2004
DOI: 10.1128/jvi.78.17.9343-9351.2004
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Change of Tropism of SL3-2 Murine Leukemia Virus, Using Random Mutational Libraries

Abstract: SL3-2 is a polytropic murine leukemia virus with a limited species tropism. We cloned the envelope gene of this virus, inserted it into a bicistronic vector, and found that the envelope protein differs from other, similar envelope proteins that also utilize the polytropic receptor (Xpr1) in that it is severely impaired in mediating infection of human and mink cells. We found that two adjacent amino acid mutations (G212R and I213T), located in a previously functionally uncharacterized segment of the surface sub… Show more

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Cited by 21 publications
(30 citation statements)
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References 38 publications
(37 reference statements)
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“…Since this insertion does not remove the ability of the AP@165 envelope protein to use its natural receptor, while insertion at position 86 completely inactivates the envelope function, the binding site for Xpr1 might be expected to be found on the other end of this surface, mostly in VRA and VR3. This is supported by our previous finding that two amino acid alterations at VR3 can enable SL3-2 to use Xpr1 in other species (4) (Fig. 7).…”
Section: Discussionsupporting
confidence: 77%
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“…Since this insertion does not remove the ability of the AP@165 envelope protein to use its natural receptor, while insertion at position 86 completely inactivates the envelope function, the binding site for Xpr1 might be expected to be found on the other end of this surface, mostly in VRA and VR3. This is supported by our previous finding that two amino acid alterations at VR3 can enable SL3-2 to use Xpr1 in other species (4) (Fig. 7).…”
Section: Discussionsupporting
confidence: 77%
“…SL3-2 envelope protein, because of its limited and ecotropiclike tropism, offers another candidate for a retargeting scaffold. This envelope belongs to the xenotropic-polytropic group but can infect only murine cells (4). Using it as a scaffold, we have produced a retargeted envelope protein that can infect through a heterologous receptor as well as its natural surface receptors.…”
Section: Discussionmentioning
confidence: 99%
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“…This specificity is frequently attributable the LTR regions (DesGroseillers and Jolicoeur, 1984a, b) although in some cases subtle mutations can also alter the tropism of the virus envelope proteins (Bahrami et al, 2004). A series of variants of the SL3-3 murine leukaemia virus that normally induces T-cell lymphomas have been shown to have altered oncogenic capabilities.…”
Section: Using Slow Transforming Retroviruses To Generate Other Tumoumentioning
confidence: 99%