The Human c- ras 1 H Oncogene: a Mutation in Normal and Neoplastic Tissue from the Same Patient
- 18 February 1983
- journal article
- retracted article
- Published by American Association for the Advancement of Science (AAAS) in Science
- Vol. 219 (4586) , 853-856
- https://doi.org/10.1126/science.6337398
Abstract
The c-ras1H oncogene can be distinguished from its normal cellular counterpart by the loss of a restriction endonuclease site. This sequence alteration is the basis of a rapid screening method for the presence of this oncogene. DNA's from 34 individuals were screened by this method, and all were homozygous for the normal allele. In contrast, DNA from a patient's bladder tumor, as well as DNA from his normal bladder and leukocytes, were heterozygous at that restriction endonuclease site. Further restriction enzyme mapping pinpointed the change in the mutant allele as being one of two nucleotides, either of which would change the 12th amino acid (glycine) in the normal c-ras1H gene product. Point mutations in the codon for this amino acid have previously been described in a bladder tumor cell line and in the viral oncogene v-rasH. These results indicate that the patient carried a c-ras1H oncogene in his germ line, raising the possibility that the c-ras1H oncogene confers a predisposition to neoplasia.This publication has 27 references indexed in Scilit:
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