Structure of the Dimeric Exonuclease TREX1 in Complex with DNA Displays a Proline-rich Binding Site for WW Domains

Brucet, M.; Querol-Audí, Jordi; Serra, Maria Paola; Ramirez-Espain, Ximena; Bertlik, Kamila; Ruiz, Lı́dia; Lloberas, Jorge; Macias, María J.; Fita, Ignacio; Celada, Antonio

doi:10.1074/jbc.m700236200

Cited by 46 publications

(76 citation statements)

References 39 publications

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“…We showed previously that TREX1 removes nucleotides from ssDNA and dsDNA oligonucleotide constructs (1,3,5) and from a nicked dsDNA plasmid generated by incubation with the NM23-H1 endonuclease (6). The TREX1 structure indicates that four nucleotides of ssDNA, not dsDNA, bind into the active sites of each protomer of the dimer (9,22) consistent with the greater TREX1 activity detected on partial duplex DNAs containing 3Ј terminal unpaired nucleotides (1,3). These combined data illustrate TREX1 exonuclease action using a variety of DNA structures that contain accessible 3Ј termini.…”

Section: Resultsmentioning

confidence: 99%

The TREX1 Double-stranded DNA Degradation Activity Is Defective in Dominant Mutations Associated with Autoimmune Disease

Lehtinen

Harvey

Mulcahy

et al. 2008

Journal of Biological Chemistry

113

117

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Mutations in TREX1 have been linked to a spectrum of human autoimmune diseases including Aicardi-Goutières syndrome (AGS), familial chilblain lupus (FCL), systemic lupus erythematosus, and retinal vasculopathy and cerebral leukodystrophy. A common feature in these conditions is the frequent detection of antibodies to double-stranded DNA (dsDNA). TREX1 participates in a cell death process implicating this major 3 3 5 exonuclease in genomic DNA degradation to minimize potential immune activation by persistent self DNA. The TREX1 D200N and D18N dominant heterozygous mutations were identified in AGS and FCL, respectively. TREX1 enzymes containing the D200N and D18N mutations were compared using nicked dsDNA and single-stranded DNA (ssDNA) degradation assays. The TREX1WT/D200N and TREX1 WT/D18N heterodimers are completely deficient at degrading dsDNA and degrade ssDNA at an expected ϳ2-fold lower rate than TREX1 WT enzyme. Further, the D200N-and D18N-containing TREX1 homo-and heterodimers inhibit the dsDNA degradation activity of TREX1 WT enzyme, providing a likely explanation for the dominant phenotype of these TREX1 mutant alleles in AGS and FCL. By comparison, the TREX1 R114H homozygous mutation causes AGS and is found as a heterozygous mutation in systemic lupus erythematosus. The TREX1 R114H/R114H homodimer has dysfunctional dsDNA and ssDNA degradation activities and does not detectibly inhibit the TREX1 WT enzyme, whereas the TREX1heterodimer has a functional dsDNA degradation activity, supporting the recessive genetics of TREX1 R114H in AGS. The dysfunctional dsDNA degradation activities of these disease-related TREX1 mutants could account for persistent dsDNA from dying cells leading to an aberrant immune response in these clinically related disorders.The TREX1 gene encodes the major 3Ј 3 5Ј exonuclease detected in mammalian cells. TREX1 is a single open reading frame located on chromosome 3p21.31 and encodes a 314-amino acid polypeptide (1-3). TREX1 is closely related to TREX2 (located on chromosome Xq28) except TREX1 contains additional coding sequence for a C-terminal region not found in TREX2 (4). The N-terminal 242 amino acids of TREX1 contain the catalytically robust 3Ј 3 5Ј exonuclease that is active on ssDNA 2 and dsDNA (5) with the highest activity detected using a partial duplex DNA containing unpaired 3Ј nucleotides (1-3). The C-terminal 72 amino acids contain a transmembrane region that localizes TREX1 to the endoplasmic reticulum in the perinuclear space of cells (6). Activation of a cell death pathway and treatment of cells with DNA-damaging agents cause TREX1 to relocate to the nucleus where it acts on DNA 3Ј termini (6 -8).The structure of TREX1 catalytic domain with bound DNA reveals the protein-polynucleotide interactions that explain the preference for multiple unpaired 3Ј termini in TREX1 exonuclease action and highlights the extensive interface contacts in the stable dimeric enzyme (9). A short ssDNA of approximately four nucleotides is accommodated in the TREX1 active site, and the Arg-1...

