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土壤中细菌HC5的分离鉴定及抑菌活性测定 被引量:4
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作者 张艳萍 令利军 +2 位作者 赵瑛 厚毅清 马海霞 《农业资源与环境学报》 CAS 北大核心 2018年第6期527-532,共6页
为了筛选出对马铃薯晚疫疫霉菌(Phytophthora infestans)有较强拮抗作用的生防细菌,从马铃薯种植地的土壤中分离细菌,并通过平板对峙法,测定分离细菌对马铃薯晚疫疫霉菌的拮抗作用。经大量拮抗实验,筛选出一株细菌HC5,经形态特征观察、... 为了筛选出对马铃薯晚疫疫霉菌(Phytophthora infestans)有较强拮抗作用的生防细菌,从马铃薯种植地的土壤中分离细菌,并通过平板对峙法,测定分离细菌对马铃薯晚疫疫霉菌的拮抗作用。经大量拮抗实验,筛选出一株细菌HC5,经形态特征观察、生理生化特性测定和16S rRNA基因序列分析,确定该菌株为假单胞菌(Pseudomonas sp.)。抑菌试验结果表明,HC5菌株对辣椒疫霉菌(Phytophthora capsici)、黄瓜尖孢镰刀菌(Fusarium oxysporum)、马铃薯晚疫疫霉菌、辣椒炭疽菌(Colletotrichum capsici)均有一定的抑制作用,尤其对马铃薯晚疫疫霉菌的抑菌效果显著,抑菌率达89%。采用PCR方法对菌株HC5进行多种抗生素合成基因的检测,扩增到786 bp的硝吡咯菌素片段和587 bp的氢氰酸片段,表明菌株HC5能够代谢产生这两种抗生素,单一或协同发挥拮抗作用。研究表明,菌株HC5是一株具有开发潜力的生防细菌。 展开更多
关键词 土壤 细菌 HC5 假单胞菌 马铃薯晚疫疫霉菌 抑菌活性
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丝裂亚菊精油抗氧化、抑菌活性及抑菌机理初步研究 被引量:1
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作者 令利军 马稳霞 +4 位作者 赵云花 焦正龙 李子彬 梁俊玉 张继 《兰州大学学报(自然科学版)》 CAS CSCD 北大核心 2021年第1期137-142,共6页
对丝裂亚菊精油进行成分分析,测定抗氧化活性和抑菌活性并初步研究其抑菌机理.蒸馏法提取丝裂亚菊精油并对其成分进行气相色谱-质谱(GC-MS)分析;滤纸片法定性测定其抑菌活性,倍比稀释法定量测定最低抑菌浓度和最低杀菌浓度;1, 1-二苯基... 对丝裂亚菊精油进行成分分析,测定抗氧化活性和抑菌活性并初步研究其抑菌机理.蒸馏法提取丝裂亚菊精油并对其成分进行气相色谱-质谱(GC-MS)分析;滤纸片法定性测定其抑菌活性,倍比稀释法定量测定最低抑菌浓度和最低杀菌浓度;1, 1-二苯基-2-三硝基苯肼测定抗氧化能力;扫描电镜观察精油对测试菌种细胞壁膜的影响. GC-MS分析结果显示,丝裂亚菊精油中含有17种化合物,占精油总含量的97.37%,主要成分为β-蒎烯(34.72%)、(1, 8-)桉树脑(24.97%)和马鞭草烯醇(20.39%);抑菌试验发现丝裂亚菊精油对供试菌种均具有较强的拮抗作用,且供试菌种的最低抑菌浓度在2.5~80μL/mL内,最低杀菌浓度在10~80μL/mL内;扫描电镜结果显示植物精油破坏了细菌的壁膜,且浓度越大,对细胞壁膜的损伤程度越大.丝裂亚菊精油对破伤风杆菌、枯草芽孢杆菌、铜绿假单胞杆菌有很强的抑制性,其抗菌机理为丝裂亚菊精油对细菌细胞的壁膜造成了不可逆转的破坏. 展开更多
关键词 丝裂亚菊精油 成分分析 抑菌活性 抗氧化活性 抑菌机理
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地衣芽孢杆菌TG116胞外蛋白酶产酶条件与酶学性质 被引量:6
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作者 令利军 焦正龙 +5 位作者 王军英 马稳霞 李子彬 赵云花 张玺 冯娟娟 《微生物学通报》 CAS CSCD 北大核心 2019年第10期2559-2568,共10页
【背景】从独角莲中分离得到的地衣芽孢杆菌TG116是一株对植物病原菌具有广谱抗性作用的生防菌株。【目的】优化TG116的产酶条件并探索其酶学性质,进一步了解其抗菌机制。【方法】采用Folin-Phenol显色法与响应曲面法,优化菌株TG116的... 【背景】从独角莲中分离得到的地衣芽孢杆菌TG116是一株对植物病原菌具有广谱抗性作用的生防菌株。【目的】优化TG116的产酶条件并探索其酶学性质,进一步了解其抗菌机制。【方法】采用Folin-Phenol显色法与响应曲面法,优化菌株TG116的产酶条件并研究其蛋白酶的酶学性质。【结果】菌株TG116产酶最适条件为:温度40.83°C,p H 8.01,发酵时间53.74 h,增加通气量可以显著提高酶活力。按照优化后的条件培养48 h后,上清液蛋白酶活力从57.46 U/mL达到了254.07 U/mL。酶学性质研究表明:该酶为碱性蛋白酶,最适反应pH为8.5,最适反应温度为50°C,具有良好的温度和pH稳定性,EDTA对酶活具有强烈的抑制作用,金属离子Mg2+、Ca2+、Na+、Co2+、K+等对酶活也具有一定的抑制作用。【结论】菌株TG116具有良好的p H与温度稳定性,在实际应用中蛋白酶不易失活,可以分解真菌的细胞壁蛋白成分,破坏细胞壁结构,从而抑制甚至杀死病原菌,达到抗菌作用。 展开更多
关键词 碱性蛋白酶 产酶条件 酶学性质
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Houttuynia cordata polysaccharide alleviated intestinal injury and modulated intestinal microbiota in H1N1 virus infected mice 被引量:29
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作者 CHEN Mei-Yu LI Hong +5 位作者 LU Xiao-Xiao ling li-jun WENG Hong-Bo SUN Wei CHEN Dao-Feng ZHANG Yun-Yi 《Chinese Journal of Natural Medicines》 SCIE CAS CSCD 2019年第3期187-197,共11页
Houttuynia cordata polysaccharide(HCP) is extracted from Houttuynia cordata, a key traditional Chinese medicine. The study was to investigate the effects of HCP on intestinal barrier and microbiota in H1N1 virus infec... Houttuynia cordata polysaccharide(HCP) is extracted from Houttuynia cordata, a key traditional Chinese medicine. The study was to investigate the effects of HCP on intestinal barrier and microbiota in H1N1 virus infected mice. Mice were infected with H1N1 virus and orally administrated HCP at a dosage of 40 mg×kg^(–1)×d^(–1). H1N1 infection caused pulmonary and intestinal injury and gut microbiota imbalance. HCP significantly suppressed the expression of hypoxia inducible factor-1α and decreased mucosubstances in