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三种灵芝甲醇提取物的体外抗肿瘤作用

In vitro antitumor effects of methanolic extracts of three Ganoderema mushrooms.

作者信息

Toson Elshahat A, El-Fallal Amira A, Oransa Marwa A, El-Gharabawy Hoda M

机构信息

Chemistry Department, Faculty of Science, Damietta University, New Damietta, 34517, Egypt.

Botany and Microbiology Department, Faculty of Science, Damietta University, New Damietta, 34517, Egypt.

出版信息

Sci Rep. 2025 Jan 17;15(1):2274. doi: 10.1038/s41598-025-86162-0.

Abstract

Ganoderma mushrooms have a variety of pharmacological activities and may have antitumor effects. Therefore, the antitumor activity of the methanolic fruiting body extracts of three Ganoderma spp. will be evaluated by estimating cell viability, cell cycle parameters and the mode of cellular death. In this regard, Sulfo-rhodamine B staining and flow cytometry were used. Hepatocellular carcinoma (HepG2) and breast ductal carcinoma (T-47D) cell lines were used as cancer models, while mouse normal liver (BNL) and oral epithelial cell (OEC) lines were used as respective controls. The results revealed that Ganoderma resinaceum extract decreased the viability of BNL at an IC > 100 µg/mL but not that of HepG2 at an IC of 72.32 µg/mL. Additionally, Ganoderma australe and Ganoderma mbrekobenum decreased the viability of OEC cell line at an IC of 328.29 and 271.56 µg/ mL, respectively. On the other hand, the IC of T-47D were 221.95 and 236.45 µg/mL, respectively. The three extracts arrested the cell life cycle at the G1 phase in each case. G. resinaceum extract stimulated total apoptosis (Q2 + Q4) of 19.99% with low necrosis (Q1). However, the percentages of total cell necrosis in the T-47D cell line treated with the other two extracts were 31.10% and 18.28%, respectively while the percentages of total cell apoptosis were 6.83% and 1.78%, respectively. Thus, G. resinaceum significantly inhibited the viability of the HepG2 cell line, while both the G. australe and G. mbrekobenum extracts significantly decreased the viability of the T-47D cell line. These results may encourage speculation about their possible use for the therapeutic management of hepatocellular carcinoma and breast ductal carcinoma after further investigation.

摘要

灵芝具有多种药理活性,可能具有抗肿瘤作用。因此,将通过评估细胞活力、细胞周期参数和细胞死亡方式来评价三种灵芝子实体甲醇提取物的抗肿瘤活性。在这方面,使用了磺基罗丹明B染色和流式细胞术。肝癌(HepG2)和乳腺导管癌(T-47D)细胞系用作癌症模型,而小鼠正常肝细胞(BNL)和口腔上皮细胞(OEC)系分别用作对照。结果显示,树舌灵芝提取物在IC>100μg/mL时降低了BNL的活力,但在IC为72.32μg/mL时对HepG2的活力没有影响。此外,南方灵芝和mbrekobenum灵芝分别在IC为328.29和271.56μg/mL时降低了OEC细胞系的活力。另一方面,T-47D的IC分别为221.95和236.45μg/mL。三种提取物在每种情况下均使细胞生命周期停滞在G1期。树舌灵芝提取物刺激总凋亡率(Q2+Q4)为19.99%,坏死率低(Q1)。然而,用其他两种提取物处理的T-47D细胞系中,总细胞坏死率分别为31.10%和18.28%,而总细胞凋亡率分别为6.83%和1.78%。因此,树舌灵芝显著抑制了HepG2细胞系的活力,而南方灵芝和mbrekobenum灵芝提取物均显著降低了T-47D细胞系的活力。这些结果可能会促使人们在进一步研究后推测它们在肝细胞癌和乳腺导管癌治疗管理中的可能用途。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7b3b/11748650/0b30f9c1ba43/41598_2025_86162_Fig1_HTML.jpg

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