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环缩酚肽抑制小鼠血管增殖性视网膜病变的研究 被引量:5
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作者 梁小玲 刘汉生 +3 位作者 陈浩宇 黄永盛 唐仕波 peter a.campochiaro 《中山大学学报(医学科学版)》 CAS CSCD 北大核心 2003年第6期532-535,共4页
【目的】观察两种环缩酚肽的衍生物(Hep-A)和(Hep-B)对氧诱导的血管增殖性视网膜病变的抑制作用。【方法】将鼠龄为7d(P7)的C57BL/6幼鼠置于体积分数75%的氧气箱中连续生活5d,建立氧诱导的血管增殖性视网膜病变模型。在12d(P12)幼鼠回... 【目的】观察两种环缩酚肽的衍生物(Hep-A)和(Hep-B)对氧诱导的血管增殖性视网膜病变的抑制作用。【方法】将鼠龄为7d(P7)的C57BL/6幼鼠置于体积分数75%的氧气箱中连续生活5d,建立氧诱导的血管增殖性视网膜病变模型。在12d(P12)幼鼠回到正常大气环境中,同时开始给小鼠皮下注安慰剂(第1组,n=23)、Hep-A10mg/kg(第2组,n=22)、或者Hep-B10mg/kg(第3组,n=22),每天两次,持续5d。在17d(P17)取鼠眼进行冰冻切片和GSA(griffoniasimplicifolialectinB4)染色,或作荧光素灌注和视网膜平铺片,用图象分析软件定量计算视网膜无灌注区和新生血管的面积。【结果】病理检测视网膜新生血管面积:第一组为(0.51±0.08)mm2/鼠(n=7);第2组为(0.11±0.01)mm2/鼠(n=8);第3组为(0.16±0.02)mm2/鼠(n=8)。视网膜平片检测视网膜新生血管面积:第1组为(1.36土0.02)mm2/眼(n=32),第2组为(0.19±0.01)mm2/眼(n=28),第3组为(0.07±0.01)mm2/眼(n=28);视网膜平片检测视网膜无灌注区面积:第1组为(2.33±0.08)mm2/眼,第2组为(1.08±0.09)mm2/眼,第3组为(1.22±0.11)mm2/眼。经ANOVA分析,第2组和第3组分别与第1组比较,视网膜新生血管的面积和视网膜无灌注区的面积,均明显减少,差异有统计学意义(P<0.01)。【结论】两种环缩酚肽衍生物均能强效? 展开更多
关键词 环缩酚肽抑制 小鼠 血管增殖性视网膜病变 视网膜新生血管 视网膜无灌注
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Regression of choroidal neovascularization often precedes macular atrophy in eyes with neovascular age-related macular degeneration treated with vascular endothelial growth factor neutralizing proteins
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作者 Saleema Kherani Roomasa Channa +12 位作者 Adrienne W.Scott James T.Handa Akrit Sodhi Adam S.Wenick Ingrid Zimmer-Galler Sharon D.Solomon peter Gehlbach Mira M.Sachdeva Becky S.Sama Anam Akhlaq Olukemi Adeyemo Mustafa Iftikhar peter a.campochiaro 《Eye Science》 2024年第4期259-275,共17页
Aims:To identify incident macular atrophy and evaluate antecedent anatomic alterations in eyes with neovascular age-related macular degeneration(NVAMD)that were treated with anti-vascular endothelial growth factor(ant... Aims:To identify incident macular atrophy and evaluate antecedent anatomic alterations in eyes with neovascular age-related macular degeneration(NVAMD)that were treated with anti-vascular endothelial growth factor(anti-VEGF)agents.Methods:All patients treated with anti-VEGF agents for NVAMD by one of the authors during the 2014 calendar year who had follow up≥12 months had evaluation of all SD-OCT scans from first treatment(usually prior to 2014)to last follow up through June 2018.Results:The ascertainment procedure identified 342 eyes of 278 patients with NVAMD among which 47 developed macular atrophy.The median time from treatment initiation to development of macular atrophy was 29.6(interquartile range,17.7-43.4)months.Three macular alterations were identified in areas that developed atrophy(some eyes had more than one);collapse of a vascularized pigment epithelial detachment(PED)and regression of choroidal neovascularization(CNV)in 25 eyes,development of subretinal hyper-reflective material and/or subretinal fibrosis in 15 eyes,or atrophy occurring in association with large drusen and pigmentary changes resulting in an arc of atrophy in a pattern typically referred to as geographic atrophy in 13 eyes.Conclusions:These data suggest that in some instances CNV may compensate for choroidal ischemia and the loss of CNV may expose retinal pigmented epithelial cells and photoreceptors to ischemic damage and atrophy. 展开更多
关键词 macular atrophy wet AMD neovascular AMD ANTI-VEGF
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