Molecules (Jan 2022)

Probable Mechanisms of Doxorubicin Antitumor Activity Enhancement by Ginsenoside Rh2

  • Alexander Popov,
  • Anna Klimovich,
  • Olga Styshova,
  • Alexander Tsybulsky,
  • Dmitry Hushpulian,
  • Andrey Osipyants,
  • Anna Khristichenko,
  • Sergey Kazakov,
  • Manuj Ahuja,
  • Navneet Kaidery,
  • Bobby Thomas,
  • Vladimir Tishkov,
  • Abraham Brown,
  • Irina Gazaryan,
  • Andrey Poloznikov

DOI
https://doi.org/10.3390/molecules27030628
Journal volume & issue
Vol. 27, no. 3
p. 628

Abstract

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Ginsenoside Rh2 increases the efficacy of doxorubicin (DOX) treatment in murine models of solid and ascites Ehrlich’s adenocarcinoma. In a solid tumor model (treatment commencing 7 days after inoculation), DOX + Rh2 co-treatment was significantly more efficacious than DOX alone. If treatment was started 24 h after inoculation, the inhibition of tumor growth of a solid tumor for the DOX + Rh2 co-treatment group was complete. Furthermore, survival in the ascites model was dramatically higher for the DOX + Rh2 co-treatment group than for DOX alone. Mechanisms underlying the combined DOX and Rh2 effects were studied in primary Ehrlich’s adenocarcinoma-derived cells and healthy mice’s splenocytes. Despite the previously established Rh2 pro-oxidant activity, DOX + Rh2 co-treatment revealed no increase in ROS compared to DOX treatment alone. However, DOX + Rh2 treatment was more effective in suppressing Ehrlich adenocarcinoma cell adhesion than either treatment alone. We hypothesize that the benefits of DOX + Rh2 combination treatment are due to the suppression of tumor cell attachment/invasion that might be effective in preventing metastatic spread of tumor cells. Ginsenoside Rh2 was found to be a modest activator in a Neh2-luc reporter assay, suggesting that Rh2 can activate the Nrf2-driven antioxidant program. Rh2-induced direct activation of Nrf2 might provide additional benefits by minimizing DOX toxicity towards non-cancerous cells.

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