靛玉红及丹参酮Ⅱa促进雄黄降解突变型PML<sup>A216T</sup>-RARα的作用机制研究

李蕊白; 潘一鸣; 刘宇; 黄子明; 王玥; 陈凌燕; 马薇; 侯丽

doi:10.16025/j.1674-1307.2021.05.004

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靛玉红及丹参酮Ⅱa促进雄黄降解突变型PML^A216T-RARα的作用机制研究

专题——血液肿瘤的中医诊疗 | 更新时间：2023-04-10

- 靛玉红及丹参酮Ⅱa促进雄黄降解突变型PML^A216T-RARα的作用机制研究
- Mechanism of indirubin and tanshinone Ⅱa in promoting degradation of mutant PML^A216T-RARα by realgar
- 北京中医药 2021年40卷第5期页码：461-465
- 作者机构：
  
  1. 北京中医药大学东直门医院血液肿瘤科
  2. 温州医科大学检验医学院生命科学学院
- 作者简介：
- 基金信息：
  
  国家自然科学基金资助项目(82074240);国家重点研发计划项目(2016YFE0202800)
- DOI：10.16025/j.1674-1307.2021.05.004
  中图分类号：
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李蕊白, 潘一鸣, 刘宇, 等. 靛玉红及丹参酮Ⅱa促进雄黄降解突变型PML^A216T-RARα的作用机制研究[J]. 北京中医药, 2021,40(5):461-465.

LI Rui-bai, PAN Yi-ming, LIU Yu, et al. Mechanism of indirubin and tanshinone Ⅱa in promoting degradation of mutant PML^A216T-RARα by realgar[J]. Beijing Journal of Traditional Chinese Medicine, 2021,40(5):461-465.
李蕊白, 潘一鸣, 刘宇, 等. 靛玉红及丹参酮Ⅱa促进雄黄降解突变型PML^A216T-RARα的作用机制研究[J]. 北京中医药, 2021,40(5):461-465. DOI： 10.16025/j.1674-1307.2021.05.004.

LI Rui-bai, PAN Yi-ming, LIU Yu, et al. Mechanism of indirubin and tanshinone Ⅱa in promoting degradation of mutant PML^A216T-RARα by realgar[J]. Beijing Journal of Traditional Chinese Medicine, 2021,40(5):461-465. DOI： 10.16025/j.1674-1307.2021.05.004.

摘要

目的探讨靛玉红及丹参酮Ⅱa联用促进雄黄降解突变型PML,A216T,-RARα的作用机制。方法用不同浓度雄黄作用于野生型及突变型PML,A216T,-RARα,观察2组细胞PML-RARα降解作用,验证PML,A216T,-RARα存在砷剂耐药。根据CCK8测出的IC50值确定各组分浓度,使用不同浓度、不同组合的雄黄、靛玉红、丹参酮Ⅱa作用于转染PML,A216T,-RARα细胞,应用蛋白质印迹法检测单用、两两联合及三者联合对PML-RARα的降解及自噬相关因子（p-mTOR、LC3B）的作用。分别联用蛋白酶体抑制剂卡非佐米及自噬抑制剂巴佛洛霉素A1,应用蛋白质印迹法检测各组细胞中PML-RARα的降解情况。结果与对照组（不用药物干预）比较,雄黄浓度为0.5μmol/L,作用于PML-RARα野生型及突变型PML,A216T,-RARα时,均使PML-RARα发生了明显降解（均P ,<,0.01）,突变型PML,A216T,-RARα表达的PML-RARα均比野生型高（均P ,<,0.01）。与对照组比较,雄黄4μmol/L、靛玉红8μmol/L、丹参酮Ⅱa 8μmol/L作用于PML,A216T,-RARα时,均使PML-RARα发生降解（均P ,<,0.01）,可降低p-mTOR水平（均P ,<,0.01）,升高LC3B水平（P ,<,0.05,P ,<,0.01）,雄黄+丹参酮Ⅱa+靛玉红三者联合时上述作用最强（P ,<,0.01）。与对照组比较,雄黄+丹参酮Ⅱa+靛玉红、雄黄+丹参酮Ⅱa+靛玉红+卡非佐米联用作用于PML,A216T,-RARα时,均使PML-RARα发生明显降解（均P ,<,0.01）;与对照组比较,单用卡非佐米、单用巴佛洛霉素A1、雄黄+丹参酮Ⅱa+靛玉红+巴佛洛霉素A1,作用于PML,A216T,-RARα时,均使PML-RARα发生了明显蓄积,且雄黄+丹参酮Ⅱa+靛玉红+巴佛洛霉素A1组PML-RARα表达高于单用卡非佐米及单用巴佛洛霉素A1组（均P ,<,0.01）。结论靛玉红及丹参酮Ⅱa联用可通过自噬增强雄黄对突变型PML,A216T,-RARα的降解作用,三者联用自噬作用最强,可能为复方黄黛片治疗急性早幼粒细胞白血病的作用机制之一。

