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Immunomodulation in the canine endometrium by uteropathogenic Escherichia coli

机译：子宫内致病性大肠杆菌对犬子宫内膜的免疫调节

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摘要

This study was designed to evaluate the role of E. coli α-hemolysin (HlyA) in the pathogenesis of canine pyometra, and on the immune response of canine endometrial epithelial and stromal cells. In Experiment 1, the clinical, hematological, biochemical and uterine histological characteristics of β-hemolytic and non-hemolytic E. coli pyometra bitches were compared. More (p < 0.05) metritis cases were observed in β-hemolytic E. coli pyometra uteri than in non-hemolytic E. coli pyometra uteri. β-hemolytic E. coli pyometra endometria had higher gene transcription of IL-1β and IL-8 and lower gene transcription of IL-6 than non-hemolytic E. coli pyometra endometria (p < 0.01). In Experiment 2, the immune response of endometrial epithelial and stromal cells, to hemolytic (Pyo18) and non-hemolytic E. coli strains (Pyo18 with deleted hlya-Pyo18ΔhlyA- and Pyo14) were compared. Following 4 h of incubation, Pyo18 decreased epithelial cell numbers to 54% (p < 0.001), and induced death of all stromal cells (p < 0.0001), whereas Pyo18ΔhlyA and Pyo14 had no effect on cell numbers. Compared to Pyo18ΔhlyA and Pyo14, respectively, Pyo18 induced a lower transcription level of IL-1β (0.99 vs 152.0 vs 50.9 fold increase, p < 0.001), TNFα (3.2 vs 49.9 vs 12.9 fold increase, p < 0.05) and IL-10 (0.4 vs 3.6 vs 2.6 fold increase, p < 0.001) in stromal cells, after 1 h of incubation. This may be seen as an attempt of hemolytic E. coli to delay the activation of the immune response. In conclusion, endometrial epithelial and stromal cell damage induced by HlyA is a potential relevant step of E. coli virulence in the pathogenesis of pyometra.

机译：这项研究旨在评估大肠杆菌α-溶血素（HlyA）在犬脓毒症的发病机理中以及在犬子宫内膜上皮和基质细胞的免疫应答中的作用。在实验1中，比较了β溶血性和非溶血性大肠杆菌脓疱性母犬的临床，血液学，生化和子宫组织学特征。与非溶血性大肠杆菌脓毒症相比，β-溶血性大肠杆菌脓毒症观察到更多（p <0.05）子宫炎病例。与非溶血性大肠杆菌脓毒症子宫内膜相比，β溶血性大肠杆菌脓毒症子宫内膜具有更高的IL-1β和IL-8基因转录，IL-6的基因转录较低（p <0.01）。在实验2中，比较了子宫内膜上皮和基质细胞对溶血性（Pyo18）和非溶血性大肠杆菌菌株（缺失hlya-Pyo18ΔhemA-和Pyo14的大肠杆菌）的免疫应答。孵育4小时后，Pyo18将上皮细胞数量减少至54％（ p <0.001），并诱导所有基质细胞死亡（ p <0.0001），而Pyo18Δ< em> hlyA 和Pyo14对细胞数没有影响。与Pyo18 ΔhlyA和Pyo14相比，Pyo18诱导了 IL -1β较低的转录水平（分别为0.99、152.0和50.9倍，< em> p <0.001），TNFα（分别增加3.2倍，49.9倍和12.9倍， p <0.05）和 IL -<孵育1小时后，基质细胞中的em> 10 （分别增加0.4倍，3.6倍和2.6倍， p <0.001）， p <0.001。这可能被认为是溶血性大肠杆菌的尝试。大肠杆菌来延迟免疫反应的激活。总之，HlyA诱导的子宫内膜上皮和基质细胞损伤是 E的潜在相关步骤。脓毒症发病机理中的大肠杆菌毒性。 展开▼

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期刊名称 Veterinary Research

作者
Sofia Henriques; Elisabete Silva; Marta F. Silva; Sandra Carvalho; Patrícia Diniz; Luís Lopes-da-Costa; Luisa Mateus;
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作者单位

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年(卷),期 2016(47),-1

年度 2016

页码 114

总页数 17

原文格式 PDF

正文语种

中图分类动物医学（兽医学）;

