1.Acupuncture combined with large amount of moxibustion for 78 cases of chronic gastritis.
Chinese Acupuncture & Moxibustion 2012;32(10):907-908
Acupuncture Therapy
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Adolescent
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Adult
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Aged
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Aged, 80 and over
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Female
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Gastritis, Atrophic
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therapy
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Humans
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Male
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Middle Aged
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Moxibustion
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Treatment Outcome
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Young Adult
2.Advances in research on oncolytic adenoviruses in tumor therapy.
Chinese Journal of Virology 2014;30(3):318-324
Oncolytic adenoviruses (Ads), which are live, replication-competent viruses that can selectively replicate in tumor cells and lead to cell lysis, have been used in tumor therapy. But due to the complexity and high mutability of human tumors, it becomes a major strategy to improve the selectivity, efficacy, and safety of oncolytic Ads. The oncolytic Ads that can express short hairpin RNA, cytokines, suicide gene, and matrix-modulating proteins have higher antitumor activity than the wild type. Tumor-specific promoters, especially hTERT and HRE promoters, increase the selectivity of oncolytic Ads for tumor cells. Moreover, oncolytic Ads surface-modified by polyethylene glycol (PEG), liposomes, biodegradable nanoparticles, and polypeptides have reduced immunogenicity and hepatotoxicity and improved antitumor activity when systemically administered, and the selectivity of oncolytic Ads can be significantly increased when linking PEG to antibodies, small peptides, cytokines, and ligands. Therefore, engineered oncolytic Ads combining the advantages of viral and non-viral vectors, as well as immunotherapy, are a promising strategy for improving the efficacy of targeted virotherapy.
Adenoviridae
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genetics
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physiology
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Animals
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Humans
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Neoplasms
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therapy
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virology
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Oncolytic Virotherapy
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trends
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Virus Replication
3.Comparative study of domestic and import vancomycin in the treatment of agranulocytosis complicated with infection in patients with acute leukemias.
Xiao-wen TANG ; Jian OUYANG ; Min ZHOU
Chinese Journal of Hematology 2011;32(9):632-633
Adolescent
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Adult
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Aged
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Agranulocytosis
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complications
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drug therapy
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Anti-Bacterial Agents
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administration & dosage
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therapeutic use
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Child
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Female
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Humans
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Leukemia
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complications
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drug therapy
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Male
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Middle Aged
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Treatment Outcome
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Vancomycin
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administration & dosage
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therapeutic use
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Young Adult
5.Biomechanical study on occipitocervical fusion fixed by metallic-rectangular frame
Zengming XIAO ; Shujin TANG ; Jieming WEN
Orthopedic Journal of China 2006;0(02):-
[Objective]To provide the mechanical evidence of self manufactured metallic-rectangular frame on the reconstruction of the stability of occipitocervical junction.[Method]Seven of the adult cervical spinal specimens which were entire wet-cadavers(from occipitale to C_6) were made to simulate the C_(0~2) fracture dislocation.These of specimens dislocated were fixed by metallic-rectangular frame and Occipito-cervical plate respectively.The three dimensional movements of C_(0~2) were recorded through photogrametry with a pure moment of 1.53 Nm.The range of motion(ROM) of each specimens in two fixation was caculated.[Result]Loaded by 1.53Nm,In metallic-rectangular frame fixation,the ROM in flexion,extension,lateral bending and axial rotation were 5.9?、7.7?、5.6?、11.2? respectively,decreased by 157.6%、68.8%、58.9%、131.3%,compared with occipitocervical plate fixation group.[Conclusion]Metallic-retangular frame fixation can reconstruct the stability of Occipitocervical junction immediatey,and is a relativity effective internal fixation for occipitocervical fusion.
