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Construction and in vitro Study of an E1B-Defective Adenovirus
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作者 XueFeng JoshuaMallamNock ZhuHua-bin DongChang-yuan QiYi-peng 《Wuhan University Journal of Natural Sciences》 CAS 2004年第2期259-264,共6页
An E1B-defective adenovirus named r1/Ad was constructed by homologous recombination. The construction, selection and propagation of recombinant virus was done in the human embryonic kidney 293 cells (HEK293). Thein vi... An E1B-defective adenovirus named r1/Ad was constructed by homologous recombination. The construction, selection and propagation of recombinant virus was done in the human embryonic kidney 293 cells (HEK293). Thein vitro study demonstrated that the recombinant virus has the ability to replicate in and lyse some p53-deficient human tumor cells such as the human glioblastoma tumor cells (U251) and human bladder tumer cells (EJ) but not in the normal cells with functional p53 such as the human fibroblast cells (MRC-5). Also, based on the cytopathic effect (CPE), it was demonstrated that the U251 cells were more sensitive to the infection of r1/Ad than that of EJ cells under identical conditions. In this paper, it was found that r1/Ad could be very useful in studying thein vitro selective replication of E1B-defective adenovirus. This may help to determine the safety of using any E1B-defective adenoviruses in cancer gene therapy. Key words E1B-defective adenovirus - cytopathic effect - cancer gene therapy CLC number Q78 Foundation item: Supported by the National Natural Science Foundation of China (3988003)Biography: Xue Feng (1978-), male, Master, research direction: cancer gene therapy by recombinant virus. 展开更多
关键词 E1B-defective adenovirus cytopathic effect cancer gene therapy
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缺氧诱导因子-1α和BCL-2/腺病毒E1B19 kDa相关蛋白3在中耳胆脂瘤表达及意义 被引量:1
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作者 岑瑞祥 赵凯 +4 位作者 万浪 彭聪 曹炜 刘原宙 龚国清 《中国耳鼻咽喉头颈外科》 CSCD 2019年第11期621-623,共3页
目的探讨缺氧诱导因子-1α(hypoxia inducible factor-1,HIF-1α)和BCL-2/腺病毒E1B19KDa相关蛋白3(Bcl2/adenovirus E1B 19 kD interacting protein 3,BNIP3)在中耳胆脂瘤中的表达及胆脂瘤上皮的凋亡情况。方法采用免疫组织化学方法检... 目的探讨缺氧诱导因子-1α(hypoxia inducible factor-1,HIF-1α)和BCL-2/腺病毒E1B19KDa相关蛋白3(Bcl2/adenovirus E1B 19 kD interacting protein 3,BNIP3)在中耳胆脂瘤中的表达及胆脂瘤上皮的凋亡情况。方法采用免疫组织化学方法检测30例中耳胆脂瘤标本与18例外耳道皮肤标本中HIF-1α和BNIP3蛋白的表达情况,使用末端脱氧核苷酸转移酶介导的dUTP缺口末端标记(terminal deoxynucleotidyl transferase-mediated dUTP nick-end-labeling,Tunel)检测20例中耳胆脂瘤标本和18例外耳道皮肤标本的凋亡情况。使用Pearson相关分析检验HIF-1α和BNIP3蛋白之间的相关性。结果 HIF-1α在胆脂瘤组和对照组的平均光密度分别为0.16±0.07和0.08±0.03,两组比较差异有统计学意义(t=4.279,P<0.01);BNIP3在胆脂瘤组和对照组的平均光密度分别为0.16±0.08和0.11±0.06,两组比较差异有统计学意义(t=2.463,P=0.0185);经pearson相关分析,在胆脂瘤上皮中,HIF-1α和BNIP3之间呈正相关(r=0.418,P=0.003);Tunel染色中,凋亡指数在胆脂瘤组和对照组分别为(52.8±12.5)%和(9.99±2.97)%,两组比较差异有统计学意义(t=14.166,P<0.01)。结论 HIF-1α和BNIP3在中耳胆脂瘤中的异常表达可能与胆脂瘤的高凋亡特性有关。 展开更多
关键词 胆脂瘤 中耳(Cholesteatoma Middle Ear) 对比研究(Comparative Study) 细胞凋亡(Apoptosis) 缺氧诱导因子-1α(hypoxia-inducible factor-1α) BCL-2/腺病毒E1B19 kDa相关蛋白3(Bcl2/adenovirus E1B 19 kD interacting protein 3)
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ROS-mediated BNIP3-dependent mitophagy promotes coelomocyte survival in Apostichopus japonicus in response to Vibrio splendidus infection 被引量:2
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作者 Lian-Lian Sun Yi-Na Shao +1 位作者 Mei-Xiang You Cheng-Hua Li 《Zoological Research》 SCIE CAS CSCD 2022年第2期285-300,共16页
Organisms produce high levels of reactive oxygen species(ROS)to kill pathogens or act as signaling molecules to induce immune responses;however,excessive ROS can result in cell death.To maintain ROS balance and cell s... Organisms produce high levels of reactive oxygen species(ROS)to kill pathogens or act as signaling molecules to induce immune responses;however,excessive ROS can result in cell death.To maintain ROS balance and cell survival,mitophagy selectively eliminates damaged mitochondria via mitophagy receptors in vertebrates.In marine invertebrates,however,mitophagy and its functions remain largely unknown.In the current study,Vibrio splendidus infection damaged mitochondrial morphology in coelomocytes and reduced mitochondrial membrane potential(ΔΨm)and mitophagosome formation.The colocalization of mitochondria and lysosomes further confirmed that lipopolysaccharide(LPS)treatment increased mitophagy flux.To explore the regulatory mechanism of mitophagy,we cloned Bcl2/adenovirus E1 B 19 kDa protein-interacting protein 3(BNIP3),a common mitophagy receptor,from sea cucumber Apostichopus japonicus(Aj BNIP3)and confirmed that Aj BNIP3 was significantly induced and accumulated in mitochondria after