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首页|期刊导航|解放军医学杂志|甜菜碱抑制ABCB1逆转前列腺癌化疗耐药的作用及其机制

甜菜碱抑制ABCB1逆转前列腺癌化疗耐药的作用及其机制

李亚杰 张航 聂黎虹 安康杰 杨尉鑫 田国林 赵瑞宁

解放军医学杂志2025,Vol.50Issue(2):197-206,10.
解放军医学杂志2025,Vol.50Issue(2):197-206,10.DOI:10.11855/j.issn.0577-7402.1176.2024.0508

甜菜碱抑制ABCB1逆转前列腺癌化疗耐药的作用及其机制

Effect and mechanism of betaine in reversing ABCB1 transporter-mediated multidrug resistance in chemotherapy of prostate cancer

李亚杰 1张航 2聂黎虹 3安康杰 1杨尉鑫 3田国林 1赵瑞宁4

作者信息

  • 1. 宁夏医科大学总医院泌尿外科,宁夏 银川 750001
  • 2. 宁夏医科大学总医院泌尿外科,宁夏 银川 750001||巴中市中心医院泌尿外科,四川 巴中 636000
  • 3. 宁夏医科大学基础医学院,宁夏 银川 750001
  • 4. 宁夏医科大学总医院泌尿外科,宁夏 银川 750001||宁夏回族自治区人民医院泌尿外科,宁夏 银川 750001
  • 折叠

摘要

Abstract

Objective To investigate the effect and mechnism of betaine(BET)in reversing chemotherapy resistance in prostate cancer(PCa)by inhibiting ATP-binding cassette subfamily B member 1(ABCB1).Methods The PCa chemotherapy-sensitive C4-2B cells were cultured,and the TaxR cells resistant to docetaxel(DTX)were established by gradient increase the concentration of DTX.The drug resistance of C4-2B and TaxR cells against DTX was assessed using CCK-8 and the colony formation experiment.Western blotting and qRT-PCR were used to detect ABCB1 expression.The TaxR cells were divided into:(1)Control group,negative control group(NC),siABCB1-1 group(transfected with siABCB1-1),and siABCB1-2 group(transfected with siABCB1-2).Western blotting was used to detect the effect of small interfering RNA on silencing ABCB1,and CCK-8 was used to detect the differences in DTX resistance between each group.(2)Different concentrations of BET(0,100,200,400,600,800 mmol/L)groups.These groups were subjected to CCK-8 to detect cell viability,and Western blotting was used to detect the protein expression of ABCB1.(3)Control group,DTX group(20 nmol/L DTX),BET group(200 mmol/L BET),and DTX+BET group(20 nmol/L DTX+200 mmol/L BET),flow cytometry was used to detect apoptosis rate and cell cycle,and Western blotting to detect the protein expression of apoptosis-related proteins(Bcl2,BAX,c-caspase-3).(4)Control group,BET group(200 mmol/L BET),wortmannin(WM)group(100 μmol/L WM),and BET+WM group(200 mmol/L BET+100 μmol/L WM).Western blotting was used to detect the protein expression of PI3K,Akt,and ABCB1.(5)Control group,BET group(200 mmol/L BET),and BAY group(10 μmol/L BAY),BAY+BET group(200 mmol/L BET+10 μmol/L BAY).Western blotting was used to detect the protein expression of NF-κB p65,p-ikBα and ABCB1.Network pharmacology combined with transcriptome sequencing was used to predict the possible pathways for BET to reverse chemotherapy resistance.Results Compared with C4-2B cells,TaxR cells showed significantly increased resistance to DTX(P<0.01),and high expression of ABCB1(P<0.01).After silencing ABCB1 with siRNA,TaxR cells'resistance to DTX was significantly inhibited(P<0.01).The inhibition rate of TaxR cells treated with 200 mmol/L BET was less than 20%,and it significantly decreased the expression of ABCB1 protein in TaxR cells(P<0.05).Compared with control group,the combination of 200 mmol/L BET and 20 nmol/L DTX resulted in higher apoptosis rate and higher S stage cell ratio,lower expression of Bcl-2 protein and higher expression of BAX and c-caspase-3 proteins than the two drugs used alone(P<0.05).Compared with control group,the combination of 200 mmol/L BET and 100 μmol/L WM significantly down-regulated the protein expression of PI3K,Akt and ABCB1(P<0.01).The combination of 200 mmol/L BET and 10 μmol/L BAY significantly down-regulated the protein expression of NF-κB p65,p-ikBα and ABCB1(P<0.01).Conclusion BET may reverse TaxR cells'chemotherapy resistance by down-regulating ABCB1 expression through the PI3K/Akt/NF-κB signaling pathway.

关键词

甜菜碱/前列腺癌/化疗耐药/ABCB1

Key words

betaine/prostate cancer/chemotherapy resistance/ABCB1

分类

临床医学

引用本文复制引用

李亚杰,张航,聂黎虹,安康杰,杨尉鑫,田国林,赵瑞宁..甜菜碱抑制ABCB1逆转前列腺癌化疗耐药的作用及其机制[J].解放军医学杂志,2025,50(2):197-206,10.

基金项目

This work was supported by the Natural Science Foundation of Ningxia Hui Autonomous Region(2023AAC03668,2022AAC03506,2022AAC03160) 宁夏回族自治区自然科学基金(2023AAC03668,2022AAC03506,2022AAC03160) (2023AAC03668,2022AAC03506,2022AAC03160)

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