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专利

1. Immunomodulation in the canine endometrium by uteropathogenic Escherichia coli [J] . Sofia Henriques, Elisabete Silva, Marta F. Silva, Veterinary research . 2016,第1期

机译：子宫内致病性大肠杆菌对犬子宫内膜的免疫调节

2. Uropathogenic virulence factor FimH facilitates binding of uteropathogenic Escherichia coli to canine endometrium. [J] . Krekeler N., Marenda M. S., Browning G. F., Comparative Immunology, Microbiology and Infectious Diseases . 2012,第5期

机译：致病性毒力因子FimH促进了致病性大肠杆菌与犬子宫内膜的结合。

3. The role of Type 1, P and S fimbriae in binding of Escherichia coli to the canine endometrium. [J] . Krekeler N., Marenda M. S., Browning G. F., Veterinary Microbiology . 2013,第3a4期

机译：1型，P型和S型菌毛在大肠杆菌与犬子宫内膜的结合中的作用。

4. Immunomodulation Effect of Meniran (Phyllanthus niruri linn) on Blood Profile of Broiler Chickens Infected with Enterotoxin of Antibiotic-Resistant Escherichia coli [C] . Diyantoro, Emy Koestanti Sabdoningrum, Sri Hidanah, International Conference Postgraduate School Universitas Airlangga . 2018

机译：Meniran（Phyllanthus niriuri Linn）对抗生素抗菌大肠杆菌肠毒素感染的肉鸡鸡血型的免疫调节作用

5. Clonality and Antimicrobial Resistance in Canine Uropathogenic Escherichia coli [D] . Lecuyer, Tessa Emily. 2018

机译：犬尿毒原性大肠杆菌的克隆性和抗药性

6. Probiotic Escherichia coli Nissle 1917-derived outer membrane vesicles enhance immunomodulation and antimicrobial activity in RAW264.7 macrophages [O] . Rujiu Hu, Hua Lin, Jing Li, 2020

机译：益生菌大肠杆菌烟头1917衍生的外膜囊泡增强了Raw264.7巨噬细胞的免疫调节和抗微生物活性

7. Immunomodulation in the canine endometrium by uteropathogenic Escherichia coli [O] . Henriques, Sofia, Silva, Elisabete, Silva, Marta F., 2016

机译：子宫内致病性大肠杆菌对犬子宫内膜的免疫调节

1. 致病性大肠杆菌诱导的小鼠子宫内膜炎模型建立 [J] . 孙凯鑫 ,王友元 ,石丽颖 . 中国畜牧杂志 . 2021,第004期

2. 奶牛子宫内膜炎致病性大肠杆菌的分离鉴定及耐药性分析 [J] . 王德志 ,王晓旭 ,张敏 . 黑龙江畜牧兽医 . 2009,第6期

3. 基于免疫调节探讨温肾消癥汤治疗卵巢子宫内膜异位囊肿的作用机制 [J] . 仇燕飞 ,彭继红 ,万贵平 . 中外医学研究 . 2019,第008期

4. 子宫内膜异位症患者免疫调节Th17细胞及Treg细胞的表达意义 [J] . 张达 ,杜艳辉 ,袁芳 . 中华细胞与干细胞杂志（电子版） . 2019,第005期

5. 卵巢子宫内膜异位囊肿患者免疫调节细胞Th17/Treg失衡的临床研究 [J] . 杨娟 ,韦成厚 ,祝彩霞 . 中山大学学报（医学科学版） . 2017,第001期

6. 犬、猫子宫内膜炎的诊断技术 [C] . 邓干臻 . 第十八届世界中兽医大会、第六届亚洲传统兽医学术研讨会、第十届中国畜牧兽医学会小动物医学分会大会、第一届国际临床马兽医大会、第十二届北京宠物医师大会 . 2016

