N-terminal half of transportin SR2 interacts with HIV integrase

Tsirkone, V.G.; Blokken, Jolien; Wit, Flore De; Breemans, Jolien; Houwer, Stéphanie De; Debyser, Zeger; Christ, Frauke; Strelkov, S.V.

doi:10.1074/jbc.m117.777029

Cited by 11 publications

(22 citation statements)

References 72 publications

(91 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…However the exact mechanism of action of TNPO3 still remains a matter of controversy [38]. Some studies suggest that TNPO3 participates in the nuclear import of PICs [9,25,39,40] whereas other authors propose that TNPO3 promotes HIV-1 infection though the interaction with HIV-1 CA [41–43] or indirectly through the interaction of CPSF6 with HIV-1 CA [12]. Besides an indirect role for TNPO3 in viral integration through its interaction with CA and/or the IN and their respective cellular partners such as CPSF6 or LEDGF/p75 [38] has been proposed.…”

Section: Discussionmentioning

confidence: 99%

“…Several cellular import factors, including importin-7, importin-α3 and Transportin 3 (TNPO3, also called TRN-SR2) have also been involved in HIV-1 nuclear import [8]. Apart from its implication in nuclear import of the viral PIC, it has been confirmed that N-terminal end of TNPO3 protein act as a direct binding partner of HIV-1 IN [9]. Interaction with the viral CA has also been documented [10,11] and nearly 30 CA-mutants able to modify HIV-1 dependence on TNPO3 have been described [12].…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

The mutation of Transportin 3 gene that causes limb girdle muscular dystrophy 1F induces protection against HIV-1 infection

et al. 2019

Self Cite

View full text Add to dashboard Cite

The causative mutation responsible for limb girdle muscular dystrophy 1F (LGMD1F) is one heterozygous single nucleotide deletion in the stop codon of the nuclear import factor Transportin 3 gene (TNPO3 ). This mutation causes a carboxy-terminal extension of 15 amino acids, producing a protein of unknown function (TNPO3_mut) that is co-expressed with wild-type TNPO3 (TNPO3_wt). TNPO3 has been involved in the nuclear transport of serine/arginine-rich proteins such as splicing factors and also in HIV-1 infection through interaction with the viral integrase and capsid. We analyzed the effect of TNPO3_mut on HIV-1 infection using PBMCs from patients with LGMD1F infected ex vivo. HIV-1 infection was drastically impaired in these cells and viral integration was reduced 16-fold. No significant effects on viral reverse transcription and episomal 2-LTR circles were observed suggesting that the integration of HIV-1 genome was restricted. This is the second genetic defect described after CCR5Δ32 that shows strong resistance against HIV-1 infection.

show abstract

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

The mutation of Transportin 3 gene that causes limb girdle muscular dystrophy 1F induces protection against HIV-1 infection

et al. 2019

Self Cite

View full text Add to dashboard Cite

show abstract

“…Cellular proteins interacting with the PIC include the barrier to autointegration factor 1 (BAF1), high mobility group proteins (HMG), lamina-associated polypeptide 2α (LAP2α), lens-epithelium-derived growth factor (LEDGF/p75), and the karyopherin transportin SR2 (TRN-SR2, TNPO3). TNPO3 binds directly to the CCD and CTD of IN [ 149 ] and may participate in shuttling the PIC to the nucleus. The size of the PIC is uncertain, but it must fit through the nuclear pore, and the process of import is essential yet remains unclear.…”

Section: Integration: the Central Event In Hiv Replicationmentioning

confidence: 99%

The role of integration and clonal expansion in HIV infection: live long and prosper

Anderson¹,

Maldarelli²

2018

Retrovirology

View full text Add to dashboard Cite

Integration of viral DNA into the host genome is a central event in the replication cycle and the pathogenesis of retroviruses, including HIV. Although most cells infected with HIV are rapidly eliminated in vivo, HIV also infects long-lived cells that persist during combination antiretroviral therapy (cART). Cells with replication competent HIV proviruses form a reservoir that persists despite cART and such reservoirs are at the center of efforts to eradicate or control infection without cART. The mechanisms of persistence of these chronically infected long-lived cells is uncertain, but recent research has demonstrated that the presence of the HIV provirus has enduring effects on infected cells. Cells with integrated proviruses may persist for many years, undergo clonal expansion, and produce replication competent HIV. Even proviruses with defective genomes can produce HIV RNA and may contribute to ongoing HIV pathogenesis. New analyses of HIV infected cells suggest that over time on cART, there is a shift in the composition of the population of HIV infected cells, with the infected cells that persist over prolonged periods having proviruses integrated in genes associated with regulation of cell growth. In several cases, strong evidence indicates the presence of the provirus in specific genes may determine persistence, proliferation, or both. These data have raised the intriguing possibility that after cART is introduced, a selection process enriches for cells with proviruses integrated in genes associated with cell growth regulation. The dynamic nature of populations of cells infected with HIV during cART is not well understood, but is likely to have a profound influence on the composition of the HIV reservoir with critical consequences for HIV eradication and control strategies. As such, integration studies will shed light on understanding viral persistence and inform eradication and control strategies. Here we review the process of HIV integration, the role that integration plays in persistence, clonal expansion of the HIV reservoir, and highlight current challenges and outstanding questions for future research.

show abstract

“…Taken together, these results suggest that the major points of contact are the Gag MA region and the TNPO3 NPC binding domain, although it is important to note that other regions of Gag and TNPO3 appear to be required for maximal binding to occur. A recent study demonstrated that the N-terminus of TNPO3 (containing the RanGTP binding domain and part of the NPC interaction domain) interacts with the catalytic core domain and C-terminal domain of HIV-1 integrase, suggesting that other retroviral cargoes of TNPO3 bind to sites outside of the CBD (49).…”

Section: Discussionmentioning

confidence: 99%

TNPO3-mediated nuclear entry of the Rous sarcoma virus Gag protein is independent of the cargo-binding domain

Rice

Stake

Parent

2020

Preprint

View full text Add to dashboard Cite

21Retroviral Gag polyproteins orchestrate the assembly and release of nascent 22show that the MA region is required for nuclear import of Gag through the TNPO3 44 pathway. Gag nuclear entry does not require the cargo binding domain of TNPO3. 45Understanding the molecular basis for TNPO3-mediated nuclear trafficking of the RSV 46Gag protein may lead to a deeper appreciation for whether different import factors play 47 distinct roles in retrovirus replication. 48

show abstract

N-terminal half of transportin SR2 interacts with HIV integrase

Cited by 11 publications

References 72 publications

The mutation of Transportin 3 gene that causes limb girdle muscular dystrophy 1F induces protection against HIV-1 infection

The mutation of Transportin 3 gene that causes limb girdle muscular dystrophy 1F induces protection against HIV-1 infection

The role of integration and clonal expansion in HIV infection: live long and prosper

TNPO3-mediated nuclear entry of the Rous sarcoma virus Gag protein is independent of the cargo-binding domain

Contact Info

Product

Resources

About