goblet cells, but restored the level of zonula occludens-1 in intestine. HCP also reversed the composition change of intestinal microbiota caused by H1N1 infection, with significantly reduced relative abundances of Vibrio and Bacillus, the pathogenic bacterial genera. Furthermore, HCP rebalanced the gut microbiota and restored the intestinal homeostasis to some degree. The inhibition of inflammation was associated with the reduced level of Toll-like receptors and interleukin-1β in intestine, as well as the increased production of interleukin-10. Oral administration of HCP alleviated lung injury and intestinal dysfunction caused by H1N1 infection. HCP may gain systemic treatment by local acting on intestine and microbiota. This study proved the high-value application of HCP. 展开更多
关键词 H1N1 influenza virus Houttuynia cordata INFLAMMATION Intestinal Barrier MICROBIOTA POLYSACCHARIDE
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A novel mouse model of human breast cancer stem-like cells with high CD44^+CD24^–/lower phenotype metastasis to human bone 被引量:10
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作者 ling li-jun WANG Shui +7 位作者 LIU Xiao-an SHEN En-chao DING Qiang LU Chao XU Jian CAO Qin-hong ZHU Hai-qing WANG Feng 《Chinese Medical Journal》 SCIE CAS CSCD 2008年第20期1980-1986,共7页
Background A satisfactory animal model of breast cancer metastasizing to bone is unavailable. In this study, we used human breast cancer stem-like cells and human bone to build a novel “human-source” model of human ... Background A satisfactory animal model of breast cancer metastasizing to bone is unavailable. In this study, we used human breast cancer stem-like cells and human bone to build a novel “human-source” model of human breast cancer skeletal metastasis. Methods Human breast cancer stem-like cells, the CD44^+/CD24^-/lower subpopulation, was separated and cultured. Before injection with the stem-like cells, mice were implanted with human bone in the right or left dorsal flanks. Animals in Groups A, B, and C were injected with 1×10^5, 1×10^6 human breast cancer stem-like cells, and 1×10^6 parental MDA-MB-231 cells, respectively. A positive control group (D) without implantation of human bone was also injected with 1×10^6 MDA-MB-231 cells. Immunohistochemistry was performed for determination of CD34, CD105, smooth muscle antibody, CD44, CD24, cytokine, CXC chemokine receptor-4 (CXCR4), and osteopontin (OPN). mRNA levels of CD44, CD24, CXCR4, and OPN in bone metastasis tissues were analyzed by real-time quantitative polymerase chain reaction (PCR).Results Our results demonstrated that cells in implanted human bones of group B, which received 1×10^6 cancer stem-like cells, stained strongly positive for CD44, CXCR4, and OPN, whereas those of other groups showed no or minimum staining. Moreover, group B had the highest incidence of human bone metastasis (77.8%, P=0.0230) and no accompaniment of other tissue metastasis. The real-time PCR showed an increase of CD44, CXCR4, and OPN mRNA in metastatic bone tissues in group B compared with those of groups C and D, however the expression of CD24 mRNA in group B were the lowest. Conclusions In the novel “human source” model of breast cancer, breast cancer stem-like cells demonstrated a higher human bone-seeking ability. Its mechanism might be related to the higher expressions of CD44, CXCR4, and OPN, and the lower expression of CD24 in breast cancer stem-like cells. 展开更多
关键词 breast cancer cancer stem-like cells human source bone metastasis animal model
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