A structurally plastic ribonucleoprotein complex mediates post‐transcriptional gene regulation in <scp>HIV</scp>‐1

Fernandes, Jason D; Booth, David S.; Frankel, Alan D.

doi:10.1002/wrna.1342

Cited by 27 publications

(20 citation statements)

References 120 publications

(192 reference statements)

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“…However, the virus has found many solutions to maximize the information contained in its genome, such as using an adaptable Rev monomer to assemble a higher order oligomeric RNA export complex59. We believe that the post-translational ubiquitination of Tat represents another viral strategy of genetic multi-tasking.…”

Section: Discussionmentioning

confidence: 99%

PJA2 ubiquitinates the HIV-1 Tat protein with atypical chain linkages to activate viral transcription

Faust

Jang

et al. 2017

Sci Rep

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Transcription complexes that assemble at the HIV-1 promoter efficiently initiate transcription but generate paused RNA polymerase II downstream from the start site. The virally encoded Tat protein hijacks positive transcription elongation factor b (P-TEFb) to phosphorylate and activate this paused polymerase. In addition, Tat undergoes a series of reversible post-translational modifications that regulate distinct steps of the transcription cycle. To identify additional functionally important Tat cofactors, we performed RNAi knockdowns of sixteen previously identified Tat interactors and found that a novel E3 ligase, PJA2, ubiquitinates Tat in a non-degradative manner and specifically regulates the step of HIV transcription elongation. Interestingly, several different lysine residues in Tat can function as ubiquitin acceptor sites, and variable combinations of these lysines support both full transcriptional activity and viral replication. Further, the polyubiquitin chain conjugated to Tat by PJA2 can itself be assembled through variable ubiquitin lysine linkages. Importantly, proper ubiquitin chain assembly by PJA2 requires that Tat first binds its P-TEFb cofactor. These results highlight that both the Tat substrate and ubiquitin modification have plastic site usage, and this plasticity is likely another way in which the virus exploits the host molecular machinery to expand its limited genetic repertoire.

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Section: Discussionmentioning

confidence: 99%

PJA2 ubiquitinates the HIV-1 Tat protein with atypical chain linkages to activate viral transcription

Faust

Jang

et al. 2017

Sci Rep

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“…Relaxed‐specificity ARMs and RNAs have been found that transit recognition strategies between distinct lentiviral Tat‐TAR interactions and between distinct lambdoid N‐boxB interactions . Like Rev‐RRE, Tat‐TAR and N‐boxB interactions are characterized by disordered proteins binding RNAs sites with conformational flexibility, a feature of RNA‐protein interactions relating to their role in complex, fine‐tuned regulation …”

Section: Discussionmentioning

confidence: 91%

“…HIV Rev is a small, 114 amino acid, essential regulatory protein that mediates the nuclear export of incompletely spliced viral transcripts that contain a large, structured RNA, the Rev‐response element (RRE) . Rev initially binds to a high‐affinity site in RRE region IIB (IIB) via its ARM that comprises residues 34 to 50, and then Rev binds to secondary sites with multimerization and further conformational changes followed by recruitment of host factors that mediate export …”

Section: Introductionmentioning

confidence: 99%

Altered‐specificity mutants of the HIV Rev arginine‐rich motif‐RRE IIB interaction

Raad

Ghattas

Amano

et al. 2020

J of Molecular Recognition

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Arginine-rich motifs (ARMs) bind RNA structures with high affinity and specificity, and the human immunodeficiency virus (HIV) exploits ARM-RNA interactions to regulate its lifecycle. The expression of HIV structural genes relies on recognition between the ARM of its Rev protein and its primary binding site, an internal loop in the viral RNA, the Rev-response element region IIB (IIB). Many functional variants of the Rev ARM-IIB interaction have been discovered, yet how easily it can evolve new specificities is poorly explored. A double mutant of Rev ARM, R35G-N40 V, uses an unknown strategy to recognize IIB. Here, isothermal titration calorimetry and gel shift assays show that the R35G-N40V-IIB interaction has high affinity and specificity in vitro and a larger unfavorable entropy change upon binding than that of wild-type Rev ARM-IIB. In stark contrast with the critical dependence of wild-type Rev on Arg35, Arg39, Asn40, and Arg44, mutational profiling shows R35G-N40V is highly mutable at positions 40 and 44 and dependent on Gly35, Arg38, Arg39, Arg42, and Arg43. Affinity measurements in vitro and reporter assay measurements in vivo are consistent with the wild-type Rev ARM and R35G-N40V maintaining their recognition strategies when binding IIB mutants specific to wild-type Rev ARM and R35G-N40V, respectively. Some single amino acid mutants of wild-type Rev ARM and R35G-N40V have enhanced specificity, recognizing mutant IIBs yet not wild-type IIB.These results provide another example of viral ARM-RNA interactions evolving new specificities with few mutations, consistent with neutral theories of evolution. K E Y W O R D Saltered specificity, arginine-rich motif, disordered protein, fitness landscape, HIV Rev, neutral evolution, RNA-protein interaction

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“…Complex retroviruses such as human immunodeficiency virus (HIV) and human T-cell lymphotropic virus (HTLV) were initially shown to encode regulatory proteins (Rev and Rex) that facilitate this process by binding to cis -acting elements in the viral mRNAs that retain introns (for reviews, see Pollard and Malim, 1998; Shida, 2012; Fernandes et al ., 2016). Rev and Rex then recruit chromosome region maintenance 1/exportin 1, a cellular export receptor, enabling nucleocytoplasmic export (Fornerod et al ., 1997; Booth et al ., 2014).…”

Section: Introductionmentioning

confidence: 99%

AnNXF1mRNA with a retained intron is expressed in hippocampal and neocortical neurons and is translated into a protein that functions as an Nxf1 cofactor

Bor

Fitzgerald

et al. 2016

MBoC

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A structurally plastic ribonucleoprotein complex mediates post‐transcriptional gene regulation in HIV‐1

Cited by 27 publications

References 120 publications

PJA2 ubiquitinates the HIV-1 Tat protein with atypical chain linkages to activate viral transcription

PJA2 ubiquitinates the HIV-1 Tat protein with atypical chain linkages to activate viral transcription

Altered‐specificity mutants of the HIV Rev arginine‐rich motif‐RRE IIB interaction

AnNXF1mRNA with a retained intron is expressed in hippocampal and neocortical neurons and is translated into a protein that functions as an Nxf1 cofactor

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