8.Technology improvement in establishing rabbit models of osteonecrosis of the femoral head induced by glucocorticoid and lipopolysaccharide
Junlun YU ; Tianyou LUO ; Shaoping WU ; Xi TANG ; Wen XIAO
Chinese Journal of Tissue Engineering Research 2015;19(20):3129-3133
BACKGROUND:The rabbits were widely used as experimental animal models in the research on etiology and pathological mechanism of steroid-induced osteonecrosis of the femoral head. It is stil a valuable and realistic research topic to improve and to innovate the modeling technology nowadays. OBJECTIVE:To improve the modeling technology on osteonecrosis of the femoral head in rabbits induced by glucocorticoid combined with lipopolysaccharide, with the focus on its reduced mortality and the guaranteed successful rate of modeling. METHODS:A total of 28 New Zealand white rabbits were randomly divided into the control group (n=10) and improvement group (n=18). Models of steroid-induced osteonecrosis of the femoral head were established according to different methods. In the improvement group, rabbits were injected with sodium penicilin (5.0 mg/kg) and amikacin sulfate (1.63×104 U/kg) in the left gluteus muscle. Twenty-four hours later, al rabbits were injected with prednisolone acetate (20 mg/kg) in the right gluteus muscle. Forty-eighthours later, 5.0 μg/kg of lipopolysaccharide was intravenously injectedvia the ear. From then on, two injections of prednisolone acetate (20 mg/kg) were respectively performed alternately in the left and right gluteal muscle at an interval of each 24 hours. Sodium penicilin (5.0 mg/kg) and amikacin sulfate (1.63×104 U/kg) were intraperitonealy injected for 2 consecutiveweeks. In the control group, 10 μg/kg lipopolysaccharide was injectedvia the ear vein of rabbit. From then on, prednisolone acetate (20 mg/kg) was intramuscularly injected at an interval of each 24 hours, totaly three times. Benzylpenicilin sodium 20×104 U/rabbit was intramuscularly injected once a week. RESULTS AND CONCLUSION:Rabbit models of steroid-induced osteonecrosis of the femoral head were successfuly established in both groups. Compared with the control group, the mortality was significantly reduced after model establishment in the improvement group, and the bone lacuna and osteonecrosis of the femoral head were apparent. These findings indicated that the improved technology of model establishment of steroid-induced osteonecrosis of the femoral head could be used to aleviate the damage degree on the gluteal muscles, to guarantee the successful rate of modeling, and to noticeably reduce the mortality of rabbits.
9.Construction of eukarytic expression vector of enhanced green fluorescence protein driven by telomerase catalytic subunit promoter and its expression targeted in human lung cancer cells
Shengming ZHU ; Yanping WANG ; Xiaohe CHEN ; Xiaojun TANG ; Wen XIAO
Journal of Medical Postgraduates 2004;0(02):-
Objective:To construct an eukaryotic expression vector of enhanced green fluorescence protein(EGFP) gene driven by telomerase catalytic subunit(hTERT) gene promoter and observe the specific expression of EGFP in lung cancer cell lines.Methods:The 1100bp promoter fragment was obtained by enzyme digestion from a recombinant plasmid of pGL3-hTERTp containing the hTERT promoter.The hTERT promoter was then subcloned into the upstream of the report gene EGFP of pEGFP-1 without promoter.The expression vector pEGFP-hTERTp was successfully constructed.The vector pEGFP-N1 containing cytomegalovirus(CMV) promoter was used as a positive control.The vector pEGFP-1 without promoter was used as a negative control.The vectors were transfected into human lung cancer cell lines 95D,NCI-H446,A2,A549,LTEP-a-2,YTMLC and normal MRC-5 through lipofectamine respectively.EGFP expression was detected under the fluorescence microscope.Results:pEGFP-hTERTp was confirmed by enzyme digestion with correct result.That the EGFP expression was detected in all of eight lung cancer cells transfected with pEGFP-hTERTp,but not in MRC cells.By contrast,high intensity EGFP expression was observed in both lung tumor cells and normal cells,which were transfected with pEGFP-N1.Conclusion:The EGFP controlled by hTERT promoter can be expressed specifically in lung cancer cell lines.hTERT promoter may be used as an excellent regulation element in tumor-targeting gene therapy.
10.SAR of benzoyl sulfathiazole derivatives as PTP1B inhibitors.
Wen-Wen YIN ; Zheng CHEN ; Yan-Bo TANG ; Fei YE ; Jin-Ying TIAN ; Zhi-Yan XIAO
Acta Pharmaceutica Sinica 2014;49(5):632-638
Protein tyrosine phosphatase (PTP) 1B is a potential target for the treatment of diabetes and obesity. We have previously identified the benzoyl sulfathiazole derivative II as a non-competitive PTP1B inhibitor with in vivo insulin sensitizing effects. Preliminary SAR study on this compound series has been carried out herein, and thirteen new compounds have been designed and synthesized. Among them, compound 10 exhibited potent inhibition against human recombinant PTP1B with the IC50 value of 3.97 micromol x L(-1), and is comparable to that of compound II.
Humans
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Protein Tyrosine Phosphatase, Non-Receptor Type 1
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antagonists & inhibitors
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Structure-Activity Relationship
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Sulfathiazoles
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chemistry
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pharmacology