Abstract

Previously, we found that Friend plan spleen focus forming virus (SFFV) encodes a membranes glycoprotein (gp55) which is structurally related to the larger env gene products of recombinant-type dualtropic MCF viruses, that gp55 causes mitosis of infected erythroblasts, and that the xeno- and eco- related portions of gp55 fold into separate globular domains connected by a proline-rich joint. Our recent results suggest that the xeno-related domain of plasma membranal gp55 contains an active site that binds to MCF receptors (and perhaps to other structurally related membrane components) to trigger erythroblast proliferation. Thus, a leukemogenic receptor may be related or identical to MCF receptors. To objectively study these issues, the following approaches are proposed: (i) Analyze additional site-directed SFFV env mutants that we have constructed. These cause different in-frame focal lesions. (ii) Previously, we found that SFFV env genes can change rapidly and that nonleukemogenic mutants often form revertants in vivo. Sets of revertants with second-site env mutations will be molecularly cloned and sequenced. In (i) and (ii), we will identify gp55 active sites and correlate pathogenesis with subcellular localization and with MCF interference. (iii) Soluble forms of gp55 will be made and their biological effects, including binding to cell surface receptors and MCF and growth factor interferences, will be studied. (iv) The xeno-related sequences of Friend SFFV will be substituted for the homologous sequences of a Friend MCF, and the recombinant will be analyzed for replication conpetency. (v) We constructed a pathogenic SFFV with an inserted """"""""tag"""""""" of foreign nucleic acid. This will be used to study SFFV integration sites and leukemic progression in the absence of a helper virus. (vi) Using different strategies, identify cell surface receptor(s) for gp55 and molecularly clone receptor gene(s). Our finding that Friend erythroleukemia is a primary membrane abnormality deserves thorough investigation. Retroviral env gp's have been increasingly implicated in leukemogenesis and in immunosuppression. Our objective has broad relevance for cancer research: to understand how an abnormality of cell membranes can cause premalignant hyperplasia that progresses to overt cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA025810-13
Application #
3167025
Study Section
Virology Study Section (VR)
Project Start
1979-08-01
Project End
1992-05-31
Budget Start
1991-06-01
Budget End
1992-05-31
Support Year
13
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
Oregon Health and Science University
Department
Type
Schools of Medicine
DUNS #
009584210
City
Portland
State
OR
Country
United States
Zip Code
97239

  Publications

Tailor, C S; Lavillette, D; Marin, M et al. (2003) Cell surface receptors for gammaretroviruses. Curr Top Microbiol Immunol 281:29-106
Marin, Mariana; Lavillette, Dimitri; Kelly, Sean M et al. (2003) N-linked glycosylation and sequence changes in a critical negative control region of the ASCT1 and ASCT2 neutral amino acid transporters determine their retroviral receptor functions. J Virol 77:2936-45
Lavillette, Dimitri; Marin, Mariana; Ruggieri, Alessia et al. (2002) The envelope glycoprotein of human endogenous retrovirus type W uses a divergent family of amino acid transporters/cell surface receptors. J Virol 76:6442-52
Tailor, C S; Marin, M; Nouri, A et al. (2001) Truncated forms of the dual function human ASCT2 neutral amino acid transporter/retroviral receptor are translationally initiated at multiple alternative CUG and GUG codons. J Biol Chem 276:27221-30
Tailor, C S; Nouri, A; Kabat, D (2000) Cellular and species resistance to murine amphotropic, gibbon ape, and feline subgroup C leukemia viruses is strongly influenced by receptor expression levels and by receptor masking mechanisms. J Virol 74:9797-801
Marin, M; Tailor, C S; Nouri, A et al. (2000) Sodium-dependent neutral amino acid transporter type 1 is an auxiliary receptor for baboon endogenous retrovirus. J Virol 74:8085-93
Tailor, C S; Nouri, A; Kabat, D (2000) A comprehensive approach to mapping the interacting surfaces of murine amphotropic and feline subgroup B leukemia viruses with their cell surface receptors. J Virol 74:237-44
Tailor, C S; Nouri, A; Zhao, Y et al. (1999) A sodium-dependent neutral-amino-acid transporter mediates infections of feline and baboon endogenous retroviruses and simian type D retroviruses. J Virol 73:4470-4
Tailor, C S; Willett, B J; Kabat, D (1999) A putative cell surface receptor for anemia-inducing feline leukemia virus subgroup C is a member of a transporter superfamily. J Virol 73:6500-5
Marin, M; Tailor, C S; Nouri, A et al. (1999) Polymorphisms of the cell surface receptor control mouse susceptibilities to xenotropic and polytropic leukemia viruses. J Virol 73:9362-8

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