Literature DB >> 10074169

Amphotropic murine leukemia virus entry is determined by specific combinations of residues from receptor loops 2 and 4.

M D Lundorf1, F S Pedersen, B O'Hara, L Pedersen.   

Abstract

Pit2 is the human receptor for amphotropic murine leukemia virus (A-MuLV); the related human protein Pit1 does not support A-MuLV entry. Interestingly, chimeric proteins in which either the N-terminal or the C-terminal part of Pit2 was replaced by the Pit1 sequence all retained A-MuLV receptor function. A possible interpretation of these observations is that Pit1 harbors sequences which can specify A-MuLV receptor function when presented in a protein context other than Pit1, e.g., in Pit1-Pit2 hybrids. We reasoned that such Pit1 sequences might be identified if presented in the Neurospora crassa protein Pho-4. This protein is distantly related to Pit1 and Pit2, predicted to have a similar membrane topology with five extracellular loops, and does not support A-MuLV entry. We show here that introduction of the Pit1-specific loop 2 sequence conferred A-MuLV receptor function upon Pho-4. Therefore, we conclude that (i) a functional A-MuLV receptor can be constructed by combining sequences from two proteins each lacking A-MuLV receptor function and that (ii) a Pit1 sequence can specify A-MuLV receptor function when presented in another protein context than that provided by Pit1 itself. Previous results indicated a role of loop 4 residues in A-MuLV entry, and the presence of a Pit2-specific loop 4 sequence was found here to confer A-MuLV receptor function upon Pho-4. Moreover, the introduction of a Pit1-specific loop 4 sequence, but not of a Pit2-specific loop 4 sequence, abolished the A-MuLV receptor function of a Pho-4 chimera harboring the Pit1-specific loop 2 sequence. Together, these data suggest that residues in both loop 2 and loop 4 play a role in A-MuLV receptor function. A-MuLV is, however, not dependent on the specific Pit2 loop 2 and Pit2 loop 4 sequences for entry; rather, the role played by loops 2 and 4 in A-MuLV entry can be fulfilled by several different combinations of loop 2 and loop 4 sequences. We predict that the residues in loops 2 and 4, identified in this study as specifying A-MuLV receptor function, are to be found among those not conserved among Pho-4, Pit1, and Pit2.

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Year:  1999        PMID: 10074169      PMCID: PMC104079     

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


  31 in total

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Authors:  A D Miller; G J Rosman
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3.  Internal initiation of translation in retroviral vectors carrying picornavirus 5' nontranslated regions.

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4.  Nucleotide sequence of pho-4+, encoding a phosphate-repressible phosphate permease of Neurospora crassa.

Authors:  B J Mann; B J Bowman; J Grotelueschen; R L Metzenberg
Journal:  Gene       Date:  1989-11-30       Impact factor: 3.688

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Authors:  B D Leverett; K B Farrell; M V Eiden; C A Wilson
Journal:  J Virol       Date:  1998-06       Impact factor: 5.103

6.  A common progenitor for neurons and glia persists in rat retina late in development.

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Authors:  J R McLachlin; N Mittereder; M B Daucher; M Kadan; M A Eglitis
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8.  GLVR1, a receptor for gibbon ape leukemia virus, is homologous to a phosphate permease of Neurospora crassa and is expressed at high levels in the brain and thymus.

Authors:  S V Johann; J J Gibbons; B O'Hara
Journal:  J Virol       Date:  1992-03       Impact factor: 5.103

9.  Construction and properties of retrovirus packaging cells based on gibbon ape leukemia virus.

Authors:  A D Miller; J V Garcia; N von Suhr; C M Lynch; C Wilson; M V Eiden
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Journal:  J Virol       Date:  1992-02       Impact factor: 5.103
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  11 in total

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3.  A 13-amino-acid Pit1-specific loop 4 sequence confers feline leukemia virus subgroup B receptor function upon Pit2.

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Journal:  J Virol       Date:  2004-09       Impact factor: 5.103

8.  Identification of an extracellular domain within the human PiT2 receptor that is required for amphotropic murine leukemia virus binding.

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9.  Mapping of the minimal inorganic phosphate transporting unit of human PiT2 suggests a structure universal to PiT-related proteins from all kingdoms of life.

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