · Protein Degradation and Inhibitors
