Cynaropicrin inhibits pancreatic cancer cell viability and disrupts cellular redox homeostasis.

Leek HR; Oberhelman AL; Rew SR; Janss OM; Davidson CD

doi:10.17912/micropub.biology.002097

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Cynaropicrin inhibits pancreatic cancer cell viability and disrupts cellular redox homeostasis.

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microPublication biology 2026 Vol.2026()

Leek HR, Oberhelman AL, Rew SR, Janss OM, Davidson CD

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Pancreatic cancer accounts for approximately 8% of all cancer-related deaths.

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APA Leek HR, Oberhelman AL, et al. (2026). Cynaropicrin inhibits pancreatic cancer cell viability and disrupts cellular redox homeostasis.. microPublication biology, 2026. https://doi.org/10.17912/micropub.biology.002097

MLA Leek HR, et al.. "Cynaropicrin inhibits pancreatic cancer cell viability and disrupts cellular redox homeostasis.." microPublication biology, vol. 2026, 2026.

PMID 42021938

DOI 10.17912/micropub.biology.002097

Abstract

Pancreatic cancer accounts for approximately 8% of all cancer-related deaths. The compound cynaropicrin (CNP) has been investigated recently in several cancer models and has been shown to decrease cell viability. We used sulforhodamine B and trypan blue assays to measure cell viability following CNP treatment in PANC-1 cells. CNP reduced cell viability in a concentration-dependent manner (IC = 5.29 µM) and significantly decreased free thiol levels. Finally, docking demonstrated the potential for CNP to bind the DNA-binding domain of NF-κB. These data support further investigation of CNP as a potential therapeutic candidate in pancreatic cancer.