Rongjuan Zhang , Xinhong Yang , Xiaomin Shi , Enhong Xing , Lihong Wang , Changlai Hao , Zhihua Zhang
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In MM cells treated with bortezomib, LC3B, Beclin-1, TFEB, and Lamp1 exhibited upregulation in a time- and concentration-dependent manner. LysoTracker dye labeling showed an increase in lysosomes in the bortezomib-treated group. Moreover, bortezomib elevated the expression of lysosome-associated factor Lamp1. Bortezomib promoted the nuclear translocation of TFEB, leading to decreased cytoplasmic TFEB and increased nuclear TFEB. TFEB gene silencing reversed bortezomib's inhibitory effect on MM cell lines, significantly reducing autophagosome expression and lysosome numbers. Furthermore, bioinformatic analysis identified the MAPK pathway as a potential downstream target of TFEB.</p></div><div><h3>Conclusion</h3><p>Bortezomib effectively inhibits MM cell proliferation and induces autophagy, partly through TFEB-mediated mechanisms, with potential involvement of the MAPK pathway.</p></div>","PeriodicalId":18051,"journal":{"name":"Leukemia research","volume":"138 ","pages":"Article 107455"},"PeriodicalIF":2.1000,"publicationDate":"2024-02-12","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":"{\"title\":\"Bortezomib modulated the autophagy-lysosomal pathway in a TFEB-dependent manner in multiple myeloma\",\"authors\":\"Rongjuan Zhang , Xinhong Yang , Xiaomin Shi , Enhong Xing , Lihong Wang , Changlai Hao , Zhihua Zhang\",\"doi\":\"10.1016/j.leukres.2024.107455\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<div><h3>Objective</h3><p>To explore the involvement of TFEB-mediated autophagy-lysosomal mechanisms in multiple myeloma (MM) during bortezomib treatment.</p></div><div><h3>Methods</h3><p>MM cells were exposed to bortezomib or subjected to TFEB knockdown. 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引用次数: 0
摘要
方法 将多发性骨髓瘤(MM)细胞暴露于硼替佐米或敲除 TFEB。采用 CCK 检测法评估细胞增殖情况。用 Western 印迹法和荧光染色法检测自噬和溶酶体。分析了 TFEB 的表达模式,并进行了全转录组测序。此外,还利用 GTRD(http://gtrd.biouml.org/) 网站预测了 TFEB 的靶基因,并进行了通路分析。结果硼替佐米对细胞增殖的抑制具有剂量依赖性和时间依赖性。在用硼替佐米处理的 MM 细胞中,LC3B、Beclin-1、TFEB 和 Lamp1 呈时间和浓度依赖性上调。溶酶体追踪染料标记显示,硼替佐米处理组的溶酶体有所增加。此外,硼替佐米还能提高溶酶体相关因子Lamp1的表达。硼替佐米促进了TFEB的核转位,导致细胞质中的TFEB减少,而细胞核中的TFEB增加。TFEB基因沉默可逆转硼替佐米对MM细胞株的抑制作用,显著减少自噬体的表达和溶酶体的数量。结论硼替佐米能有效抑制 MM 细胞增殖并诱导自噬,部分是通过 TFEB 介导的机制,MAPK 途径也可能参与其中。
Bortezomib modulated the autophagy-lysosomal pathway in a TFEB-dependent manner in multiple myeloma
Objective
To explore the involvement of TFEB-mediated autophagy-lysosomal mechanisms in multiple myeloma (MM) during bortezomib treatment.
Methods
MM cells were exposed to bortezomib or subjected to TFEB knockdown. CCK assay was used to assess the cell proliferation. Western blotting and fluorescent staining were conducted to examine autophagy and lysosomes. The TFEB expression pattern was analyzed, and whole transcriptome sequencing was carried out. Additionally, TFEB target genes were predicted using the GTRD(http://gtrd.biouml.org/) website, and pathway analysis was performed.
Results
Bortezomib demonstrated a dose-dependent and time dependent inhibition of cell proliferation. In MM cells treated with bortezomib, LC3B, Beclin-1, TFEB, and Lamp1 exhibited upregulation in a time- and concentration-dependent manner. LysoTracker dye labeling showed an increase in lysosomes in the bortezomib-treated group. Moreover, bortezomib elevated the expression of lysosome-associated factor Lamp1. Bortezomib promoted the nuclear translocation of TFEB, leading to decreased cytoplasmic TFEB and increased nuclear TFEB. TFEB gene silencing reversed bortezomib's inhibitory effect on MM cell lines, significantly reducing autophagosome expression and lysosome numbers. Furthermore, bioinformatic analysis identified the MAPK pathway as a potential downstream target of TFEB.
Conclusion
Bortezomib effectively inhibits MM cell proliferation and induces autophagy, partly through TFEB-mediated mechanisms, with potential involvement of the MAPK pathway.
期刊介绍:
Leukemia Research an international journal which brings comprehensive and current information to all health care professionals involved in basic and applied clinical research in hematological malignancies. The editors encourage the submission of articles relevant to hematological malignancies. The Journal scope includes reporting studies of cellular and molecular biology, genetics, immunology, epidemiology, clinical evaluation, and therapy of these diseases.