7. 子宫内膜再生细胞在溃疡性结肠炎模型中免疫调节的相关机制研究 [A] . 史刚刚 . 2017

1. 一种子宫内膜样腺癌检测试剂及其在子宫内膜样腺癌检测中的应用 [P] . 中国专利： CN114136932A . 2022-03-04

2. 子宫内膜癌相关的标志分子及其在诊断子宫内膜癌中的应用 [P] . 中国专利： CN113493838B . 2021.11.23

3. GENE-THERAPEUTIC DNA-VECTOR BASED ON GENE-THERAPEUTIC DNA-VECTOR VTVAF17, CARRYING TARGET GENE SELECTED FROM GROUP OF GENES ANG, ANGPT1, VEGFA, FGF1, HIF1Α, HGF, SDF1, KLK4, PDGFC, PROK1, PROK2 TO INCREASE EXPRESSION LEVEL OF SAID TARGET GENES, METHOD FOR PRODUCTION AND USE THEREOF, STRAIN ESCHERICHIA COLI SCS110-AF/VTVAF17-ANG, OR ESCHERICHIA COLI SCS110-AF/VTVAF17-ANGPT1, OR ESCHERICHIA COLI SCS110-AF/VTVAF17-VEGFA, OR ESCHERICHIA COLI SCS110-AF/VTVAF17-FGF1, OR ESCHERICHIA COLI SCS110-AF/VTVAF17-HIF1Α, OR ESCHERICHIA COLI SCS110-AF/VTVAF17-HGF, OR ESCHERICHIA COLI SCS110-AF/VTVAF17-SDF1, OR ESCHERICHIA COLI SCS110-AF/VTVAF17-KLK4, OR ESCHERICHIA COLI SCS110-AF/VTVAF17-PDGFC, OR ESCHERICHIA COLI SCS110-AF/VTVAF17-PROK1, OR ESCHERICHIA COLI SCS110-AF/VTVAF17-PROK2, CARRYING GENE-THERAPEUTIC DNA VECTOR, METHOD FOR PRODUCTION THEREOF, METHOD FOR INDUSTRIAL PRODUCTION OF GENE-THERAPEUTIC DNA VECTOR [P] . 外国专利： RU2730664C2 . 2020-08-24

机译：基于基因治疗DNA载体VTVAF17的基因治疗DNA载体，携带选自基因ANG，ANGPT1，VEGFA，FGF1，HIF1α，HGF，SDF1，KLK4，PDGFC，PROK1，PROK2表达的靶基因所述的靶标基因，其生产和使用方法，应变大肠埃希氏菌SCS110-AF / VTVAF17-ANG或大肠埃希氏菌SCS110-AF / VTVAF17-ANGPT1或大肠埃希氏菌SCS110-AF / VTVAF17-VEGFA或大肠埃希氏菌SCS110-AF / VTVAF17-FGF1，或大肠埃希氏菌SCS110-AF / VTVAF17-HIF1A，或大肠埃希氏菌COLI SCS110-AF / VTVAF17-HGF，或大肠埃希氏菌SCS110-AF / VTVAF17-SDF1，或大肠埃希氏菌SCS110-AF / VTVAF17-KLK4，大肠埃希氏菌SCS110-AF / VTVAF17-PDGFC或大肠埃希氏菌SCS110-AF / VTVAF17-PROK2，携带基因-治疗性DNA载体，生产方法，工业生产方法-治疗性DNA载体

4. GENE-THERAPEUTIC DNA VECTOR BASED ON THE GENE-THERAPEUTIC DNA VECTOR GDTT1_8NAS12, CARRYING THE TARGET GENE SELECTED FROM A GROUP OF GENES DDC, IL10, IL13, IFNB1, TNFRSF4, TNFSF10, BCL2, HGF, IL2 TO INCREASE THE EXPRESSION LEVEL OF SAID TARGET GENES, A METHOD FOR PRODUCTION AND USE THEREOF, A STRAIN ESCHERICHIA COLI JM110-NAS/GDTT1_8NAS12-DDC OR ESCHERICHIA COLI JM110-NAS/GDTT1_8NAS12-IL10 OR ESCHERICHIA COLI JM110-NAS/GDTT1_8NAS12-IL13 OR ESCHERICHIA COLI JM110-NAS/GDTT1_8NAS12-IFNB1 OR ESCHERICHIA COLI JM110-NAS/GDTT1_8NAS12-TNFRSF4 OR ESCHERICHIA COLI JM110-NAS/GDTT1_8NAS12-TNFSF10 OR ESCHERICHIA COLI JM110-NAS/GDTT1_8NAS12-BCL2 OR ESCHERICHIA COLI JM110-NAS/GDTT1_8NAS12-HGF OR ESCHERICHIA COLI JM110-NAS/GDTT1_8NAS12-IL2, CARRYING A GENE-THERAPEUTIC DNA VECTOR, METHOD FOR PRODUCTION THEREOF, A METHOD FOR INDUSTRIAL PRODUCTION OF A GENE-THERAPEUTIC DNA VECTOR [P] . 外国专利： RU2734726C1 . 2020-10-22

