热休克蛋白
转基因
荧光素酶
Fas配体
体内
分子生物学
热休克蛋白70
生物
腺相关病毒
基因表达
细胞凋亡
转染
重组DNA
基因
程序性细胞死亡
生物化学
生物技术
载体(分子生物学)
作者
Roy C. Smith,Marcelle Machluf,Peter Bromley,Anthony Atala,Kenneth Walsh
出处
期刊:Human Gene Therapy
[Mary Ann Liebert, Inc.]
日期:2002-04-10
卷期号:13 (6): 697-706
被引量:58
标识
DOI:10.1089/104303402317322267
摘要
Adenoviral vectors have been constructed that express the transgenes luciferase (Adeno-HSP-Luc) or Fas ligand (Adeno-HSP-FasL) under the control of the heat shock protein 70B (hsp70B) promoter. Cultures infected with Adeno-HSP-Luc transiently expressed high levels of luciferase after heat shock. When cultures infected with Adeno-HSP-FasL were maintained at 37 degrees C, no transgene expression was observed, but when cultures were exposed to heat stress, transgene expression resulted in apoptotic cell death. In vivo, transgene expression was induced by ultrasound-mediated heating of adenovirus-infected tissue. In mice or rats injected with the Adeno-HSP-Luc construct, high levels of localized expression of luciferase activity were observed in regions subjected to ultrasound-mediated irradiation. Adeno-HSP-FasL was administered systemically to mice via the tail vein to evaluate safety. Animals receiving Adeno-HSP-FasL in the absence of ultrasound treatment did not display liver toxicity, whereas animals receiving ultrasound treatment to induce the expression of Fas ligand from the hsp70B promoter had significant increases in serum levels of liver enzymes. These data demonstrate that combining the inducible hsp70B promoter with ultrasound induction allows safe local expression of cytotoxic genes with possible therapeutic utility.
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