V.splendidus infection and LPS exposure.At the mitochondrial membrane,Aj BNIP3 interacts with microtubule-associated protein 1 light chain 3(LC3)on phagophore membranes to mediate mitophagy.After Aj BNIP3 interference,mitophagy flux decreased significantly.Furthermore,Aj BNIP3-mediated mitophagy was activated by ROS following the addition of exogenous hydrogen peroxide(H2 O2),ROS scavengers,and ROS inhibitors.Finally,inhibition of BNIP3-mediated mitophagy by Aj BNIP3 small interfering RNA(si RNA)or high concentrations of lactate increased apoptosis and decreased coelomocyte survival.These findings highlight the essential role of Aj BNIP3 in damaged mitochondrial degradation during mitophagy.This mitophagy activity is required for coelomocyte survival in A.japonicus against V.splendidus infection. 展开更多
关键词 Apostichopus japonicus MITOPHAGY Bcl2/adenovirus E1B 19 kDa protein-interacting protein 3 Reactive oxygen species Microtubule-associated protein 1 light chain 3
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Role of Mitophagy in Myocardial Ischemia/Reperfusion Injury and Chinese Medicine Treatment 被引量:6
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作者 XIA Jun-yan CHEN Cong +4 位作者 LIN Qian CUI Jie WAN Jie LI Yan LI Dong 《Chinese Journal of Integrative Medicine》 SCIE CAS CSCD 2023年第1期81-88,共8页
Mitophagy is one of the important targets for the prevention and treatment of myocardial ischemia/reperfusion injury(MIRI).Moderate mitophagy can remove damaged mitochondria,inhibit excessive reactive oxygen species a... Mitophagy is one of the important targets for the prevention and treatment of myocardial ischemia/reperfusion injury(MIRI).Moderate mitophagy can remove damaged mitochondria,inhibit excessive reactive oxygen species accumulation,and protect mitochondria from damage.However,excessive enhancement of mitophagy greatly reduces adenosine triphosphate production and energy supply for cell survival,and aggravates cell death.How dysfunctional mitochondria are selectively recognized and engulfed is related to the interaction of adaptors on the mitochondrial membrane,which mainly include phosphatase and tensin homolog deleted on chromosome ten(PTEN)-induced kinase 1/Parkin,hypoxia-inducible factor-1α/Bcl-2 and adenovirus e1b19k Da interacting protein 3,FUN-14 domain containing protein 1 receptor-mediated mitophagy pathway and so on.In this review,the authors briefly summarize the main pathways currently studied on mitophagy and the relationship between mitophagy and MIRI,and incorporate and analyze research data on prevention and treatment of MIRI with Chinese medicine,thereby provide relevant theoretical basis and treatment ideas for clinical prevention of MIRI. 展开更多
关键词 MITOPHAGY myocardial ischemia/reperfusion injury PTEN-induced kinase 1/Parkin hypoxia-inducible factor-1α/Bcl-2 and adenovirus e1b19k Da interacting protein 3 FUN-14 domain containing protein 1 Chinese medicine
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Targeting neuronal mitophagy in ischemic stroke:an update 被引量:2
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作者 Jun Li Jiaying Wu +3 位作者 Xinyu Zhou Yangyang Lu Yuyang Ge Xiangnan Zhang 《Burns & Trauma》 SCIE 2023年第1期459-469,共11页
Cerebral ischemia is a neurological disorder associated with complex pathological mechanisms,including autophagic degradation of neuronal mitochondria,or termed mitophagy,following ischemic events.Despite being well-d... Cerebral ischemia is a neurological disorder associated with complex pathological mechanisms,including autophagic degradation of neuronal mitochondria,or termed mitophagy,following ischemic events.Despite being well-documented,the cellular and molecular mechanisms under-lying the regulation of neuronal mitophagy remain unknown.So far,the evidence suggests neuronal autophagy and mitophagy are separately regulated in ischemic neurons,the latter being more likely activated by reperfusional injury.Specifically,given the polarized morphology of neurons,mitophagy is regulated by different neuronal compartments,with axonal mitochondria being degraded by autophagy in the cell body following ischemia-reperfusion insult.A variety of molecules have been associated with neuronal adaptation to ischemia,including PTEN-induced kinase 1,Parkin,BCL2 and adenovirus E1B 19-kDa-interacting protein 3(Bnip3),Bnip3-like(Bnip3l)and FUN14 domain-containing 1.Moreover,it is still controversial whether mitophagy protects against or instead aggravates ischemic brain injury.Here,we review recent studies on this topic and provide an updated overview of the role and regulation of mitophagy during ischemic events. 展开更多
