Feline leukemia virus variants in experimentally induced thymic lymphosarcomas

被引：12

作者：

Pandey, R

Bechtel, MK

Su, Y

Ghosh, AK

Hayes, KA

Mathes, LE

RoyBurman, P

机构：

[1] UNIV SO CALIF,SCH MED,DEPT PATHOL,LOS ANGELES,CA 90033

[2] UNIV SO CALIF,SCH MED,DEPT BIOCHEM & MOLEC BIOL,LOS ANGELES,CA 90033

[3] OHIO STATE UNIV,CTR RETROVIRUS RES,COLUMBUS,OH 43210

[4] OHIO STATE UNIV,DEPT VET BIOSCI,COLUMBUS,OH 43210

来源：

VIROLOGY | 1995年 / 214卷 / 02期

关键词：

D O I：

10.1006/viro.1995.0069

中图分类号：

Q93 [微生物学];

学科分类号：

071005 ; 100705 ;

摘要：

This study was initiated to evaluate the in vivo infectivity and pathogenicity of a group of recombinant feline leukemia viruses (rFeLVs) previously generated by in vitro forced recombination between a FeLV subgroup A virus (FeLV-A) and an endogenous FeLV (enFeLV) envelope (env) element (Sheets et al, 1992, Virology 190, 849-855). To determine infectivity of rFelVs, neonatal cats were inoculated with rFelVs alone or in combination with feLV-A. The recombinant viruses were able to replicate efficiently in vivo only when administered along with FeLV-A. Of six cc-infected cats, three developed thymic lymphosarcomas, one severe aplastic anemia, and two cachexia and depression; all were viremic and seroconverted shortly after inoculation. While both virus types were detected in virtually all tissues examined from these tumor-bearing cats, there was a particularly noteworthy sequence reversion in the rFeLVs. It is known that exogenous FeLV isolates carry a conserved neutralizing MGPNL epitope in the middle of the surface glycoprotein domain of the env gene. In contrast, the parental recombinant viruses used to inoculate these cats harbored the enFeLV-derived MGPNP-sequence at this position. However, all in vivo-propagated recombinants displayed the MGPNL sequence, while the env-encoded backbone flanking the MGPNL sequence was that of the parental recombinant virus. These results suggest that viruses with the MGPNL epitope have an in vivo proliferative advantage. The data also provide an explanation for the conservation of this epitope in exogenous FeLVs despite the existence of variant forms in enFeLV proviral elements with which they can recombine. (C) 1995 Academic Press, Inc.

引用

页码：584 / 592

页数：9

共 38 条

[1] ABNORMAL PROCESSING OF A RECOMBINANT FELINE LEUKEMIA-VIRUS ENVELOPE POLYPROTEIN AND ITS INTERFERENCE WITH SUBGROUP-C VIRUS-INFECTION
BECHTEL, MK
STALLCUP, MR
BEDGOOD, RM
COREY, JL
PANDEY, R
ROYBURMAN, P
[J]. VIROLOGY, 1994, 202 (01) : 329 - 338
[2] CHAKRABARTI R, 1994, AM J PATHOL, V144, P348
[3] ISOLATION OF BIOLOGICALLY-ACTIVE RIBONUCLEIC-ACID FROM SOURCES ENRICHED IN RIBONUCLEASE
CHIRGWIN, JM
PRZYBYLA, AE
MACDONALD, RJ
RUTTER, WJ
[J]. BIOCHEMISTRY, 1979, 18 (24) : 5294 - 5299
[4] CHOMCZYNSKI P, 1987, ANAL BIOCHEM, V162, P156, DOI 10.1016/0003-2697(87)90021-2
[5] STRONG SEQUENCE CONSERVATION AMONG HORIZONTALLY TRANSMISSIBLE, MINIMALLY PATHOGENIC FELINE LEUKEMIA VIRUSES
DONAHUE, PR
HOOVER, EA
BELTZ, GA
RIEDEL, N
HIRSCH, VM
OVERBAUGH, J
MULLINS, JI
[J]. JOURNAL OF VIROLOGY, 1988, 62 (03) : 722 - 731
[6] NUCLEOTIDE-SEQUENCE OF THE ENVELOPE GENE OF GARDNER-ARNSTEIN FELINE LEUKEMIA VIRUS-B REVEALS UNIQUE SEQUENCE HOMOLOGIES WITH A MURINE MINK CELL FOCUS-FORMING VIRUS
ELDER, JH
MULLINS, JI
[J]. JOURNAL OF VIROLOGY, 1983, 46 (03) : 871 - 880
[7] LOCALIZATION OF NEUTRALIZING REGIONS OF THE ENVELOPE GENE OF FELINE LEUKEMIA-VIRUS BY USING ANTISYNTHETIC PEPTIDE ANTIBODIES
ELDER, JH
MCGEE, JS
MUNSON, M
HOUGHTEN, RA
KLOETZER, W
BITTLE, JL
GRANT, CK
[J]. JOURNAL OF VIROLOGY, 1987, 61 (01) : 8 - 15
[8] CORRELATION BETWEEN HUMORAL ANTIBODY AND REGRESSION OF TUMOURS INDUCED BY FELINE SARCOMA VIRUS
ESSEX, M
KLEIN, G
SNYDER, SP
HARROLD, JB
[J]. NATURE, 1971, 233 (5316) : 195 - &
[9] SIMPLE, QUANTITATIVE ASSAY FOR BOTH XENOTROPIC MURINE LEUKEMIA AND ECOTROPIC FELINE LEUKEMIA VIRUSES
FISCHINGER, PJ
BLEVINS, CS
NOMURA, S
[J]. JOURNAL OF VIROLOGY, 1974, 14 (01) : 177 - 179
[10] GRANT CK, 1983, J IMMUNOL, V131, P3042

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