K. Perk scite author profile

The biophysical and biochemical properties of the virus particles released by guinea pig embryo cells treated with 5-bromo-2'-deoxyuridine (BUdR) have been compared to those of the B-type mouse mammary tumor virus (MMTV) and the C-type Rauscher murine leukemia virus. The high-molecular-weight (60 to 70S) RNA of the BUdR-induced guinea pig virus (GPV) has a molecular weight of 8 x 106 when measured by mixed agarose polyacrylamide gel electrophoresis. The virus particles isolated from the tissue culture medium of BUdR-induced guinea pig cells have the following properties in common with MMTV: (i) a buoyant density of 1.18 g/ml in sucrose and 1.21 g/ml in CsCl, and (ii) a DNA polymerase that prefers Mg2+ over Mn2+ in an assay using the synthetic template poly(rC):oligo(dG). No nucleic acid sequence homology between GPV RNA and the viral RNAs of the MMTV, murine leukemia virus, hamster sarcoma virus, or Mason-Pfizer monkey virus could be observed in a competition hybridization assay using the radioactive-labeled GPV 60 to 70S RNA. By this same competition hybridization assay the frequency of GPV proviral sequences was estimated to be at least 83 per haploid cellular genome of guinea pig cells. No nucleic acid sequences related to the GPV RNA were detected in the DNA of normal tissues of mice, rats, cats, dogs, baboons, or humans by direct RNA-DNA hybridization using radioactive GPV 60 to 70S RNA.

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Morphological and immunological comparison of caprine arthritis encephalitis and ovine progressive pneumonia viruses

Dahlberg¹,

Gaskin²,

Perk³

1981

J Virol

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Caprine arthritis encephalitis virus (CAEV) causes a variety of pathological conditions ranging from mild to very severe and from acute to chronic, depending upon the age of initial infection and other variables. Although the virus has been reported to have properties characteristic of retroviruses and to be related to maedi-visna virus (also called progressive pneumonia virus [PPV]), relatively little information about its morphological and immunological characteristics has been reported. We describe the morphological features of CAEV replicating in cultured caprine cells. Although the virus replicates slowly and very little virus is released from productively infected cells, it is apparent that the morphogenesis of CAEV is strikingly similar to that of maedi-visna. After the transmission of CAEV to a more permissive permanent cell line derived from Himalayan tahr ovary, it was possible to grow and purify enough virus to initiate biochemical characterization. The structural proteins of CAEV are generally very similar to those of PPV, suggesting that the two viruses are closely related but not identical. This was substantiated by showing that serum from a CAEV-infected goat immunoprecipitated both CAEV and PPV virion structural antigens from extracts of radiolabeled virus and also precipitated putative nonstructural viral antigens from extracts of both CAEV-and PPV-infected cells.

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The Camel's Erythrocyte

Perk

1963

Nature

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Biological, pathological and physical characterization of a possible variant of a murine sarcoma virus (Moloney)

Chirigos

Scott

Turner

et al. 1968

Intl Journal of Cancer

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K. Perk

Reovirus infection of young muscovy ducks(Cairina Moschata)

Biochemical properties of the bromodeoxyuridine-induced guinea pig virus

Morphological and immunological comparison of caprine arthritis encephalitis and ovine progressive pneumonia viruses

The Camel's Erythrocyte

Biological, pathological and physical characterization of a possible variant of a murine sarcoma virus (Moloney)

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