关键词 MITOPHAGY Cerebral ischemia Neuroprotection PTEN-induced kinase 1 PARKIN BCL2 and adenovirus E1B 19-kDainteracting protein 3 Bnip3-like FUN14 domain-containing 1
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Gene-viral vectors: a promising way to target tumor cells and express anticancer genes simultaneously
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作者 钱其军 岑信棠 +5 位作者 车小燕 徐建国 薛惠斌 崔贞福 朱斌 吴孟超 《Chinese Medical Journal》 SCIE CAS CSCD 2002年第8期1213-1217,154-155,共5页
OBJECTIVE: To develop a new kind of vector system called gene-viral vector, which combines the advantages of gene and virus therapies. METHODS: Using recombinant technology, an anti-tumor gene was inserted into the ge... OBJECTIVE: To develop a new kind of vector system called gene-viral vector, which combines the advantages of gene and virus therapies. METHODS: Using recombinant technology, an anti-tumor gene was inserted into the genome of replicative virus specific for tumor cells. The cell killing effect, reporter gene expression of the green fluorescence protein, anti-tumor gene expression of mouse interleukin-12 (mIL-12) and replication of virus were observed by the methods of cell pathology, fluorescence microscopy, ELISA and electron microscopy, respectively. RESULTS: A new kind of gene-viral vector system of adenovirus, in which the E1b-55 kD gene was deleted but the E1a gene was preserved, was constructed. The vector system, like the replicative virus ONYX-015, replicated and proliferated in tumor cells but not in normal ones. Our vector had an advantage over ONYX-015 in that it carried different kinds of anti-tumor genes to enhance its therapeutic effect. The reporter gene expression of the green fluorescence protein in tumor cells was much better than the adenovirus vector employed in conventional gene the rapy, and the expression in our vector system was as low as or even less than that in the conventional adenovirus gene therapy system. Similar results were observed in experiments with this vector system carrying the anti-tumor gene mIL-12. Replication and proliferation of the virus carrying the mIL-12 gene in tumor cells were confirmed by electron microscopy. CONCLUSIONS: Gene-viral vectors are new vectors with an anti-tumor gene inserted into the genome of replicative virus specific for tumor cells. Because of the specific replication and proliferation of the virus in tumor cells, expression of the anti-tumor gene is increased hundreds to thousands of times. This approach takes full advantages of gene therapy and virus therapy to enhance the effect on the tumor. It overcomes the disadvantages of conventional gene therapy, such as low transfer rate, low gene expression, lack of target tropism, and low anti-tumor activity. We believe that this is a promising means for future tumor treatment. 展开更多
关键词 ADENOVIRIDAE adenovirus e1a Proteins adenovirus E1B Proteins Gene Therapy Genetic Vectors Humans INTERLEUKIN-12 Neoplasms Recombination Genetic Research Support Non-U.S. Gov't Tumor Cells Cultured Virus Replication
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Effects of Arsenic on Cell Proliferation and Its Related Gene Expression in Human Epidermal Keratinocyte
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作者 顾军 毕新岭 +1 位作者 米庆胜 文军慧 《Chinese Journal of Integrative Medicine》 SCIE CAS 2002年第4期284-286,共3页
Objective:To study the effects of low concentration of ar senic (As 2O 3) on DNA synthesis and related transcription factor gene E2F1 express ion in keratinocyte. Methods:Human epidermal keratinocyte (cell line HaCa... Objective:To study the effects of low concentration of ar senic (As 2O 3) on DNA synthesis and related transcription factor gene E2F1 express ion in keratinocyte. Methods:Human epidermal keratinocyte (cell line HaCaT) cultured in vitro was used. After treatment with various concentrations of arsenic, DNA s ynthesis and E2F1 expression in HaCaT cells were detected by using 3H-TdR method and RT-PCR.Results:Arsenic caused a modest increase of keratinocyte DNA synth esis when the concentration reached the range within 0.5-16 nmol/L, but the amo unt of incorporated 3H-TdR decreased and returned to baseline level when th e concentration of arsenic increased to over 16 nmol/L. RT-PCR analysis showe d the level of E2F1 mRNA was elevated in HaCaT cells with the increase of DNA sy nthesis. Conclusion:Arsenic of a certain concentration could increase DNA s ynthesis and enhance E2F1 expression in HaCaT cell line, which might be one of t he pathological mechanisms of skin disease related to arsenic. 展开更多
关键词 ARSENIC KERATINOCYTE cell proliferation transcription factor 1 combined with adenovirus E2 promotor
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