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High-Affinity Cu(I)-Chelator with Potential Anti-Tumorigenic Action-A Proof-of-Principle Experimental Study of Human H460 Tumors in the CAM Assay. | LitMetric

AI Article Synopsis

  • Human lung cancer is a common cancer, and copper plays a key role in its growth, making copper removal a potential treatment strategy.
  • Researchers tested a new copper chelator, PSP-2, on H460 lung cancer cells using chicken embryo models, finding that it significantly reduced tumor weight and blood vessel density.
  • While low doses of PSP-2 showed promising results in decreasing tumor growth and specific cell markers, more research in various animal models is needed to confirm its effectiveness before moving to clinical trials.

Article Abstract

Human lung cancer ranks among the most frequently treated cancers worldwide. As copper appears critical to angiogenesis and tumor growth, selective removal of copper represents a promising strategy to restrict tumor growth. To this end, we explored the activity of the novel high-affinity membrane-permeant Cu(I) chelator PSP-2 featuring a low-zeptomolar dissociation constant. Using H460 human lung cancer cells, we generated small tumors on the chorioallantoic membrane of the chicken embryo (CAM assay) and studied the effects of topical PSP-2 application on their weight and vessel density after one week. We observed a significant angiosuppression along with a marked decrease in tumor weight under PSP-2 application compared to controls. Moreover, PSP-2 exposure resulted in lower ki67 cell numbers at a low dose but increased cell count under a high dose. Moreover, HIF-1α cells were significantly reduced with low-dose PSP-2 exposure compared to high-dose and control. The total copper content was considerably lower in PSP-2 treated tumors, although statistically not significant. Altogether, PSP-2 shows promising potential as an anti-cancer drug. Nevertheless, further animal experiments and application to different tumor types are mandatory to support these initial findings, paving the way toward clinical trials.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9600560PMC
http://dx.doi.org/10.3390/cancers14205122DOI Listing

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