目的观察人脐带间充质干细胞(HUMSC)对糖尿病肾病大鼠肾脏缺氧诱导因子(HIF-1α)表达的影响。方法50只健康清洁级8周龄雄性SD大鼠,随机选取20只为健康对照组,其余30只采用链脲菌素复制糖尿病肾病大鼠模型(模型组),两组大鼠饲养12周。第1...目的观察人脐带间充质干细胞(HUMSC)对糖尿病肾病大鼠肾脏缺氧诱导因子(HIF-1α)表达的影响。方法50只健康清洁级8周龄雄性SD大鼠,随机选取20只为健康对照组,其余30只采用链脲菌素复制糖尿病肾病大鼠模型(模型组),两组大鼠饲养12周。第12周,随机选取两组大鼠各3只分别尾静脉注射DiR-HUMSCs,代谢12~16 h后在小动物活体光学3D成像系统下观察DiR-HUMSCs在大鼠体内的分布。随机选取9只模型组大鼠进行HUMSCs移植(HUMSCs移植组)。HUMSCs移植采用尾静脉注射方式移植浓度为1×10^(6)个/mL HUMSCs 500μL至大鼠体内,每周1次,连续4周,共28 d。检测3组大鼠的24 h尿蛋白定量(24 h UPro)、血清肌酐(Scr)、血尿素氮(BUN)、尿肌酐(Ucr)、尿白蛋白与肌酐比值(UACR)水平;酶联免疫吸附试验(ELISA)检测3组大鼠血清HIF-1α水平;采用PAS和Masson染色进行肾脏组织病理检测;免疫荧光法检测3组大鼠肾组织HIF-1α、Slc12A3和Aquaporin1蛋白的表达。结果移植HUMSCs治疗4周后,与健康对照组比较,模型组和HUMSCs移植组大鼠Ucr水平降低(P<0.05),Scr、24 h UPro、BUN、UCAR均升高(P<0.05);与模型组比较,HUMSCs移植组大鼠Ucr水平差异无统计学意义(P>0.05),Scr、24 h UPro、BUN、UCAR均降低(P<0.05)。糖尿病肾病大鼠病理损伤缓解,系膜增生和基底膜增厚改善,小管空泡变性减少,间质纤维化减轻。模型组大鼠血清HIF-1α水平较健康对照组升高(P<0.05),HUMSCs移植组血清HIF-1α水平较模型组下降(P<0.05)。与健康对照组比较,模型组大鼠肾脏远端小管中HIF-1α蛋白水平增加(P<0.05);HUMSCs移植组的HIF-1α蛋白水平较模型组降低(P<0.05)。模型组远端小管标记蛋白Slc12A3水平低于健康对照组(P<0.05),HUMSCs移植组Slc12A3水平较模型组升高(P<0.05)。HUMSCs移植组的Aquaporin1蛋白水平较模型组和健康对照组均降低(P<0.05)。糖尿病肾病大鼠近端小管中无HIF-1α表达。结论HIF-1α主要在糖尿病肾病大鼠肾脏远端小管表达,且HUMSCs可通过抑制HIF-1α的表达修复肾小管的损伤。展开更多
Osteosarcoma is a very serious primary bone cancer with a high death rate and a dismal prognosis.Since there is no permanent therapy for this condition,it is necessary to develop a cure.Therefore,this investigation wa...Osteosarcoma is a very serious primary bone cancer with a high death rate and a dismal prognosis.Since there is no permanent therapy for this condition,it is necessary to develop a cure.Therefore,this investigation was carried out to assess the impacts and biological functions of hydroxysafflor yellow A(HYSA)in osteosarcoma cell lines(MG63).In this investigational study,MG63 cells were utilized.Microarray experiments,quantitative polymerase chain reaction(qPCR),immunofluorescent staining,extracellular acidification rate(ECAR),oxygen consumption rate(OCR),glucose consumption,lactate production,and ATP levels,proliferation assay,5-Ethynyl-2′-deoxyuridine(EDU)staining,and Western blot were performed.In MG63 cells,HYSA lowered cell proliferation and metastasis rates,suppressed EDU cell number,and enhanced caspase-3/9 activity levels.HYSA reduced the Warburg effect and induced ferroptosis(FPT)in MG63 cells.Inhibiting ferroptosis diminished HYSA’s anti-cancer activities in MG63 cells.The stimulation of the HIF-1α/SLC7A11 pathway decreased HYSA’s anti-cancer activities in MG63 cells.HIF-1αis one target spot for HYSA in a model of osteosarcoma cancer(OC).HYSA altered HIF-1α’s thermophoretic