Alshehri Afnan F, Khodier Ahmed E, Al-Gayyar Mohammed M
PharmD, University of Tabuk Faculty of Pharmacy, Tabuk, SAU.
Pharmacology, Horus University, Faculty of Pharmacy, New Damietta, EGY.
Cureus. 2023 Jun 16;15(6):e40499. doi: 10.7759/cureus.40499. eCollection 2023 Jun.
Background Cancer is the second-leading cause of death worldwide. According to a 2018 WHO report, 9.6 million deaths occurred globally due to cancer. Ehrlich carcinoma is characterized by rapid proliferation and a short survival time. Ligustilide is a phthalide derivative and is one of the main compounds in Danggui essential oil and . It has many protective effects, such as anticancer, anti-inflammatory, antioxidant, and neuroprotective effects. Aims We conducted this study to investigate the antitumor activity of ligustilide against Ehrlich solid carcinoma (ESC) in rats by affecting beclin 1, mammalian target of rapamycin (mTOR), B-cell lymphoma 2 (BCL2), and 5' AMP-activated protein kinase (AMPK). Materials and methods Twenty rats were intramuscularly implanted in the thigh of the left hind limb with a 200-µL tumor cell suspension in PBS containing 2 × 10 cells. After eight days of inoculation, 10 rats out of the 20 were treated with oral 20 mg/kg ligustilide daily. At the end of the experiment, samples of muscles with ESC were separated. Sections prepared from the muscle samples with ESC were immunohistochemically stained with anti-Ki67 antibodies. Another part of the muscle samples with ESC was used to assess gene expression and protein levels of beclin 1, mTOR, BCL2, and AMPK. Results Treatment of carcinoma rats with ligustilide elevated the mean survival time and reduced tumor volume and weight. Moreover, examination of tumor tissue stained with hematoxylin/eosin showed an infiltrative, highly cell-dense mass supported by a small to moderate amount of fibrovascular stroma and intersected with multifocal myofibril necrosis. Treatment with ligustilide ameliorated all these effects in the carcinoma group without affecting the control group. Finally, treatment with ligustilide significantly decreased the expression of beclin 1, mTOR, and AMPK associated with elevated expression of BCL2. Conclusions Our study aimed to explore the potential chemotherapeutic activity of ligustilide against ESC. We found that ligustilide effectively reduced tumor size and weight, indicating its antineoplastic activity against ESC. We further investigated that ligustilide inhibits cell proliferation by suppressing Ki67 and mTOR and activates autophagy through beclin 1 activation. Moreover, ligustilide inhibits apoptosis by upregulating BCL2. Finally, ligustilide reduced the expression of AMPK, preventing its ability to promote tumor cell growth.
背景
癌症是全球第二大死因。根据世界卫生组织2018年的一份报告,全球有960万人死于癌症。艾氏腹水癌具有增殖迅速和生存时间短的特点。藁本内酯是一种苯酞衍生物,是当归精油中的主要成分之一。它具有许多保护作用,如抗癌、抗炎、抗氧化和神经保护作用。
目的
我们进行这项研究是为了通过影响贝林1、雷帕霉素哺乳动物靶蛋白(mTOR)、B细胞淋巴瘤2(BCL2)和5'腺苷酸活化蛋白激酶(AMPK)来研究藁本内酯对大鼠艾氏实体癌(ESC)的抗肿瘤活性。
材料和方法
将20只大鼠左后肢大腿肌肉内注射200μL含2×10个细胞的PBS肿瘤细胞悬液。接种8天后,20只大鼠中的10只每天口服20mg/kg藁本内酯。实验结束时,分离出患有ESC的肌肉样本。用抗Ki67抗体对患有ESC的肌肉样本制备的切片进行免疫组织化学染色。另一部分患有ESC的肌肉样本用于评估贝林1、mTOR、BCL2和AMPK的基因表达和蛋白水平。
结果
用藁本内酯治疗癌大鼠可延长平均生存时间,减小肿瘤体积和重量。此外,苏木精/伊红染色的肿瘤组织检查显示,肿瘤为浸润性、细胞高度密集的肿块,由少量至中等量的纤维血管间质支持,并伴有多灶性肌原纤维坏死。藁本内酯治疗改善了癌组的所有这些效应,而对对照组无影响。最后,藁本内酯治疗显著降低了与BCL2表达升高相关的贝林1、mTOR和AMPK的表达。
结论
我们的研究旨在探索藁本内酯对ESC的潜在化疗活性。我们发现藁本内酯有效地减小了肿瘤大小和重量,表明其对ESC具有抗肿瘤活性。我们进一步研究发现,藁本内酯通过抑制Ki67和mTOR来抑制细胞增殖,并通过激活贝林1来激活自噬。此外,藁本内酯通过上调BCL2来抑制细胞凋亡。最后,藁本内酯降低了AMPK的表达,阻止了其促进肿瘤细胞生长的能力。
