Altered central nervous system cytokine-growth factor expression profiles and angiogenesis in metallothionein-I+II deficient mice.

Penkowa M; Carrasco J; Giralt M; Molinero A; Hernandez J; Campbell IL; Hidalgo J

首页> 外文期刊>Journal of Cerebral Blood Flow and Metabolism: Official Journal of the International Society of Cerebral Blood Flow and Metabolism >Altered central nervous system cytokine-growth factor expression profiles and angiogenesis in metallothionein-I+II deficient mice.

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Altered central nervous system cytokine-growth factor expression profiles and angiogenesis in metallothionein-I+II deficient mice.

机译：金属硫蛋白-I + II缺陷小鼠中中枢神经系统细胞因子生长因子表达谱和血管生成的改变。

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To study the importance of metallothionein-I and -II (MT-I+II) for brain inflammation and regeneration, the authors examined normal and MT-I+II knock-out (MT-KO) mice subjected to a cortical freeze injury. Normal mice showed profound neurodegeneration, inflammation, and gliosis around the injury, which was repaired by 20 days postlesion (dpl). However, in MT-KO mice the lesion-associated inflammation was still present as late as 90 dpl. Scanning electron microscopy demonstrated that the number of capillaries was lower, and ultrastructural preservation of the lesioned parenchyma was poorer in MT-KO mice, suggesting an altered angiogenesis. To gain insight into the mechanisms involved, a number of cytokines and growth factors were evaluated. The number of cells expressing the proinflammatory cytokines IL-1beta, IL-6, and TNF-alpha was higher in MT-KO mice than in normal mice, which was confirmed by RNase protection analysis, whereas the number of cells expressing the growth factors bFGF, TGFbeta1, VEGF, and NT-3 was lower. Increased expression of proinflammatory cytokines could be involved in the sustained recruitment of CD-14+ and CD-34+ inflammatory cells and their altered functions observed in MT-KO mice. Decreases in trophic factors bFGF, TGFbeta1, and VEGF could mediate the decreased angiogenesis and regeneration observed in MT-KO mice after the freeze lesion. A role for MT-I+II in angiogenesis was also observed in transgenic mice expressing IL-6 under the control of the promoter of glial fibrillary acidic protein gene (GFAP-IL6 mice) because MT-I+II deficiency dramatically decreased the IL-6-induced angiogenesis of the GFAP-IL6 mice. In situ hybridization analysis indicated that the MT-III expression was not altered by MT-I+II deficiency. These results suggest that the MT-I+II isoforms have major regulatory functions in the brain inflammatory response to injury, especially in the angiogenesis process.

机译：为了研究金属硫蛋白-I和-II（MT-I + II）在脑部炎症和再生中的重要性，作者检查了遭受皮层冷冻损伤的正常和MT-I + II基因敲除（MT-KO）小鼠。正常小鼠在损伤周围表现出严重的神经退行性变，炎症和神经胶质增生，损伤后20天（dpl）可修复。但是，在MT-KO小鼠中，与病变相关的炎症仍然存在，直至90 dpl。扫描电子显微镜显示，在MT-KO小鼠中，毛细血管的数量较少，病变实质的超微结构保存较差，表明血管新生改变。为了深入了解所涉及的机制，评估了许多细胞因子和生长因子。 MT-KO小鼠中表达促炎细胞因子IL-1beta，IL-6和TNF-α的细胞数量高于正常小鼠，这通过RNase保护分析得到证实，而表达生长因子bFGF的细胞数量，TGFbeta1，VEGF和NT-3较低。促炎细胞因子表达的增加可能与CD-14 +和CD-34 +炎性细胞的持续募集及其在MT-KO小鼠中观察到的功能改变有关。营养因子bFGF，TGFbeta1和VEGF的减少可介导冷冻损伤后MT-KO小鼠中观察到的血管生成和再生减少。在由神经胶质原纤维酸性蛋白基因启动子控制的表达IL-6的转基因小鼠中也观察到MT-I + II在血管生成中的作用（GFAP-IL6小鼠），因为MT-I + II缺乏会大大降低IL- GFAP-IL6小鼠的6诱导血管生成。原位杂交分析表明MT-III表达没有被MT-I + II缺乏症改变。这些结果表明MT-I + II同工型在对损伤的脑炎反应中，特别是在血管生成过程中具有主要的调节功能。

