Skip to main content
OSTI.GOVU.S. Department of Energy Office of Scientific and Technical Information
U.S. Department of Energy
Office of Scientific and Technical Information
 

Sequence comparison in the crossover region of an oncogenic avian retrovirus recombinant and its nononcogenic parent: Genetic regions that control growth rate and oncogenic potential

Journal Article · · Mol. Cell. Biol.; (United States)
; ; ; ; ; ;

NTRE is an avian retrovirus recombinant of the endogeneous nononcogenic Rous-associated virus-0 (RAV-0) and the oncogenic, exogeneous, transformation-defective (td) Prague strain of Rous sarcoma virus B (td-PrRSV-B). Oligonucleotide mapping had shown that the recombinant virus is indistinguishable from its RAV-0 parent except for the 3'-end sequences, which were derived from td-PrRSV-B. However, the virus exhibits properties which are typical of an exogenous virus: it grows to high titers in tissue culture, and it is oncogenic in vivo. To accurately define the genetic region responsible for these properties, the authors determined the nucleotide sequences of the recombinant and its RAV-0 parent by using molecular clones of their DNA. These were compared with sequences already available for PrRSV-C, a virus closely related to the exogenous parent td-PrRSV-B. The results suggested that the crossover event which generated NTRE 7 took place in a region -501 to -401 nucleotides from the 3' end of the td-PrRSV parental genome and that sequences to the right of the recombination region were responsible for its growth properties and oncogenic potential. Since the exogenous-virus-specific sequences are expected to be missing from transformation-defective mutants of the Schmidt-Ruppin strain of RSV, which, like other exogeneous viruses, grow to high tiers in tissue culture and are oncogenic in vivo, the authors concluded that the growth properties and oncogenic potential of the exogeneous viruses are determined by sequences in the U3 region of the long terminal repeat. However, the authors propose that the exogeneous-virus-specific region may play a role in determining the oncogenic spectrum of a given oncogenic virus.

Research Organization:
Lab. of Tumor Virus Genetics, National Cancer Institute, Bethesda, MD 20205
OSTI ID:
5996595
Journal Information:
Mol. Cell. Biol.; (United States), Journal Name: Mol. Cell. Biol.; (United States) Vol. 2:11; ISSN MCEBD
Country of Publication:
United States
Language:
English

Similar Records

Defective C-type retrovirus particles secreted by L1210 leukemia cells
Journal Article · Thu Nov 30 23:00:00 EST 1978 · Cancer Res.; (United States) · OSTI ID:6002259
Characterization of some isolates of newly recovered avian sarcoma virus. [X Radiation]
Journal Article · Sun Dec 31 23:00:00 EST 1978 · J. Virol.; (United States) · OSTI ID:6433138
Generation of fibrosarcomas in vivo by a retrovirus that expresses the normal B chain of platelet-derived growth factor and mimics the alternative splice pattern of the v-sis oncogene
Journal Article · Fri Mar 31 23:00:00 EST 1989 · Proceedings of the National Academy of Sciences of the United States of America; (USA) · OSTI ID:5162359

Related Subjects

550200 -- Biochemistry
550400* -- Genetics
59 BASIC BIOLOGICAL SCIENCES
ANIMALS
BIRDS
CELL PROLIFERATION
CELL TRANSFORMATIONS
CLONING
CONTROL
DEFECTS
DNA
DNA SEQUENCING
DNA-CLONING
GENES
GENETIC CONTROL
GENETIC MAPPING
IN VIVO
MAPPING
MICROORGANISMS
MUTANTS
NUCLEIC ACIDS
OLIGONUCLEOTIDES
ONCOGENES
ONCOGENIC TRANSFORMATIONS
ONCOGENIC VIRUSES
ORGANIC COMPOUNDS
PARASITES
PEST CONTROL
RECOMBINANT DNA
STRUCTURAL CHEMICAL ANALYSIS
TISSUE CULTURES
VERTEBRATES
VIRUSES