Genome Replication Is Associated With Release of Immunogenic DNA Waste

Nadja Schubert; Tina Schumann; Elena Daum; Karolin Flade; Yan Ge; Lara Hagedorn; Winfried Edelmann; Luise Müller; Marc Schmitz; Gunnar Kuut; Veit Hornung; Rayk Behrendt; Axel Roers

doi:10.3389/fimmu.2022.880413

Genome Replication Is Associated With Release of Immunogenic DNA Waste

Nadja Schubert, Tina Schumann, Elena Daum, Karolin Flade, Yan Ge, Lara Hagedorn, Winfried Edelmann, Luise Müller, Marc Schmitz, Gunnar Kuut, Veit Hornung, Rayk Behrendt, Axel Roers

Cell Biology

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

Innate DNA sensors detect foreign and endogenous DNA to induce responses to infection and cellular stress or damage. Inappropriate activation by self-DNA triggers severe autoinflammatory conditions, including Aicardi-Goutières syndrome (AGS) that can be caused by defects of the cytosolic DNase 3’repair exonuclease 1 (TREX1). TREX1 loss-of-function alleles are also associated with systemic lupus erythematosus (SLE). Chronic activation of innate antiviral immunity in TREX1-deficient cells depends on the DNA sensor cGAS, implying that accumulating TREX1 DNA substrates cause the inflammatory pathology. Retrotransposon-derived cDNAs were shown to activate cGAS in TREX1-deficient neuronal cells. We addressed other endogenous sources of cGAS ligands in cells lacking TREX1. We find that induced loss of TREX1 in primary cells induces a rapid IFN response that requires ongoing proliferation. The inflammatory phenotype of Trex1^-/- mice was partially rescued by additional knock out of exonuclease 1, a multifunctional enzyme providing 5’ flap endonuclease activity for Okazaki fragment processing and postreplicative ribonucleotide excision repair. Our data imply genome replication as a source of DNA waste with pathogenic potential that is efficiently degraded by TREX1.

Original language	English (US)
Article number	880413
Journal	Frontiers in immunology
Volume	13
DOIs	https://doi.org/10.3389/fimmu.2022.880413
State	Published - May 11 2022

Keywords

Exo1
Trex1
cytosolic DNA
interferonopathy
replication
type I interferon

ASJC Scopus subject areas

Immunology and Allergy
Immunology

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10.3389/fimmu.2022.880413

Cite this

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title = "Genome Replication Is Associated With Release of Immunogenic DNA Waste",

abstract = "Innate DNA sensors detect foreign and endogenous DNA to induce responses to infection and cellular stress or damage. Inappropriate activation by self-DNA triggers severe autoinflammatory conditions, including Aicardi-Gouti{\`e}res syndrome (AGS) that can be caused by defects of the cytosolic DNase 3{\textquoteright}repair exonuclease 1 (TREX1). TREX1 loss-of-function alleles are also associated with systemic lupus erythematosus (SLE). Chronic activation of innate antiviral immunity in TREX1-deficient cells depends on the DNA sensor cGAS, implying that accumulating TREX1 DNA substrates cause the inflammatory pathology. Retrotransposon-derived cDNAs were shown to activate cGAS in TREX1-deficient neuronal cells. We addressed other endogenous sources of cGAS ligands in cells lacking TREX1. We find that induced loss of TREX1 in primary cells induces a rapid IFN response that requires ongoing proliferation. The inflammatory phenotype of Trex1-/- mice was partially rescued by additional knock out of exonuclease 1, a multifunctional enzyme providing 5{\textquoteright} flap endonuclease activity for Okazaki fragment processing and postreplicative ribonucleotide excision repair. Our data imply genome replication as a source of DNA waste with pathogenic potential that is efficiently degraded by TREX1.",

keywords = "Exo1, Trex1, cytosolic DNA, interferonopathy, replication, type I interferon",

