The use of computational
tools to identify biological targets of
natural products with anticancer properties and unknown modes of action
is gaining momentum. We employed self-organizing maps to deconvolute
the phenotypic effects of piperlongumine (PL) and establish a link
to modulation of the human transient receptor potential vanilloid
2 (hTRPV2) channel. The structure of the PL-bound full-length rat
TRPV2 channel was determined by cryo-EM. PL binds to a transient allosteric
pocket responsible for a new mode of anticancer activity against glioblastoma
(GBM) in which hTRPV2 is overexpressed. Calcium imaging experiments
revealed the importance of Arg539 and Thr522 residues on the antagonistic
effect of PL and calcium influx modulation of the TRPV2 channel. Downregulation
of hTRPV2 reduces sensitivity to PL and decreases ROS production.
Analysis of GBM patient samples associates hTRPV2 overexpression with
tumor grade, disease progression, and poor prognosis. Extensive tumor
abrogation and long term survival was achieved in two murine models
of orthotopic GBM by formulating PL in an implantable scaffold/hydrogel
for sustained local therapy. Furthermore, in primary tumor samples
derived from GBM patients, we observed a selective reduction of malignant
cells in response to PL
ex vivo
. Our results establish
a broadly applicable strategy, leveraging data-motivated research
hypotheses for the discovery of novel means tackling cancer.
The use of computational tools to identify biological targets of natural products with anticancer properties and unknown modes of action is gaining momentum. We employed self-organizing maps to deconvolute the phenotypic effects of Piperlongumine (PL) and establish a link to modulation of the human transient receptor potential vanilloid 2 (hTRPV2) channel. The structure of the PL-bound full-length rat TRPV2 channel was determined by cryo-EM. PL binds to a transient allosteric pocket responsible for a new mode of anticancer activity against glioblastoma (GBM) in which hTRPV2 is overexpressed. Calcium imaging experiments revealed the importance of Arg539 and Thr522 residues on the antagonistic effect of PL and calcium influx modulation of the TRPV2 channel. Down-regulation of hTRPV2 reduces sensitivity to PL and decreases ROS production. Analysis of GBM patient samples associates hTRPV2 overexpression with tumour grade, disease progression and poor prognosis. PL formulation for sustained local therapy using an implantable scaffold/hydrogel yielded extensive tumour abrogation in two murine models of orthotopic GBM by formulating PL for sustained local therapy using an implantable scaffold/hydrogel, together with long-term survival of treated animals. Furthermore, in primary tumour samples derived from GBM patients, we observed a selective reduction of malignant cells in response to PL ex vivo. Our data establish a broadly applicable strategy, leveraging data-motivated research hypotheses for the discovery of novel therapeutic vulnerabilities.
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