Broussoflavonol F exhibited anti-proliferative and anti-angiogenesis effects in colon cancer via modulation of the HER2-RAS-MEK-ERK pathway.

IF 6.7 1区 医学 Q1 CHEMISTRY, MEDICINAL
Phytomedicine Pub Date : 2024-12-01 Epub Date: 2024-11-09 DOI:10.1016/j.phymed.2024.156243
Yiying Zhu, Xiaoli Li, Grace Gar-Lee Yue, Julia Kin-Ming Lee, Si Gao, Mengru Wang, Chun Kwok Wong, Wei-Lie Xiao, Clara Bik-San Lau
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引用次数: 0

Abstract

Background: A prenylated flavonoid, broussoflavonol F (BFF), was isolated from Macaranga genus with cytotoxicities against various cancer cells, though its underlying mechanisms have not been fully elucidated.

Hypothesis: This study aimed to investigate the anti-tumor and anti-angiogenesis activities of BFF and its underlying mechanisms in colon cancer.

Method: In the in vitro study, the cytotoxic effects of BFF in human colon cancer HCT-116 and LoVo cells were examined using MTT assay, BrdU assay and colony formation assay. The anti-proliferative effects of BFF in these cells were assessed via cell apoptosis and cell cycle analysis using flow cytometry. The anti-angiogenesis effects of BFF in human endothelial HEMC-1 cells were also detected using scratch wound healing assay and tube formation assay. While the in vivo effects of BFF in colon cancer were further examined in zebrafish embryos and HCT116 tumor-bearing mice. The underlying mechanisms of BFF were predicted using network pharmacology analysis, and Western blotting was performed to validate both in vitro and in vivo results.

Results: BFF exhibited cytotoxicities on 5 colon cancer cell lines, as well as anti-proliferative activities via inducing apoptosis and cell cycle arrest at the G0/G1 phase in HCT116 and LoVo cells. BFF at 1.25-5 µM also suppressed cell proliferation in these two colon cancer cell lines by downregulating HER2, RAS, p-BRAF, p-MEK and p-Erk protein expressions. In addition, BFF at 2.5-5 µM could significantly decrease the length of subintestinal vessels of zebrafish embryos through decreasing mRNA expressions of NRP1a, PDGFba, PDGFRb, KDR, FLT1 and VEGRaa. Besides, BFF exhibited anti-angiogenesis activity via inhibiting cell proliferation, motility and tube formation in HMEC-1 cells. Furthermore, intraperitoneal administration of BFF (10 mg/kg) suppressed tumor growth and decreased the expression of tumor proliferation marker Ki-67 and angiogenesis marker CD31 in the tumor tissues in HCT116 tumor-bearing mice. BFF treatment could also significantly decrease expressions of RAS, p-BRAF, p-MEK and p-Erk in the tumor section, which are consistent with the in vitro results.

Conclusions: This study revealed the anti-tumor and anti-angiogenesis effects of BFF in colon cancer. This is the first report of the in vitro and in vivo anti-proliferative activity of BFF in colon cancer through regulating the HER2-RAS-MEK-ERK pathway. These findings further support the research development of BFF as an anti-cancer agent in colon cancer.

Broussoflavonol F通过调节HER2-RAS-MEK-ERK通路对结肠癌具有抗增殖和抗血管生成作用。
背景:从Macaranga属植物中分离出一种前烯基黄酮类化合物--broussoflavonol F(BFF),对多种癌细胞具有细胞毒性,但其潜在机制尚未完全阐明:本研究旨在探讨 BFF 在结肠癌中的抗肿瘤和抗血管生成活性及其内在机制:在体外研究中,采用MTT试验、BrdU试验和集落形成试验检测了BFF对人结肠癌HCT-116和LoVo细胞的细胞毒作用。使用流式细胞仪通过细胞凋亡和细胞周期分析评估了 BFF 对这些细胞的抗增殖作用。此外,还使用划痕伤口愈合试验和管形成试验检测了 BFF 在人内皮 HEMC-1 细胞中的抗血管生成作用。在斑马鱼胚胎和 HCT116 肿瘤小鼠体内进一步研究了 BFF 对结肠癌的体内作用。利用网络药理学分析预测了 BFF 的内在机制,并进行了 Western 印迹分析以验证体外和体内结果:结果:BFF对5种结肠癌细胞株具有细胞毒性,并通过诱导HCT116和LoVo细胞凋亡和细胞周期停滞在G0/G1期而具有抗增殖活性。浓度为 1.25-5 µM 的 BFF 还能通过下调 HER2、RAS、p-BRAF、p-MEK 和 p-Erk 蛋白表达,抑制这两种结肠癌细胞系的细胞增殖。此外,2.5-5 µM 的 BFF 还能通过降低 NRP1a、PDGFba、PDGFRb、KDR、FLT1 和 VEGRaa 的 mRNA 表达,显著减少斑马鱼胚胎肠下血管的长度。此外,BFF 还通过抑制 HMEC-1 细胞的增殖、运动和管形成,表现出抗血管生成活性。此外,腹腔注射 BFF(10 mg/kg)可抑制 HCT116 肿瘤小鼠的肿瘤生长,降低肿瘤组织中肿瘤增殖标志物 Ki-67 和血管生成标志物 CD31 的表达。BFF还能显著降低肿瘤切片中RAS、p-BRAF、p-MEK和p-Erk的表达,与体外实验结果一致:本研究揭示了 BFF 在结肠癌中的抗肿瘤和抗血管生成作用。这是首次报道 BFF 通过调节 HER2-RAS-MEK-ERK 通路对结肠癌具有体外和体内抗增殖活性。这些发现进一步支持了 BFF 作为结肠癌抗癌剂的研究发展。
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来源期刊
Phytomedicine
Phytomedicine 医学-药学
CiteScore
10.30
自引率
5.10%
发文量
670
审稿时长
91 days
期刊介绍: Phytomedicine is a therapy-oriented journal that publishes innovative studies on the efficacy, safety, quality, and mechanisms of action of specified plant extracts, phytopharmaceuticals, and their isolated constituents. This includes clinical, pharmacological, pharmacokinetic, and toxicological studies of herbal medicinal products, preparations, and purified compounds with defined and consistent quality, ensuring reproducible pharmacological activity. Founded in 1994, Phytomedicine aims to focus and stimulate research in this field and establish internationally accepted scientific standards for pharmacological studies, proof of clinical efficacy, and safety of phytomedicines.
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