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来源
《Journal of Cerebral Blood Flow and Metabolism: Official Journal of the International Society of Cerebral Blood Flow and Metabolism》 |2000年第8期|共16页
作者
Penkowa M; Carrasco J; Giralt M; Molinero A; Hernandez J; Campbell IL; Hidalgo J;
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正文语种 eng
中图分类神经病学;内分泌腺疾病及代谢病;
关键词
Brain; Cytokines; Growth Substances; Metallothionein; Neovascularization; Physiologic; 脑; 细胞活素类; 生长物质; 金属硫蛋白; 新生血管化; 生理性;

机译：Brain;Cytokines;Growth Substances;Metallothionein;Neovascularization;Physiologic;脑;细胞活素类;生长物质;金属硫蛋白;新生血管化;生理性;

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1. Altered central nervous system cytokine-growth factor expression profiles and angiogenesis in metallothionein-I+II deficient mice. [J] . Penkowa M, Carrasco J, Giralt M, Journal of Cerebral Blood Flow and Metabolism: Official Journal of the International Society of Cerebral Blood Flow and Metabolism . 2000,第8期

机译：金属硫蛋白-I + II缺陷小鼠中中枢神经系统细胞因子生长因子表达谱和血管生成的改变。
2. Interleukin (IL)-6 gene expression in the central nervous system is necessary for fever response to lipopolysaccharide or IL-1 beta: a study on IL-6-deficient mice. [J] . Z Chai, S Gatti, C Toniatti, The Journal of Experomental Medicine . 1996,第1期

机译：中枢神经系统中的白细胞介素（IL）-6基因表达对于对脂多糖或IL-1β的发烧反应是必需的：IL-6缺陷小鼠的研究。
3. Increased tumor necrosis factor and interleukin-6 production in the central nervous system of interleukin-10-deficient mice. [J] . Agnello D, Villa P, Ghezzi P Brain research . 2000,第1a2期

机译：白细胞介素10缺陷小鼠中枢神经系统中肿瘤坏死因子的增加和白细胞介素6的产生。
4. Pathogenic Rabies Virus Alters Host Protein Expression in the Central Nervous System: Implications for Neuronal Dysfunction [C] . Z.F. Fu, X. Li, V. Dhingra Joint World Organisation for Animal Health/World Health Organization/European Union International Conference "Towards the elimination of rabies in Eurasia" . 2008

机译：致病性狂犬病病毒改变了中枢神经系统中的宿主蛋白表达：对神经元功能障碍的影响
5. Pathogenesis of transforming growth factor-beta-1 overexpression in the central nervous system of transgenic mice. [D] . Galbreath, Elizabeth Jayne. 1997

机译：转基因小鼠中枢神经系统中转化生长因子-β-1过表达的发病机制。
6. Elevated interferon gamma expression in the central nervous system of tumour necrosis factor receptor 1-deficient mice with experimental autoimmune encephalomyelitis [O] . Rachel D Wheeler, Simone P Zehntner, Lisa M Kelly, 2006

机译：实验性自身免疫性脑脊髓炎的肿瘤坏死因子受体1缺陷小鼠中枢神经系统中干扰素γ的表达升高
7. Altered Central Nervous System Cytokine-Growth Factor Expression Profiles and Angiogenesis in Metallothionein-I+II Deficient Mice [O] . Milena Penkowa, Javier Carrasco, Mercedes Giralt, 2000

机译：改变的中枢神经系统细胞因子 - 生长因子表达谱和血管生成在金属硫蛋白-i + II缺陷小鼠中

Altered central nervous system cytokine-growth factor expression profiles and angiogenesis in metallothionein-I+II deficient mice.

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