Biochanin A reduces pancreatic cancer survival and progression

Pancreatic cancer has dismally low mean survival rates worldwide. Only a few chemotherapeutic agents including gemcitabine have been shown to improve the survival of pancreatic cancer patients. Biochanin A, an isoflavone, is known to exert an anticancer effect on various cancer types. In this study,...

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Veröffentlicht in:	Anti-cancer drugs 2014-03, Vol.25 (3), p.296-302
Hauptverfasser:	Bhardwaj, Vikas, Tadinada, Satya Murthy, Jain, Aditi, Sehdev, Vikas, Daniels, Christopher K, Lai, James C.K, Bhushan, Alok
Format:	Artikel
Sprache:	eng
Schlagworte:	Antineoplastic Agents - pharmacology Apoptosis - drug effects Cell Line, Tumor - drug effects Cell Proliferation - drug effects Cell Survival - drug effects Genistein - pharmacology Humans Neoplasm Invasiveness Pancreatic Neoplasms - pathology Signal Transduction
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container_title	Anti-cancer drugs
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creator	Bhardwaj, Vikas Tadinada, Satya Murthy Jain, Aditi Sehdev, Vikas Daniels, Christopher K Lai, James C.K Bhushan, Alok
description	Pancreatic cancer has dismally low mean survival rates worldwide. Only a few chemotherapeutic agents including gemcitabine have been shown to improve the survival of pancreatic cancer patients. Biochanin A, an isoflavone, is known to exert an anticancer effect on various cancer types. In this study, we examined the anticancer properties of biochanin A on pancreatic cancer cells. The effect of biochanin A on cellular survival, apoptosis, and proliferation was analyzed using MTT, flow cytometry, and colony formation assay. The effect of biochanin A on pancreatic cancer’s mitogenic signaling was determined using western blot analysis. Migration assay and zymography were used to determine biochanin A’s effect on pancreatic cancer progression. Biochanin A induced dose-dependent toxicity on pancreatic cancer cells (Panc1 and AsPC-1). It reduced colony formation ability of Panc1 cells and induced dose-dependent apoptosis. Activation of Akt and MAPK was inhibited. Furthermore, the migratory and invasive potential of the cancer cells was also reduced. The results suggest that biochanin A is effective in reducing pancreatic cancer cell survival by inhibiting their proliferation and inducing apoptosis. It affects mitogenic, migratory, and invasive processes involved in cancer progression. These findings may lead to novel approaches to treat pancreatic cancer using isoflavones in combination with other therapeutic drugs.
doi_str_mv	10.1097/CAD.0000000000000044
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The results suggest that biochanin A is effective in reducing pancreatic cancer cell survival by inhibiting their proliferation and inducing apoptosis. It affects mitogenic, migratory, and invasive processes involved in cancer progression. 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Only a few chemotherapeutic agents including gemcitabine have been shown to improve the survival of pancreatic cancer patients. Biochanin A, an isoflavone, is known to exert an anticancer effect on various cancer types. In this study, we examined the anticancer properties of biochanin A on pancreatic cancer cells. The effect of biochanin A on cellular survival, apoptosis, and proliferation was analyzed using MTT, flow cytometry, and colony formation assay. The effect of biochanin A on pancreatic cancer’s mitogenic signaling was determined using western blot analysis. Migration assay and zymography were used to determine biochanin A’s effect on pancreatic cancer progression. Biochanin A induced dose-dependent toxicity on pancreatic cancer cells (Panc1 and AsPC-1). It reduced colony formation ability of Panc1 cells and induced dose-dependent apoptosis. Activation of Akt and MAPK was inhibited. Furthermore, the migratory and invasive potential of the cancer cells was also reduced. 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subjects	Antineoplastic Agents - pharmacology Apoptosis - drug effects Cell Line, Tumor - drug effects Cell Proliferation - drug effects Cell Survival - drug effects Genistein - pharmacology Humans Neoplasm Invasiveness Pancreatic Neoplasms - pathology Signal Transduction
title	Biochanin A reduces pancreatic cancer survival and progression
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