基于JAK2/STAT3/PDL1通路研究白术内酯Ⅱ对肺癌小鼠细胞凋亡的影响

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中文摘要：通过观察白术内酯Ⅱ(atractylenolide Ⅱ,AT-Ⅱ)对Lewis肺癌小鼠JAK2/STAT3/PDL1通路的影响,探究其对小鼠肿瘤组织细胞凋亡的作用机制.建立肺癌小鼠模型,成瘤后,将小鼠随机分为4组,即模型组、白术内酯Ⅱ低、中、高剂量组,每组10只.白术内酯Ⅱ低、中、高剂量组灌胃0.2 mL白术内酯Ⅱ(剂量依次为25、50、100mg/kg),1次/d,模型组灌胃等体积溶剂,1次/d.各组连续干预21 d,末次给药后24 h,处死小鼠,分离肿瘤组织、脾组织.观察各组肿瘤体积随时间变化,计算脾指数、肿瘤生长抑制率;采用TUNEL荧光染色法观察各组肿瘤组织细胞凋亡情况;采用Western blot法测定肿瘤组织JAK2、p-JAK2、STAT3、p-STAT3、PDL1蛋白表达情况;免疫荧光法测定p-JAK2、p-STAT3、F4/80+、CD206+表达.于脾指数而言,给药组与模型组差异无统计学意义(P＞0.05);与模型组相比,白术内酯Ⅱ低、中、高剂量组的肿瘤体积、肿瘤质量显著减小(P＜0.05);肿瘤生长抑制率明显提高;TUNEL法荧光染色显示:与模型组相比,白术内酯Ⅱ低剂量组细胞凋亡指数差异无统计学意义(P＞0.05),白术内酯Ⅱ中剂量组细胞凋亡指数升高(P＜0.05),白术内酯Ⅱ高剂量组细胞凋亡指数显著升高(P＜0.01);Western blot实验结果显示:给药组肿瘤组织中p-JAK2、p-STAT3、PDL1蛋白的表达较模型组显著降低;免疫荧光实验测定p-JAK2、p-STAT3、CD206+给药组显著降低(P＜0.01)、F4/80+无显著差异(P＞0.05).以上实验结果表明AT-Ⅱ能够基于JAK2/STAT3通路调控PDL1表达,影响Lewis肺癌小鼠肿瘤组织细胞凋亡.

外文标题：Effect of whittenolactone Ⅱ on apoptosis of lung cancer mice based on JAK2/STAT3/PDL1 pathway

外文摘要：This study aims to investigate the effect of atractylenolide Ⅱ(AT-Ⅱ)on JAK2/STAT3/PDL1 pathway in Lewis lung cancer mice,and explore its mechanism on apoptosis of tumor cells in mice.The mice were randomly divided into four groups:model group,AT-Ⅱ low,middle and high dose groups(n=10 in each group).0.2 mL of AT-Ⅱ(25,50,100 mg/kg)was given intragastrically to the low,middle and high dose groups once a day,and the same volume of solvent was given intra-gastrically to the model group once a day.Twent-four hours after the last administration,the tumor tissues and spleen tissues were separated.The changes of tumor volume,spleen index and tumor growth inhibition rate were observed,and the apoptosis of tumor cells was observed by TUNEL fluorescence staining.The expression of JAK2,p-JAK2,STAT3,p-STAT3 and PDL1 protein was detected by Western blot,and the expression of p-JAK2,p-STAT3,F4/80+and CD206+was detected by immu-nofluorescence.There was no statistical difference of spleen index in each group(P＞0.05).Compared with the model group,the volume and quality of the tumor in the low,middle and high dose groups of atractylodes macrocephala were signifi-cantly decreased(P＜0.05),the growth inhibition rate was significantly increased,tunel staining showed that compared with the model group,there was no significant difference in apoptosis index in the low dose group(P＞0.05),but significantly in-creased in middle and high dose groups,the results of Western blot showed that the expression of p-JAK2,p-STAT3 and PDL1 in the tumor tissues of the treated group was significantly lower than that of the model group.The levels of p-JAK2,p-STAT3 and CD206+were significantly lower than those of the model group(P＜0.01),while the levels of F4/80+were not signifi-cantly different(P＞0.05).These results suggest that AT-Ⅱ can modulate the expression of PDL1 based on JAK2/STAT3 pathway and influence tumor cell apoptosis in Lewis lung cancer mice.

外文关键词：

Lewis lung cancer miceatractylolide ⅡPDL1 proteinapoptosis

作者：

赵云辉、蒋宗蓥、王艳杰

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作者单位：

辽宁中医药大学中西医结合学院,沈阳 110847

关键词：

Lewis肺癌小鼠白术内酯Ⅱ PDL1蛋白凋亡

基金：

国家自然科学基金青年基金辽宁省自然科学基金指导计划辽宁省教育厅一般项目

项目编号：

812027892019-ZD-0950LJKM20221311

出版年：

2024

DOI：

10.16333/j.1001-6880.2024.9.001

天然产物研究与开发

中国科学院成都文献情报中心

天然产物研究与开发

CSTPCD北大核心

影响因子：0.783

ISSN：1001-6880

年,卷(期)：2024.36(9)

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