Abstract

Objective To explore the mechanism of Indirubin and tanshinone Ⅱa in promoting the degradation of mutant PML,A216T,RARα by realgar.Methods Different concentrations of realgar were acted on wild type and mutant PML,A216T,-RARα to observe the degradation of PML-RARα in two groups of cells to verify that PML,A216T,-RARα is resistant to arsenic.The concentration of each component was determined according to the IC50 value measured by CCK8,and different concentrations and different combinations of realgar,indirubin,and tanshinone Ⅱa were used to act on the transfected PML,A216T,-RARα cells.Western blotting was used to detect the effects of single use,pairwise combination and triple combination on PML-RARα degradation and autophagy-related factors（ pm TOR,LC3 B）.The proteasome inhibitor carfilzomib and the autophagy inhibitor bafilomycin A1 were used to detect the degradation of PML-RARα in each group of cells by Western blotting.Results Compared with the control group（ without drug intervention）,when the concentration of realgar was 0.5 μmol/L,which was acted on PML-RARα wild type and mutant PML,A216T,-RARα,the expression of PML-RARα were significantly degra ded（ both P ,<, 0.01）.Moreover,the comparison between the groups showed that the expression of PML-RARα of mutant PML,A216T,-RARα was higher than that of wild type（ all P ,<, 0.01）.Compared with the control group,when realgar was 4 μmol/L,indirubin was 8 μmol/L,and tanshinone Ⅱa was 8 μmol/L,and were acted on PML,A216T,-RARα respetively,they could all degrade PML-RARα（ all P ,<, 0.01） and reduce the level of p-mTOR（ all P ,<, 0.01）,increase the level of LC3 B（ P ,<, 0.05 or P ,<, 0.01）.The above effect was the strongest when realgar + tanshinone Ⅱa + indirubin was combined（ P ,<, 0.01）.Compared with the control group,when realgar + tanshinone Ⅱa + indirubin,realgar + tanshinone Ⅱa + indirubin + carfilzomib were used on PML,A216T,RARα,PML-RARα were significantly degraded（ all P ,<, 0.01）.Compared with the control group,carfilzomib alone,bafilomycin A1 alone,realgar + tanshinone Ⅱa + indirubin + bafilomycin A1,when acting on PML,A216T,-RARα,all caused PML-RARα to a significant accumulation,and the expression of PML-RARα in the realgar + tanshinone Ⅱa + indirubin + bafilomycin A1 group was higher than that in the carfilzomib alone and bafilomycin A1 group（ all P ,<, 0.01）.Conclusion The combination of indirubin and tanshinone Ⅱa can enhance the degradation effect of realgar on mutant PML,A216T,-RARα through autophagy,and the combination of the three has the strongest autophagy effect,which may be one of the mechanisms of Chinese medicinal formula Realgar-Indigo naturalis in the treatment of acute promyelocytic leukemia.

关键词

雄黄靛玉红丹参酮Ⅱa急性髓细胞性白血病自噬PML-RARα基因突变蛋白降解

Keywords

Realgarindirubintanshinone Ⅱaacute myeloid leukemiaautophagyPML-RARαgene mutationprotein degradation

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靛玉红及丹参酮Ⅱa促进雄黄降解突变型PMLA216T-RARα的作用机制研究

Mechanism of indirubin and tanshinone Ⅱa in promoting degradation of mutant PMLA216T-RARα by realgar

DOI：10.16025/j.1674-1307.2021.05.004

摘要

Abstract

关键词

Keywords

references

靛玉红及丹参酮Ⅱa促进雄黄降解突变型PML^A216T-RARα的作用机制研究

Mechanism of indirubin and tanshinone Ⅱa in promoting degradation of mutant PML^A216T-RARα by realgar