机译：基于基因治疗DNA矢量GDTT1_8NAS12的基因治疗DNA矢量，携带从一组基因中选择的目标基因DDC，IL10，IL13，IFNB1，TNFRSF4，TNFSF10，BCL2，HGF，IL2可以增加表达水平基因，一种生产和使用其的方法，应变大肠埃希氏菌JM110-NAS / GDTT1_8NAS12-DDC或大肠埃希氏菌JM110-NAS / GDTT1_8NAS12-IL10或大肠埃希氏菌JM110-NAS / GDTT1_8NAS12-IL13或大肠埃希氏菌COLI JM110-NAS / GDTT1_8NAS12-IL13 IFNB1或ESCHERICHIA COLI JM110-NAS / GDTT1_8NAS12-TNFRSF4或ESCHERICHIA COLI JM110-NAS / GDTT1_8NAS12-TNFSF10或ESCHERICHIA COLI JM110-NAS / GDTT1_8NAS12-BCL2或ESCHERICHIA COLI JM110-NAS / GDTT1_8NAS12 IL2，携带基因治疗性DNA载体，其生产方法，工业生产基因治疗性DNA载体的方法

5. Gene therapeutic DNA vector based on VTvaf17 gene therapeutic DNA vector carrying a target gene selected from the group of genes ANG, ANGPT1, VEGFA, FGF1, HIF1α, HGF, SDF1, KLK4, PDGFC, PROK1, PROK2 to increase the expression level of these target genes, method its preparation and use, Escherichia coli strain SCS110-AF / VTvaf17-ANG or Escherichia coli SCS110-AF / VTvaf17-ANGPT1 or Escherichia coli SCS110-AF / VTvaf17-VEGFA or Escherichia coli SCS110-AF / VTvaf17-Fichia-SC110 AF / VTvaf17-HIF1α or Escherichia coli SCS110-AF / VTvaf17-HGF or Escherichia coli SCS110-AF / VTvaf17-SDF1 or Escherichia coli SCS110-AF / VTvaf17-KLK4 or Escherichia coli SCS110-AF / VTviFi10 SCF110 AF / VTvaf17-PROK1 or Escherichia coli SCS110-AF / VTvaf17-PROK2 carrying a gene therapy DNA vector, a method for its preparation, a method for the industrial production of a gene therapy DNA vector [P] . 外国专利： RU2018147085A . 2020-06-29

机译：基于VTvaf17基因治疗DNA载体的基因治疗DNA载体，其携带选自ANG，ANGPT1，VEGFA，FGF1，HIF1α，HGF，SDF1，KLK4，PDGFC，PROK1，PROK2的靶基因以增加这些靶标的表达水平基因，方法的制备和使用，大肠杆菌菌株SCS110-AF / VTvaf17-ANG或大肠杆菌SCS110-AF / VTvaf17-ANGPT1或大肠杆菌SCS110-AF / VTvaf17-VEGFA或大肠杆菌SCS110-AF / VTvaf17-Fichia-SC110 AF /VTvaf17-HIF1α或大肠杆菌SCS110-AF / VTvaf17-HGF或大肠杆菌SCS110-AF / VTvaf17-SDF1或大肠杆菌SCS110-AF / VTvaf17-KLK4或大肠杆菌SCS110-AF / VTviFi10 S1携带基因治疗DNA载体的大肠杆菌SCS110-AF / VTvaf17-PROK2，其制备方法，工业生产基因治疗DNA载体的方法

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Immunomodulation in the canine endometrium by uteropathogenic Escherichia coli

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