The inability of in vitro transforming SV40 subgenomes to cause tumors in vivo

Mary Pat Moyer; Helen Arizpe; Aurora Sosa; Katia Pierson; Rex C. Moyer

doi:10.1159/000149506

The inability of in vitro transforming SV40 subgenomes to cause tumors in vivo

Mary Pat Moyer, Helen Arizpe, Aurora Sosa, Katia Pierson, Rex C. Moyer

Producción científica: Article › revisión exhaustiva

Resumen

Linear or subgenomic SV40 DNAs were transfected into cells from a variety of species (including rodent, dog, muntjak, and monkey) and injected subcutaneously into neonate Syrian hamsters for tumorigenicity testing. The 'early-region' subgenomes were capable of transforming cells in vitro. Complete genomes or complementary subgenomes could transform non- permissive and semipermissive cells, were infectious for permissive cells, and induced tumors from which infectious virus could be rescued. Tumors were not formed in neonate hamsters upon injection with subgenomic SV40 DNAs, even those capable of transforming cells in vitro. These results suggested that SV40 tumor formation in vivo may require a complete genome.

Idioma original	English (US)
Páginas (desde-hasta)	87-95
Número de páginas	9
Publicación	Intervirology
Volumen	21
N.º	2
DOI	https://doi.org/10.1159/000149506
Estado	Published - 1984

ASJC Scopus subject areas

Virology
Infectious Diseases

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title = "The inability of in vitro transforming SV40 subgenomes to cause tumors in vivo",

abstract = "Linear or subgenomic SV40 DNAs were transfected into cells from a variety of species (including rodent, dog, muntjak, and monkey) and injected subcutaneously into neonate Syrian hamsters for tumorigenicity testing. The 'early-region' subgenomes were capable of transforming cells in vitro. Complete genomes or complementary subgenomes could transform non- permissive and semipermissive cells, were infectious for permissive cells, and induced tumors from which infectious virus could be rescued. Tumors were not formed in neonate hamsters upon injection with subgenomic SV40 DNAs, even those capable of transforming cells in vitro. These results suggested that SV40 tumor formation in vivo may require a complete genome.",

keywords = "Papovaviruses, Recombinant DNA techniques, Restriction enzymes, SV40, Transformation, Tumorigenesis, Virus production",

author = "Moyer, {Mary Pat} and Helen Arizpe and Aurora Sosa and Katia Pierson and Moyer, {Rex C.}",

year = "1984",

doi = "10.1159/000149506",

language = "English (US)",

volume = "21",

pages = "87--95",

journal = "Intervirology",

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T1 - The inability of in vitro transforming SV40 subgenomes to cause tumors in vivo

AU - Moyer, Mary Pat

AU - Arizpe, Helen

AU - Sosa, Aurora

AU - Pierson, Katia

AU - Moyer, Rex C.

PY - 1984

Y1 - 1984

N2 - Linear or subgenomic SV40 DNAs were transfected into cells from a variety of species (including rodent, dog, muntjak, and monkey) and injected subcutaneously into neonate Syrian hamsters for tumorigenicity testing. The 'early-region' subgenomes were capable of transforming cells in vitro. Complete genomes or complementary subgenomes could transform non- permissive and semipermissive cells, were infectious for permissive cells, and induced tumors from which infectious virus could be rescued. Tumors were not formed in neonate hamsters upon injection with subgenomic SV40 DNAs, even those capable of transforming cells in vitro. These results suggested that SV40 tumor formation in vivo may require a complete genome.

AB - Linear or subgenomic SV40 DNAs were transfected into cells from a variety of species (including rodent, dog, muntjak, and monkey) and injected subcutaneously into neonate Syrian hamsters for tumorigenicity testing. The 'early-region' subgenomes were capable of transforming cells in vitro. Complete genomes or complementary subgenomes could transform non- permissive and semipermissive cells, were infectious for permissive cells, and induced tumors from which infectious virus could be rescued. Tumors were not formed in neonate hamsters upon injection with subgenomic SV40 DNAs, even those capable of transforming cells in vitro. These results suggested that SV40 tumor formation in vivo may require a complete genome.

KW - Papovaviruses

KW - Recombinant DNA techniques

KW - Restriction enzymes

KW - SV40

KW - Transformation

KW - Tumorigenesis

KW - Virus production

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U2 - 10.1159/000149506

DO - 10.1159/000149506

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JO - Intervirology

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The inability of in vitro transforming SV40 subgenomes to cause tumors in vivo

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