Literature DB >> 23903838

The surface glycoprotein of feline leukemia virus isolate FeLV-945 is a determinant of altered pathogenesis in the presence or absence of the unique viral long terminal repeat.

Lisa L Bolin1, Shamim Ahmad, Patricia A Lobelle-Rich, Tara G Ooms, Xavier Alvarez-Hernandez, Peter J Didier, Laura S Levy.   

Abstract

Feline leukemia virus (FeLV) is a naturally transmitted gammaretrovirus that infects domestic cats. FeLV-945, the predominant isolate associated with non-T-cell disease in a natural cohort, is a member of FeLV subgroup A but differs in sequence from the FeLV-A prototype, FeLV-A/61E, in the surface glycoprotein (SU) and long terminal repeat (LTR). Substitution of the FeLV-945 LTR into FeLV-A/61E resulted in pathogenesis indistinguishable from that of FeLV-A/61E, namely, thymic lymphoma of T-cell origin. In contrast, substitution of both FeLV-945 LTR and SU into FeLV-A/61E resulted in multicentric lymphoma of non-T-cell origin. These results implicated the FeLV-945 SU as a determinant of pathogenic spectrum. The present study was undertaken to test the hypothesis that FeLV-945 SU can act in the absence of other unique sequence elements of FeLV-945 to determine the disease spectrum. Substitution of FeLV-A/61E SU with that of FeLV-945 altered the clinical presentation and resulted in tumors that demonstrated expression of CD45R in the presence or absence of CD3. Despite the evident expression of CD45R, a typical B-cell marker, T-cell receptor beta (TCRβ) gene rearrangement indicated a T-cell origin. Tumor cells were detectable in bone marrow and blood at earlier times during the disease process, and the predominant SU genes from proviruses integrated in tumor DNA carried markers of genetic recombination. The findings demonstrate that FeLV-945 SU alters pathogenesis, although incompletely, in the absence of FeLV-945 LTR. Evidence demonstrates that FeLV-945 SU and LTR are required together to fully recapitulate the distinctive non-T-cell disease outcome seen in the natural cohort.

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Year:  2013        PMID: 23903838      PMCID: PMC3807393          DOI: 10.1128/JVI.01130-13

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  35 in total

1.  The FeLV-945 LTR confers a replicative advantage dependent on the presence of a tandem triplication.

Authors:  S Prabhu; P A Lobelle-Rich; L S Levy
Journal:  Virology       Date:  1999-10-25       Impact factor: 3.616

Review 2.  Receptors and entry cofactors for retroviruses include single and multiple transmembrane-spanning proteins as well as newly described glycophosphatidylinositol-anchored and secreted proteins.

Authors:  J Overbaugh; A D Miller; M V Eiden
Journal:  Microbiol Mol Biol Rev       Date:  2001-09       Impact factor: 11.056

3.  Selection forces and constraints on retroviral sequence variation.

Authors:  J Overbaugh; C R Bangham
Journal:  Science       Date:  2001-05-11       Impact factor: 47.728

4.  Feline leukaemia virus LTR variation and disease association in a geographical and temporal cluster.

Authors:  Chandtip Chandhasin; Patricia Lobelle-Rich; Laura S Levy
Journal:  J Gen Virol       Date:  2004-10       Impact factor: 3.891

5.  Determinants of the host range of feline leukaemia viruses.

Authors:  O Jarrett; H M Laird; D Hay
Journal:  J Gen Virol       Date:  1973-08       Impact factor: 3.891

6.  Differential pathogenicity of two feline leukemia virus subgroup A molecular clones, pFRA and pF6A.

Authors:  A J Phipps; H Chen; K A Hayes; P Roy-Burman; L E Mathes
Journal:  J Virol       Date:  2000-07       Impact factor: 5.103

7.  Presence of B220 within thymocytes and its expression on the cell surface during apoptosis.

Authors:  S Oka; N Mori; S Matsuyama; Y Takamori; K Kubo
Journal:  Immunology       Date:  2000-08       Impact factor: 7.397

8.  Surface antigen expression and immunoglobulin gene rearrangement during mouse pre-B cell development.

Authors:  R L Coffman
Journal:  Immunol Rev       Date:  1982       Impact factor: 12.988

Review 9.  Viral determinants of FeLV infection and pathogenesis: lessons learned from analysis of a natural cohort.

Authors:  Lisa L Bolin; Laura S Levy
Journal:  Viruses       Date:  2011-09-09       Impact factor: 5.048

10.  CD11c(+)B220(+)Gr-1(+) cells in mouse lymph nodes and spleen display characteristics of plasmacytoid dendritic cells.

Authors:  H Nakano; M Yanagita; M D Gunn
Journal:  J Exp Med       Date:  2001-10-15       Impact factor: 14.307

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