The effect of the human papillomaviral (HPV) oncogenes E6 and E7 was examined in transgenic mice with a construct containing the human beta-actin promoter regulating HPV16 E6 and E7 open reading frames. In the sole line of mice that transmitted the transgene, neuroepithelial tumors appeared at 2.5 mouths of life, and by 10 mouths, 87 of 122 (71%) of the animals were dead from brain tumors. The most frequent type of tumor (74%) was an anaplastic neuroepithelial tumor associated with the ependyma of the third and fourth ventricles, which locally invaded adjacent brain tissue and spread for considerable distances along the ventricular surface. The other two types of tumors were well-differentiated choroid plexus carcinomas (26%) and rare pituitary carcinomas (8.7%). HPV16 E6 P-NA and E7 oncoprotein expression were demonstrated in tumor tissue and primary cell lines derived from the tumors. Examination of two tumor suppressor gene products, the retinoblastoma protein and p53, known to bind to HPV16 E7 and E6 oncoproteins, respectively, showed both were expressed in the primary tumor cell lines. These data support a causative role for the HPV oncoproteins in epithelial carcinogenesis.
机构:
MEM UNIV NEWFOUNDLAND, FAC MED, DIV BASIC MED SCI, ST JOHNS, NF A1B 3V6, CANADAMEM UNIV NEWFOUNDLAND, FAC MED, DIV BASIC MED SCI, ST JOHNS, NF A1B 3V6, CANADA
BELAGULI, NS
PATER, MM
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机构:
MEM UNIV NEWFOUNDLAND, FAC MED, DIV BASIC MED SCI, ST JOHNS, NF A1B 3V6, CANADAMEM UNIV NEWFOUNDLAND, FAC MED, DIV BASIC MED SCI, ST JOHNS, NF A1B 3V6, CANADA
PATER, MM
PATER, A
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MEM UNIV NEWFOUNDLAND, FAC MED, DIV BASIC MED SCI, ST JOHNS, NF A1B 3V6, CANADAMEM UNIV NEWFOUNDLAND, FAC MED, DIV BASIC MED SCI, ST JOHNS, NF A1B 3V6, CANADA