activity;following binding with HYSA,HIF-1α’s melting point increased from~55°C to~60°C.HYSA significantly enhanced the thermal stability of exogenous WT HIF-1αwhile not affecting Mut HIF-1α,suggesting that ARG-311,GLY-312,GLN-347,and GLN-387 may be involved in the interaction between HIF-1αand HYSA.Conclusively,our study revealed that HYSA induced FPT and reduced the Warburg effect of OC through mitochondrial damage by HIF-1α/HK2/SLC7A11 pathway.HYSA is a possible therapeutic option for OC or other cancers.展开更多
缺氧诱导因子(hypoxia-inducible factor, HIF)与肝细胞癌的发生发展相关。HIF-1α在包括肝细胞癌在内的多种癌症类型的发生发展中发挥着重要作用,但其在肝细胞癌中的靶基因尚未完全确定。为找到HIF-1α在肝癌中新的致癌靶点,通过整合HI...缺氧诱导因子(hypoxia-inducible factor, HIF)与肝细胞癌的发生发展相关。HIF-1α在包括肝细胞癌在内的多种癌症类型的发生发展中发挥着重要作用,但其在肝细胞癌中的靶基因尚未完全确定。为找到HIF-1α在肝癌中新的致癌靶点,通过整合HIF-1α敲除的RNA-seq数据,HIF-1α的ChIP-Seq数据,HIF-1α在肝癌中的共表达基因,以及肝癌相关的GEO(Gene Expression Omnibus)数据集,寻找HIF-1α的潜在靶基因。通过分析TCGA(The Cancer Genome Atlas)肝癌数据库、GEO和HPA(Human Protein Atlas)数据集,研究HIF-1α与ATP2C1的相关性,ATP2C1在肝癌中的表达及预后。通过建立物理和化学(氯化钴)缺氧模型验证ATP2C1与低氧及HIF-1α的关系。通过GO(Gene Ontology),KEGG(Kyoto Encyclopedia of Genes and Genomes)和GSEA(Gene Set Enrichment Analysis)分析探索ATP2C1的生物学功能。通过设计体外实验证实ATP2C1对HCC的作用。利用STRING和BioGRID两个蛋白互作在线数据库获得ATP2C1的互作蛋白,并研究其在肝癌中的表达及相关性。通过整合及筛选数据,ATP2C1被鉴定为一个HIF-1α的潜在靶基因。ATP2C1与HIF-1α高度相关,在肝细胞癌中高表达,且伴随有不良预后。富集分析与体外实验的结果表明ATP2C1参与调控HCC细胞的增殖迁移。蛋白互作数据表明ATP2C1与TMEM165存在互作关系,生存分析表明TMEM1651高表达的肝癌患者预后较差。相关性分析的结果显示ATP2C1与肝癌中TMEM165和MMP2的表达高度相关,表明ATP2C1可能与TMEM165和MMP2存在互作关系,并参与了肝癌的进展过程。结果表明,ATP2C1是HIF-1α的靶基因和肝细胞癌的生物标志物,其敲低抑制了HCC的增殖和迁移。展开更多
文摘目的观察人脐带间充质干细胞(HUMSC)对糖尿病肾病大鼠肾脏缺氧诱导因子(HIF-1α)表达的影响。方法50只健康清洁级8周龄雄性SD大鼠,随机选取20只为健康对照组,其余30只采用链脲菌素复制糖尿病肾病大鼠模型(模型组),两组大鼠饲养12周。第12周,随机选取两组大鼠各3只分别尾静脉注射DiR-HUMSCs,代谢12~16 h后在小动物活体光学3D成像系统下观察DiR-HUMSCs在大鼠体内的分布。随机选取9只模型组大鼠进行HUMSCs移植(HUMSCs移植组)。HUMSCs移植采用尾静脉注射方式移植浓度为1×10^(6)个/mL HUMSCs 500μL至大鼠体内,每周1次,连续4周,共28 d。检测3组大鼠的24 h尿蛋白定量(24 h UPro)、血清肌酐(Scr)、血尿素氮(BUN)、尿肌酐(Ucr)、尿白蛋白与肌酐比值(UACR)水平;酶联免疫吸附试验(ELISA)检测3组大鼠血清HIF-1α水平;采用PAS和Masson染色进行肾脏组织病理检测;免疫荧光法检测3组大鼠肾组织HIF-1α、Slc12A3和Aquaporin1蛋白的表达。结果移植HUMSCs治疗4周后,与健康对照组比较,模型组和HUMSCs移植组大鼠Ucr水平降低(P<0.05),Scr、24 h UPro、BUN、UCAR均升高(P<0.05);与模型组比较,HUMSCs移植组大鼠Ucr水平差异无统计学意义(P>0.05),Scr、24 h UPro、BUN、UCAR均降低(P<0.05)。糖尿病肾病大鼠病理损伤缓解,系膜增生和基底膜增厚改善,小管空泡变性减少,间质纤维化减轻。模型组大鼠血清HIF-1α水平较健康对照组升高(P<0.05),HUMSCs移植组血清HIF-1α水平较模型组下降(P<0.05)。与健康对照组比较,模型组大鼠肾脏远端小管中HIF-1α蛋白水平增加(P<0.05);HUMSCs移植组的HIF-1α蛋白水平较模型组降低(P<0.05)。模型组远端小管标记蛋白Slc12A3水平低于健康对照组(P<0.05),HUMSCs移植组Slc12A3水平较模型组升高(P<0.05)。HUMSCs移植组的Aquaporin1蛋白水平较模型组和健康对照组均降低(P<0.05)。糖尿病肾病大鼠近端小管中无HIF-1α表达。结论HIF-1α主要在糖尿病肾病大鼠肾脏远端小管表达,且HUMSCs可通过抑制HIF-1α的表达修复肾小管的损伤。
