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Nitric oxide-elicited resistance to anti-glioblastoma photodynamic therapy 被引量:1
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作者 Albert W.Girotti Jonathan M.Fahey Witold Korytowski 《Cancer Drug Resistance》 2020年第3期401-414,共14页
Glioblastoma multiforme is a highly aggressive primary brain malignancy that resists most conventional chemoand radiotherapeutic interventions.Nitric oxide(NO),a short lived free radical molecule produced by inducible... Glioblastoma multiforme is a highly aggressive primary brain malignancy that resists most conventional chemoand radiotherapeutic interventions.Nitric oxide(NO),a short lived free radical molecule produced by inducible NO synthase(iNOS)in glioblastomas and other tumors,is known to play a key role in tumor persistence,progression,and chemo/radiotherapy resistance.Site-specific and minimally invasive photodynamic therapy(PDT),based on oxidative damage resulting from non-ionizing photoactivation of a sensitizing agent,is highly effective against glioblastoma,but resistance also exists in this case.Studies in the authors’laboratory have shown that much of the latter is mediated by iNOS/NO.For example,when glioblastoma U87 or U251 cells sensitized in mitochondria with 5-aminolevulinic acid-induced protoporphyrin IX were exposed to a moderate dose of visible light,the observed apoptosis was strongly enhanced by an iNOS activity inhibitor or NO scavenger,indicating that iNOS/NO had increased cell resistance to photokilling.Moreover,cells that survived the photochallenge proliferated,migrated,and invaded more aggressively than controls,and these responses were also driven predominantly by iNOS/NO.Photostress-upregulated iNOS rather than basal enzyme was found to be responsible for all the negative effects described.Recognition of NO-mediated hyper-resistance/hyper-aggression in PDT-stressed glioblastoma has stimulated interest in how these responses can be prevented or at least minimized by pharmacologic adjuvants such as inhibitors of iNOS activity or transcription.Recent developments along these lines and their clinical potential for improving anti-glioblastoma PDT are discussed. 展开更多
关键词 GLIOBLASTOMA photodynamic therapy nitric oxide inducible nitric oxide synthase nitric oxide-mediated photodynamic therapy resistance anti-nitric oxide adjuvants
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糖基化产物对正常大鼠尿蛋白排泄和肾脏结构的影响 被引量:9
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作者 隋立荣 李才 +2 位作者 苗春生 邹雅斌 刘景英 《中华内分泌代谢杂志》 CAS CSCD 北大核心 1998年第4期260-262,共3页
目的为探讨糖基化产物对正常肾脏的特异性损害作用。方法正常大鼠静脉注射体外制备的糖基化血清蛋白(GSP),为期2个月,观察GSP对大鼠尿蛋白排泄、肾皮质糖基化产物和肾脏形态的影响。结果接受GSP的大鼠血清和肾组织中糖基... 目的为探讨糖基化产物对正常肾脏的特异性损害作用。方法正常大鼠静脉注射体外制备的糖基化血清蛋白(GSP),为期2个月,观察GSP对大鼠尿蛋白排泄、肾皮质糖基化产物和肾脏形态的影响。结果接受GSP的大鼠血清和肾组织中糖基化终产物(AGEs)水平、肾小球硝基四氮唑蓝(NBT)染色强度、尿蛋白排泄量和尿量均明显高于对照组。光学和电子显微镜观察显示,给予GSP的大鼠肾小球体积明显增大,肾小球系膜区扩大伴有细胞外基质增加,PAS阳性物质沉着增多和肾小球基底膜节段性增厚。结论糖基化产物能引起类似糖尿病肾病的肾脏损害。 展开更多
关键词 糖基化血清蛋白 糖尿病 糖尿病肾病
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