HECTD2 as a target for veratric acid in the regulation of ferroptosis in renal cell carcinoma

IF 3 3区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY
Dong Lv, Ying Xiang, Tao Song, Jinze Li, Yongbo Chen, Youlong Huili, Taimin Shen
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Abstract

Function of HECTD2 in renal cell carcinoma malignant progression is undefined. Molecular mechanism behind anti-cancer effects of veratric acid (VA) from traditional Chinese medicine (TCM) is underexplored. The Cancer Genome Atlas was leveraged to study HECTD2 expression in renal cell carcinoma and its relationship with histological grading. Kaplan–Meier survival analysis was performed. HECTD2 expression was detected in cancer cells and tissues via qRT-PCR and immunohistochemistry. GPX4 and SLC7A11 expression in tumor samples with high or low HECTD2 expression was examined by immunohistochemistry, cell viability by CCK8, cell proliferation by colony formation assay, lipid ROS and mitochondrial superoxide levels by flow cytometry, Fe2+ and MDA content by assay kits, and GPX4 and SLC7A11 proteins by western blot. SeeSAR software screened TCM small molecule compounds with highest affinity to HECTD2, confirmed with cellular thermal shift assay. VA IC50 was measured by CCK8. Xenograft model was developed and treated with VA. Tumor size and weight were monitored, with immunohistochemistry to detect HECTD2 expression in tumors and assess ferroptosis-related markers. HECTD2 was overexpressed in tumor tissues and cells, which positively correlated with histological grading. HECTD2 depletion inhibited cell vitality and proliferation, raised intracellular lipid ROS, mitochondrial superoxide, Fe2+, and MDA. HECTD2 was a target with highest VA affinity. In vitro and vivo experiments concurred that VA treatment hindered malignancy of renal cell carcinoma and enhanced its susceptibility to ferroptosis. HECTD2 supports ferroptosis resistance in renal cell carcinoma, but VA, through its targeting of HECTD2, initiates ferroptosis, showcasing its anti-cancer efficacy.

HECTD2是藜芦酸调控肾细胞癌铁蛋白沉积的靶点
HECTD2在肾细胞癌恶性进展中的功能尚未明确。中药藜芦酸(VA)抗癌作用背后的分子机制尚未得到充分探索。我们利用癌症基因组图谱研究了肾细胞癌中HECTD2的表达及其与组织学分级的关系。研究还进行了Kaplan-Meier生存分析。通过 qRT-PCR 和免疫组化技术检测了癌细胞和组织中 HECTD2 的表达。通过免疫组化检测了HECTD2高表达或低表达的肿瘤样本中GPX4和SLC7A11的表达情况,通过CCK8检测了细胞活力,通过集落形成试验检测了细胞增殖,通过流式细胞术检测了脂质ROS和线粒体超氧化物水平,通过检测试剂盒检测了Fe2+和MDA含量,通过Western印迹检测了GPX4和SLC7A11蛋白。SeeSAR 软件筛选出了与 HECTD2 亲和力最高的中药小分子化合物,并通过细胞热转移试验进行了确认。用 CCK8 测定 VA IC50。建立异种移植模型并用 VA 治疗。用免疫组化法检测肿瘤中 HECTD2 的表达,并评估铁突变相关标记物。HECTD2在肿瘤组织和细胞中过表达,与组织学分级呈正相关。消耗 HECTD2 可抑制细胞活力和增殖,提高细胞内脂质 ROS、线粒体超氧化物、Fe2+ 和 MDA。HECTD2是VA亲和力最高的靶标。体外和体内实验一致表明,VA 治疗阻碍了肾细胞癌的恶性发展,并增强了其对铁变态反应的敏感性。HECTD2支持肾细胞癌的铁变态反应抗性,但VA通过靶向HECTD2启动了铁变态反应,从而显示了其抗癌功效。
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来源期刊
Amino Acids
Amino Acids 生物-生化与分子生物学
CiteScore
6.40
自引率
5.70%
发文量
99
审稿时长
2.2 months
期刊介绍: Amino Acids publishes contributions from all fields of amino acid and protein research: analysis, separation, synthesis, biosynthesis, cross linking amino acids, racemization/enantiomers, modification of amino acids as phosphorylation, methylation, acetylation, glycosylation and nonenzymatic glycosylation, new roles for amino acids in physiology and pathophysiology, biology, amino acid analogues and derivatives, polyamines, radiated amino acids, peptides, stable isotopes and isotopes of amino acids. Applications in medicine, food chemistry, nutrition, gastroenterology, nephrology, neurochemistry, pharmacology, excitatory amino acids are just some of the topics covered. Fields of interest include: Biochemistry, food chemistry, nutrition, neurology, psychiatry, pharmacology, nephrology, gastroenterology, microbiology
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