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Functional 20S Proteasomes in Retroviruses: Evidence in Favor
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Proteasomes are barrel-like cellular protein complexes responsible for the degradation of most intracellular proteins. Earlier, it has been shown that during assembly, hundreds of different cellular proteins are incorporated into retro-and herpes viruses. Among detected cellular proteins, there were different proteasome subunits (PS). Previous reports postulated the incorporation of 20S proteasome subunits and subunits of proteasome regulator complexes inside retroviruses. Here, we demonstrated the association of functional 20S proteasome with gammaretroviruses, betaretroviruses, and lentiviruses. Cleaved proteasome subunits β1, β2 and β5 were detected in tested viruses. Using fluorescent peptides and a cell-permeable proteasome activity probe, proteasome activity was detected in endogenous and exogenous retroviruses, including recombinant HIV-1. Taken together, our data favors the insertion of functional proteasomes into the retroviruses during assembly. The possible role of proteasomes in retroviruses is discussed.
Title: Functional 20S Proteasomes in Retroviruses: Evidence in Favor
Description:
Proteasomes are barrel-like cellular protein complexes responsible for the degradation of most intracellular proteins.
Earlier, it has been shown that during assembly, hundreds of different cellular proteins are incorporated into retro-and herpes viruses.
Among detected cellular proteins, there were different proteasome subunits (PS).
Previous reports postulated the incorporation of 20S proteasome subunits and subunits of proteasome regulator complexes inside retroviruses.
Here, we demonstrated the association of functional 20S proteasome with gammaretroviruses, betaretroviruses, and lentiviruses.
Cleaved proteasome subunits β1, β2 and β5 were detected in tested viruses.
Using fluorescent peptides and a cell-permeable proteasome activity probe, proteasome activity was detected in endogenous and exogenous retroviruses, including recombinant HIV-1.
Taken together, our data favors the insertion of functional proteasomes into the retroviruses during assembly.
The possible role of proteasomes in retroviruses is discussed.
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