author = "Nadja Schubert and Tina Schumann and Elena Daum and Karolin Flade and Yan Ge and Lara Hagedorn and Winfried Edelmann and Luise M{\"u}ller and Marc Schmitz and Gunnar Kuut and Veit Hornung and Rayk Behrendt and Axel Roers",

note = "Publisher Copyright: Copyright {\textcopyright} 2022 Schubert, Schumann, Daum, Flade, Ge, Hagedorn, Edelmann, M{\"u}ller, Schmitz, Kuut, Hornung, Behrendt and Roers.",

year = "2022",

month = may,

day = "11",

doi = "10.3389/fimmu.2022.880413",

language = "English (US)",

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T1 - Genome Replication Is Associated With Release of Immunogenic DNA Waste

AU - Schubert, Nadja

AU - Schumann, Tina

AU - Daum, Elena

AU - Flade, Karolin

AU - Ge, Yan

AU - Hagedorn, Lara

AU - Edelmann, Winfried

AU - Müller, Luise

AU - Schmitz, Marc

AU - Kuut, Gunnar

AU - Hornung, Veit

AU - Behrendt, Rayk

AU - Roers, Axel

PY - 2022/5/11

Y1 - 2022/5/11

N2 - Innate DNA sensors detect foreign and endogenous DNA to induce responses to infection and cellular stress or damage. Inappropriate activation by self-DNA triggers severe autoinflammatory conditions, including Aicardi-Goutières syndrome (AGS) that can be caused by defects of the cytosolic DNase 3’repair exonuclease 1 (TREX1). TREX1 loss-of-function alleles are also associated with systemic lupus erythematosus (SLE). Chronic activation of innate antiviral immunity in TREX1-deficient cells depends on the DNA sensor cGAS, implying that accumulating TREX1 DNA substrates cause the inflammatory pathology. Retrotransposon-derived cDNAs were shown to activate cGAS in TREX1-deficient neuronal cells. We addressed other endogenous sources of cGAS ligands in cells lacking TREX1. We find that induced loss of TREX1 in primary cells induces a rapid IFN response that requires ongoing proliferation. The inflammatory phenotype of Trex1-/- mice was partially rescued by additional knock out of exonuclease 1, a multifunctional enzyme providing 5’ flap endonuclease activity for Okazaki fragment processing and postreplicative ribonucleotide excision repair. Our data imply genome replication as a source of DNA waste with pathogenic potential that is efficiently degraded by TREX1.

AB - Innate DNA sensors detect foreign and endogenous DNA to induce responses to infection and cellular stress or damage. Inappropriate activation by self-DNA triggers severe autoinflammatory conditions, including Aicardi-Goutières syndrome (AGS) that can be caused by defects of the cytosolic DNase 3’repair exonuclease 1 (TREX1). TREX1 loss-of-function alleles are also associated with systemic lupus erythematosus (SLE). Chronic activation of innate antiviral immunity in TREX1-deficient cells depends on the DNA sensor cGAS, implying that accumulating TREX1 DNA substrates cause the inflammatory pathology. Retrotransposon-derived cDNAs were shown to activate cGAS in TREX1-deficient neuronal cells. We addressed other endogenous sources of cGAS ligands in cells lacking TREX1. We find that induced loss of TREX1 in primary cells induces a rapid IFN response that requires ongoing proliferation. The inflammatory phenotype of Trex1-/- mice was partially rescued by additional knock out of exonuclease 1, a multifunctional enzyme providing 5’ flap endonuclease activity for Okazaki fragment processing and postreplicative ribonucleotide excision repair. Our data imply genome replication as a source of DNA waste with pathogenic potential that is efficiently degraded by TREX1.

KW - Exo1

KW - Trex1

KW - cytosolic DNA

KW - interferonopathy

KW - replication

KW - type I interferon

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JO - Frontiers in immunology

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Genome Replication Is Associated With Release of Immunogenic DNA Waste

Abstract

Keywords

ASJC Scopus subject areas

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