Abstract
BackgroundHerbal plants are a preferred source of anticancer agents. This study aims to screen the anticancer activity of a crude extract of twigs of (a) Bombax anceps Pierre var. anceps (BA); (b) Catunaregam tomentosa (Blume ex DC.) Tirveng. (CT); (c) Erythrophleum succirubrum Gagnep. (ES); (d) Lannea coromandelica (Houtt.) Merr. (LC); and (e) leaves and (f) twigs of Diospyros castanea (Craib) Fletcher (DC).MethodsThe 50 % ethanol–water extracts were prepared from each plant sample. In vitro anticancer effects of six extracts on the human hepatocellular carcinoma cell line (HepG2) in terms of cytotoxicity were investigated by neutral red assay, apoptosis induction by 4′,6-diamidino-2-phenylindole (DAPI) staining, and DNA fragmentation by agarose gel electrophoresis. Normal Vero cells were tested for comparison and to determine cancer selectivity. Gas chromatography–mass spectrometry analysis was performed to identify the compounds in the extracts.ResultsThe six crude extracts had different cytotoxicities and were classified into three groups based on their IC50 value and selectivity index (SI). DC (twig) crude extract had both a high cytotoxicity and SI toward HepG2 cells comparable to melphalan (P = 0.023). The crude extracts of DC (leaves), LC (twig), and BA (twig) had moderate cytotoxicity and a lower SI. Although all crude plant extracts induced apoptosis in more than 50 % of the DAPI-positive apoptotic HepG2 cells, only DC (twig) and LC (twig) showed laddering in the DNA fragmentation assay. 2-Palmitoylglycerol was the major compound common to both. Pyrogallol and lupeol were the major compounds in DC (twig) crude extract. Hexadecanoic acid and octadecenoic acid were the major compounds in LC (twig) crude extract, which had high toxicity but low selectivity.ConclusionEthanolic extracts from DC and LC twigs induced apoptosis in the HepG2 cell line. Pyrogallol and lupeol in DC (twig) might be responsible for the cytotoxicity toward the HepG2 cancer cells.
Highlights
Herbal plants are a preferred source of anticancer agents
Subsequent study was performed on the plants locally found in Thailand which were used in this study including Lannea coromandelica (Houtt.) Merr. (LC); Catunaregam tomentosa (Blume ex DC.) Tirveng. (CT); Erythrophleum succirubrum Gagnep (ES); Diospyros castanea (Craib) Fletcher (DC); and Bombax anceps Pierre var. anceps (BA)
The 50 % inhibitory concentration (IC50) and selectivity index (SI) of crude extract were demonstrated for the leaves of DC, twigs of DC, and LC
Summary
Herbal plants are a preferred source of anticancer agents. This study aims to screen the anticancer activity of a crude extract of twigs of (a) Bombax anceps Pierre var. anceps (BA); (b) Catunaregam tomentosa (Blume ex DC.) Tirveng. (CT); (c) Erythrophleum succirubrum Gagnep. (ES); (d) Lannea coromandelica (Houtt.) Merr. (LC); and (e) leaves and (f ) twigs of Diospyros castanea (Craib) Fletcher (DC). (CT); Erythrophleum succirubrum Gagnep (ES); Diospyros castanea (Craib) Fletcher (DC); and Bombax anceps Pierre var. CT belongs to the family Rubiaceae and has been used to treat diabetes mellitus, cancer, and tuberculosis. It possesses antimicrobial, antifungal, hypotensive, analgesic, antimalaria, antioxidant, and antileukemia pharmacological properties [19]. Plants in this family are active against many different diseases [21,22,23,24] (Table 1); the dichloromethane extract from the root of B. malabaricum is inactive in the human epidermoid carcinoma (KB) and human cervical carcinoma (HeLa) cell lines [25]
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