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Section: Resultsmentioning

confidence: 99%

The TREX1 Double-stranded DNA Degradation Activity Is Defective in Dominant Mutations Associated with Autoimmune Disease

Lehtinen

Harvey

Mulcahy

et al. 2008

Journal of Biological Chemistry

113

117

View full text Add to dashboard Cite

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“…PPII refers to the polyproline II motif implicated in mediating protein-protein interactions with proline-binding domain containing proteins. In fact, PPII has been shown to be required for the interaction of Trex1 with the transcription factor CA150 [16]. The functional significance of this interaction remains to be clarified.…”

Section: The Futurementioning

confidence: 99%

“…Trex1 functions as a homodimer and its crystal structure has recently been solved [16,17]. For a detailed discussion of Trex1 structure-function analysis readers are referred to the studies by Brucet and colleagues and de Silva and colleagues [16,17]. Exo 1-3 represent the exonuclease domains which co-ordinate Mg +2 which is essential for catalysis.…”

Section: The Futurementioning

confidence: 99%

“…exonuclease activity but impact on Trex1 intra-cellular localisation [52]. Work on TREX1 is currently uncovering novel interacting proteins and should provide more information on the multifunctional nature of this enzyme [16]. Finally, it will be important to uncover the extent of functional overlap, if any, between TREX1 and Trex2.…”

Section: Some Outstanding Questionsmentioning

confidence: 99%

“…The precise biological function of TREX2 is currently unclear although a possible role in mediating genomic stability has been suggested [15]. The crystal structure of Trex1 has recently been described and readers are referred to these studies for in-depth description of TREX1 structure-function analysis [16,17].…”

Section: A Brief Summary Of Mammalian Dna Exonucleasesmentioning

confidence: 99%

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TREX1 DNA exonuclease deficiency, accumulation of single stranded DNA and complex human genetic disorders

O’Driscoll

2008

DNA Repair

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Functionalization of the 3′‐Ends of DNA and RNA Strands with N‐ethyl‐N‐coupled Nucleosides: A Promising Approach To Avoid 3′‐Exonuclease‐Catalyzed Hydrolysis of Therapeutic Oligonucleotides

et al. 2013

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The development of nucleic acid derivatives to generate novel medical treatments has become increasingly popular, but the high vulnerability of oligonucleotides to nucleases limits their practical use. We explored the possibility of increasing the stability against 3'-exonucleases by replacing the two 3'-terminal nucleotides by N-ethyl-N-coupled nucleosides. Molecular dynamics simulations of 3'-N-ethyl-N-modified DNA:Klenow fragment complexes suggested that this kind of alteration has negative effects on the correct positioning of the adjacent scissile phosphodiester bond at the active site of the enzyme, and accordingly was expected to protect the oligonucleotide from degradation. We verified that these modifications conferred complete resistance to 3'-exonucleases. Furthermore, cellular RNAi experiments with 3'-N-ethyl-N-modified siRNAs showed that these modifications were compatible with the RNAi machinery. Overall, our experimental and theoretical studies strongly suggest that these modified oligonucleotides could be valuable for therapeutic applications.

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Structure of the Dimeric Exonuclease TREX1 in Complex with DNA Displays a Proline-rich Binding Site for WW Domains

Cited by 46 publications

References 39 publications

The TREX1 Double-stranded DNA Degradation Activity Is Defective in Dominant Mutations Associated with Autoimmune Disease

The TREX1 Double-stranded DNA Degradation Activity Is Defective in Dominant Mutations Associated with Autoimmune Disease

TREX1 DNA exonuclease deficiency, accumulation of single stranded DNA and complex human genetic disorders

Functionalization of the 3′‐Ends of DNA and RNA Strands with N‐ethyl‐N‐coupled Nucleosides: A Promising Approach To Avoid 3′‐Exonuclease‐Catalyzed Hydrolysis of Therapeutic Oligonucleotides

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