文摘Osteosarcoma is a very serious primary bone cancer with a high death rate and a dismal prognosis.Since there is no permanent therapy for this condition,it is necessary to develop a cure.Therefore,this investigation was carried out to assess the impacts and biological functions of hydroxysafflor yellow A(HYSA)in osteosarcoma cell lines(MG63).In this investigational study,MG63 cells were utilized.Microarray experiments,quantitative polymerase chain reaction(qPCR),immunofluorescent staining,extracellular acidification rate(ECAR),oxygen consumption rate(OCR),glucose consumption,lactate production,and ATP levels,proliferation assay,5-Ethynyl-2′-deoxyuridine(EDU)staining,and Western blot were performed.In MG63 cells,HYSA lowered cell proliferation and metastasis rates,suppressed EDU cell number,and enhanced caspase-3/9 activity levels.HYSA reduced the Warburg effect and induced ferroptosis(FPT)in MG63 cells.Inhibiting ferroptosis diminished HYSA’s anti-cancer activities in MG63 cells.The stimulation of the HIF-1α/SLC7A11 pathway decreased HYSA’s anti-cancer activities in MG63 cells.HIF-1αis one target spot for HYSA in a model of osteosarcoma cancer(OC).HYSA altered HIF-1α’s thermophoretic activity;following binding with HYSA,HIF-1α’s melting point increased from~55°C to~60°C.HYSA significantly enhanced the thermal stability of exogenous WT HIF-1αwhile not affecting Mut HIF-1α,suggesting that ARG-311,GLY-312,GLN-347,and GLN-387 may be involved in the interaction between HIF-1αand HYSA.Conclusively,our study revealed that HYSA induced FPT and reduced the Warburg effect of OC through mitochondrial damage by HIF-1α/HK2/SLC7A11 pathway.HYSA is a possible therapeutic option for OC or other cancers.
文摘缺氧诱导因子(hypoxia-inducible factor, HIF)与肝细胞癌的发生发展相关。HIF-1α在包括肝细胞癌在内的多种癌症类型的发生发展中发挥着重要作用,但其在肝细胞癌中的靶基因尚未完全确定。为找到HIF-1α在肝癌中新的致癌靶点,通过整合HIF-1α敲除的RNA-seq数据,HIF-1α的ChIP-Seq数据,HIF-1α在肝癌中的共表达基因,以及肝癌相关的GEO(Gene Expression Omnibus)数据集,寻找HIF-1α的潜在靶基因。通过分析TCGA(The Cancer Genome Atlas)肝癌数据库、GEO和HPA(Human Protein Atlas)数据集,研究HIF-1α与ATP2C1的相关性,ATP2C1在肝癌中的表达及预后。通过建立物理和化学(氯化钴)缺氧模型验证ATP2C1与低氧及HIF-1α的关系。通过GO(Gene Ontology),KEGG(Kyoto Encyclopedia of Genes and Genomes)和GSEA(Gene Set Enrichment Analysis)分析探索ATP2C1的生物学功能。通过设计体外实验证实ATP2C1对HCC的作用。利用STRING和BioGRID两个蛋白互作在线数据库获得ATP2C1的互作蛋白,并研究其在肝癌中的表达及相关性。通过整合及筛选数据,ATP2C1被鉴定为一个HIF-1α的潜在靶基因。ATP2C1与HIF-1α高度相关,在肝细胞癌中高表达,且伴随有不良预后。富集分析与体外实验的结果表明ATP2C1参与调控HCC细胞的增殖迁移。蛋白互作数据表明ATP2C1与TMEM165存在互作关系,生存分析表明TMEM1651高表达的肝癌患者预后较差。相关性分析的结果显示ATP2C1与肝癌中TMEM165和MMP2的表达高度相关,表明ATP2C1可能与TMEM165和MMP2存在互作关系,并参与了肝癌的进展过程。结果表明,ATP2C1是HIF-1α的靶基因和肝细胞癌的生物标志物,其敲低抑制了HCC的增殖和迁移。