Anticancer Effects of Eleven Triterpenoids Derived from Antrodia Camphorata

Overview

Journal Anticancer Res

Specialty Oncology

Date 2012 Jul 4

PMID 22753732

Citations 14

Authors

Yi-Pang Lee

Wan-Chi Tsai

Chih-Jan Ko

Yerra Koteswara Rao

Chiung-Ru Yang

Dar-Ren Chen

Ming-Hui Yang

Chi-Chiang Yang

Yew-Min Tzeng

Affiliations

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Abstract

Eleven derivatives from Antrodia camphorata were isolated in order to evaluate their selective cytotoxicity toward 14 types of human cancer cell and two non-transformed cell types. Among these triterpenoids, methyl antcinate A (MAA) exhibited the most potent spectrum of anticancer effects in KB cells, four different oral cancer cell lines (TSCCa, GNM, OC-2, and OEC-M1), Panc-1, BT474, PC-3, OVCAR-3, HeLa, and U2OS cells with high selectivity indices (CC(50)/IC(50)). The expression of B-cell lymphoma 2 (Bcl-2), Bcl-2-associated X protein (Bax), and poly(ADP-ribose) polymerase (PARP) of PC-3 cells tested by western blotting suggested that MAA exerts cell death through the caspase-dependent cascade and the Bax-mediated mitochondrial apoptotic pathway, not only on liver and oral cancer cells but on other types as well, including prostate cancer, in a dose-dependent manner. In addition to MAA, methyl antcinate B, dehydroeburicoic acid, and 15α-acetyl-dehydrosulfurenic acid also exhibited significant selective cytotoxic effects to respective cancer cells. Modifications of these triterpenoids may lead to the development of more potent anticancer drugs.

Citing Articles

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Antrodia cinnamomea induces anti-tumor activity by inhibiting the STAT3 signaling pathway in lung cancer cells.

Huang T, Lan Y, Chen C, Ko Y, Ojcius D, Martel J Sci Rep. 2019; 9(1):5145.

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