Growth-inhibitory effect of adenovirus-mediated p53 gene transfer on medulloblastoma cell line, Daoy, harboring mutant p53

被引:0
|
作者
Seung-Hoon Lee
Hee-Seog Kang
Chang-Hun Rhee
Mi-Sook Kim
Hee Chung Kwon
Myoun-Jin Park
In-Chul Park
Choon-Taek Lee
Chang Min Kim
Seok-Il Hong
机构
[1] Laboratory of Cell Biology,
[2] Korea Cancer Center Hospital,undefined
[3] 215–4,undefined
[4] Nowon-Ku,undefined
[5] Gongneung-Dong,undefined
[6] 139–706 Seoul,undefined
[7] Korea,undefined
[8] Department of Neurosurgery,undefined
[9] Korea Cancer Center Hospital,undefined
[10] Seoul,undefined
[11] Korea,undefined
[12] Neurooncology Clinic,undefined
[13] National Cancer Center,undefined
[14] 809 Madudong,undefined
[15] Ilsan-gu,undefined
[16] Koyang,undefined
[17] Kyonggi,undefined
[18] 411–351,undefined
[19] Korea e-mail: nslsh@mail.kcch.re.kr Tel.: +82-31-920-1660 Fax: +82-31-920-1520,undefined
[20] Laboratory of Molecular Oncology,undefined
[21] Korea Cancer Center Hospital,undefined
[22] Seoul,undefined
[23] Korea,undefined
[24] Department of Internal Medicine and Lung Institute,undefined
[25] Seoul National University,undefined
[26] College of Medicine,undefined
[27] Seoul,undefined
[28] Korea,undefined
来源
Child's Nervous System | 2001年 / 17卷
关键词
Keywords Gene therapy; p53; Adenovirus; Medulloblastoma;
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学科分类号
摘要
To improve the survival rate, gene therapy, such as the replacement of inactivated tumor suppressor genes, has become a new investigational adjuvant treatment modality for human malignancies. We investigated the effect of adenovirus(Ad)-mediated transfer of wild-type p53 tumor suppressor gene on the medulloblastoma cell line, Daoy, which harbors mutant-type p53 gene. At 50 multiplicity of infection (moi), immunohistochemical staining with p53 monoclonal antibody showed positive staining in all cells 2 days after Ad-CMV-p53 infection. The high expression of wild-type p53 protein was detected in Ad-CMV-p53-infected cells, and expression of wild-type p53 protein peaked on day 2 after the infection. The growth of Ad-CMV-p53-infected cells was greatly suppressed in vitro, and the Ad-CMV-p53 treatment significantly reduced the tumor mass in vivo. The mean weight of Ad-CMV- infected tumors was only 16% of those which were mock infected, and 25% of those which were Ad-CMV-β-gal infected. On microscopic examination, Ad-CMV-p53-infected tumors showed numerous apoptotic bodies. This Ad-CMV-p53 gene transfer showed high transduction efficacy and expression, resulting in significant growth inhibition of Daoy harboring mutant type p53.
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页码:134 / 138
页数:4
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