LEDGF/p75 interacts with mRNA splicing factors and targets HIV-1 integration to highly spliced genes

Singh, Parmit K.; Plumb, Matthew R.; Ferris, Andrea L.; Iben, James R.; Wu, Xiaolin; Fadel, Hind J.; Luke, Brian T.; Esnault, Caroline; Poeschla, Eric M.; Hughes, Stephen H.; Kvaratskhelia, Mamuka; Levin, Henry L.

doi:10.1101/gad.267609.115

Cited by 96 publications

(157 citation statements)

References 57 publications

(91 reference statements)

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“…3F). Consistent with a recent report (42), LKO changed the shape of the entire curve, with integration now highly favored within the initial 30% and disfavored to below the MRC for latter halves of genes (Fig. 3F).…”

Section: −26supporting

confidence: 91%

“…6, WT cell). LKO was reported recently to decrease integration into genes enriched for intron content to near random (42). Interestingly, we found that CPSF6 more prominently affected integration into intron-dense genes than did LEDGF/ p75 (Fig.…”

Section: Cpsf6 Directs Hiv-1 Integration To Active Genes and Ledgf/p75supporting

confidence: 49%

“…LEDGF/p75 is implicated in mRNA splicing (42,43), and CFI m components CPSF6 and CPSF7 interact with several spliceosome components (44)(45)(46). To investigate the relationship between splicing and integration targeting, frequencies of genetropic integration were correlated to intron density.…”

Section: −26mentioning

confidence: 99%

“…3A), we normalized our datasets to integrations within genes. Integration density kb −1 biases data with fewer gene-tropic integrations toward random because it fails to account for the decreased preference for genes upon LKO (42). Thus, although LEDGF/p75 influences integration targeting to genes, CPSF6 is the primary factor targeting HIV-1 to intron-rich genes.…”

Section: Cpsf6 Directs Hiv-1 Integration To Active Genes and Ledgf/p75mentioning

confidence: 99%

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A critical role for alternative polyadenylation factor CPSF6 in targeting HIV-1 integration to transcriptionally active chromatin

Sowd

Serrao

Wang

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

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Integration is vital to retroviral replication and influences the establishment of the latent HIV reservoir. HIV-1 integration favors active genes, which is in part determined by the interaction between integrase and lens epithelium-derived growth factor (LEDGF)/p75. Because gene targeting remains significantly enriched, relative to random in LEDGF/p75 deficient cells, other host factors likely contribute to gene-tropic integration. Nucleoporins 153 and 358, which bind HIV-1 capsid, play comparatively minor roles in integration targeting, but the influence of another capsid binding protein, cleavage and polyadenylation specificity factor 6 (CPSF6), has not been reported. In this study we knocked down or knocked out CPSF6 in parallel or in tandem with LEDGF/p75. CPSF6 knockout changed viral infectivity kinetics, decreased proviral formation, and preferentially decreased integration into transcriptionally active genes, spliced genes, and regions of chromatin enriched in genes and activating histone modifications. LEDGF/p75 depletion by contrast preferentially altered positional integration targeting within gene bodies. Dual factor knockout reduced integration into genes to below the levels observed with either single knockout and revealed that CPSF6 played a more dominant role than LEDGF/p75 in directing integration to euchromatin. CPSF6 complementation rescued HIV-1 integration site distribution in CPSF6 knockout cells, but complementation with a capsid binding mutant of CPSF6 did not. We conclude that integration targeting proceeds via two distinct mechanisms: capsid-CPSF6 binding directs HIV-1 to actively transcribed euchromatin, where the integrase-LEDGF/p75 interaction drives integration into gene bodies.

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Section: −26supporting

confidence: 91%

Section: Cpsf6 Directs Hiv-1 Integration To Active Genes and Ledgf/p75supporting

confidence: 49%

Section: −26mentioning

confidence: 99%

Section: Cpsf6 Directs Hiv-1 Integration To Active Genes and Ledgf/p75mentioning

confidence: 99%

See 2 more Smart Citations

A critical role for alternative polyadenylation factor CPSF6 in targeting HIV-1 integration to transcriptionally active chromatin

Sowd

Serrao

Wang

et al. 2016

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

212

333

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show abstract

“…It is not surprising, therefore, that retroviruses evolved genus-specific and contrasting traits with respect to the types of chromosomal loci they preferentially target. HIV-1, a highly pathogenic lentivirus, channels integration toward genedense chromosomal domains, integrating predominantly within active transcription units (4,5). Recent studies uncovered a hierarchical mechanism that depends on HIV-1 capsid, the major viral structural protein (a product of the viral gag gene), and integrase, which interact with cellular proteins CPSF6 and LEDGF/p75, respectively (6)(7)(8)(9)(10)(11).…”

mentioning

confidence: 99%

Structural basis for spumavirus GAG tethering to chromatin

Lesbats

Serrao

Maskell

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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The interactions between a retrovirus and host cell chromatin that underlie integration and provirus expression are poorly understood. The prototype foamy virus (PFV) structural protein GAG associates with chromosomes via a chromatin-binding sequence (CBS) located within its C-terminal region. Here, we show that the PFV CBS is essential and sufficient for a direct interaction with nucleosomes and present a crystal structure of the CBS bound to a mononucleosome. The CBS interacts with the histone octamer, engaging the H2A-H2B acidic patch in a manner similar to other acidic patch-binding proteins such as herpesvirus latency-associated nuclear antigen (LANA). Substitutions of the invariant arginine anchor residue in GAG result in global redistribution of PFV and macaque simian foamy virus (SFV mac ) integration sites toward centromeres, dampening the resulting proviral expression without affecting the overall efficiency of integration. Our findings underscore the importance of retroviral structural proteins for integration site selection and the avoidance of genomic junkyards.retrovirus | integration | nucleosome | chromatin-binding

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Transfer Learning-Based Advanced Deep Learning Architecture for the Identification of HIV-1 Integration Sites Using Imbalanced Dataset

Boruah

Das

2023

Intelligent Data Engineering and Analytics

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LEDGF/p75 interacts with mRNA splicing factors and targets HIV-1 integration to highly spliced genes

Cited by 96 publications

References 57 publications

A critical role for alternative polyadenylation factor CPSF6 in targeting HIV-1 integration to transcriptionally active chromatin

A critical role for alternative polyadenylation factor CPSF6 in targeting HIV-1 integration to transcriptionally active chromatin

Structural basis for spumavirus GAG tethering to chromatin

Transfer Learning-Based Advanced Deep Learning Architecture for the Identification of HIV-1 Integration Sites Using Imbalanced Dataset

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