miR-9-5p通过靶向UBE4B调节缺氧诱导转录因子1α泛素化介导瓦博格效应在胶质瘤细胞中的应用

目的探讨miR-9-5p在胶质瘤中对瓦博格效应的调控作用及机制情况。方法选择新疆医科大学第二附属医院2018年5月至2020年10月确诊的30例神经胶质瘤和癌旁组织样品。设立对照组、miR-9-5p过表达组及miR-9-5p抑制剂组,采用实时荧光定量PCR分别检测miR-9-5p的表达情况及其与糖酵解相关基因表达的相关性。构建异位肿瘤模型及体外细胞实验,采用实时荧光定量PCR、蛋白质印迹法、葡萄糖摄取分析、乳酸产生量检测及细胞活力检测判断miR-9-5p对胶质瘤及瓦博格效应的影响情况,采用双荧光素酶报告基因检测miR-9-5p与UBE4B的靶向性关系。结果miR-9-5p过表达组缺氧诱导转录因子1α(HIF1α)蛋白,葡萄糖转运蛋白同工型1(Glut1)、己糖激酶(HK2)、乳酸脱氢酶A(LDHA)和血管内皮生长因子(VEGF)mRNA表达显著高于对照组,差异有统计学意义(P<0.05);而HIF1αmRNA水平比较,差异无统计学意义(P>0.05)。miR-9-5p抑制剂组HIF1α蛋白,Glut1、HK2、LDHA和VEGF mRNA表达显著低于对照组,差异有统计学意义(P<0.05);而HIF1αmRNA水平比较,差异无统计学意义(P>0.05)。与对照组比较,miR-9-5p过表达组显著增强了代谢及转移(P<0.05),而miR-9-5p抑制剂组显著降低了U251细胞中的葡萄糖摄取和乳酸生成(P<0.05)。miR-9-5p过表达组在处理24 h和48 h后的细胞活力显著高于对照组,差异有统计学意义(P<0.05);而miR-9-5p抑制剂组与对照组比较,细胞活力在24 h和48 h出现明显下降,差异有统计学意义(P<0.05)。miR-9-5p过表达组的肿瘤体积和湿重显著高于对照组,差异有统计学意义(P<0.05)。miR-9-5p过表达组的UBE4B的蛋白质水平低于对照组,差异有统计学意义(P<0.05);而HIF1α及糖酵解相关基因(Glut1、HK2和LDHA)的表达显著高于对照组,差异有统计学意义(P<0.05)。结论miR-9-5p能够通过UBE4B/HIF1α途径调节胶质瘤的Warburg效应并促进胶质瘤的发生发展。

泛素连接酶UBE4B的研究进展

泛素化是一类重要的蛋白质翻译后修饰,参与了体内多种生命活动。UBE4B作为泛素连接酶U-box家族的一员,含有一种约70个氨基酸组成的特征性U-box结构域,负责底物识别和结合。UBE4B还具有一种特殊的E4活性,可以在E1、E2和E3存在的情况下继续对泛素链进行延长。UBE4B参与了胚胎发育、神经元保护等一系列重要生命过程,它还可降解多种具有重要生理功能的底物,如p53、EGFR、FEZ1及Ataxin-3等,与癌症、神经退行性疾病、肥胖等疾病的发生发展有关。因此研究UBE4B参与的底物调控对于疾病治疗和新药开发有重大意义。从UBE4B的结构特征、生理功能、相关疾病与底物功能等方面,对近20年的研究进展进行了综述及展望,为后续深入研究UBE4B对生命活动的影响提供理论基础。

Growth factor receptor trafficking as a potential therapeutic target in pediatric cancer

Growth factor receptors （GFRs） are often aberrantly expressed in tumor cells, and altered GFR expressionand activity contribute to the pathogenesis of many types of cancer. A variety of mechanisms have been identified that result in enhanced GFR expression and activity in cancer cells. Defects in the pathways responsible for GFR internalization and intraceilular trafficking are likely to be involved in altered GFR expression in a variety of cancers. The roles of GFR trafficking pathways in the regulation of GFR expression, in the pathogenesis of tumors, and in the response of tumors to treatment have not been fully delineated, but the likely contributions of GFR signaling to the development and progression of various malignancies suggest that therapies that modify GFR trafficking may be effective as anticancer treatments. The intraceHular trafficking of GFRs is regulated by a number of protein complexes and by protein ubiquitination. Many of the proteins required for this trafficking are products of tumor suppressor genes, and the expression and function of the protein machinery utilized for intracellular trafficking is frequently altered in tumor cells, consistent with the likely role of GFR trafficking in tumorigenesis. Many of the proteins involved in GFR trafficking have been identified as potential targets for anticancer treatment, and novel treatments directed against these targets are currently in preclinical development and in clinical trials. Ubiquitin ligases are critical for GFR trafficking and represent potentially important targets for the development of novel therapies. The genes for the ubiquitin ligases c-Cbl and UBE4B are located in chromosome regions commonly altered in a variety of tumors and therefore are likely to be important for tumorigenesis, c-Cbl nbiquitinates a number of GFRs and directs them for degradation. Mutations in c-Cbl have been identified in cases of myeloid leukemia and myelodysplasia, providing a link between GFR ubiquitination and trafficking and leukemogenesis. We have shown that UBE4B plays a crucial role in GFR trafficking and degradation in tumor cells, suggesting a previously uncharacterized link between UBE4B and tumorigenesis. With the critical need for new and effective therapies for pediatric malignancies, the recently identified roles for the GFR trafficking pathway in the pathogenesis of various forms of cancer confirm the importance of the further development of novel therapies targeting this pathway in children with cancer.