The Exonuclease Trex2 Shapes Psoriatic Phenotype

The stratum corneum of the epidermis constitutes the mammalian skin barrier to the environment. It is formed by cornification of keratinocytes, a process which involves the removal of nuclear DNA. Here, we investigated the mechanism of cornification-associated DNA degradation by generating mouse models deficient of candidate DNA-degrading enzymes and characterizing their epidermal phenotypes. In contrast to Dnase1l2 −/− mice and keratinocyte-specific DNase2 knockout mice (Dnase2 Δep), Dnase1l2 −/− Dnase2 Δep mice aberrantly retained nuclear DNA in the stratum corneum, a phenomenon commonly referred to as parakeratosis. The DNA within DNase1L2/DNase2-deficient corneocytes was partially degraded in a DNase1-independent manner. Isolation of corneocytes, i.e. the cornified cell components of the stratum corneum, and labelling of DNA demonstrated that corneocytes of Dnase1l2 −/− Dnase2 Δep mice contained DNA in a nucleus-shaped compartment that also contained nucleosomal histones but lacked the nuclear intermediate filament protein lamin A/C. Parakeratosis was not associated with altered corneocyte resistance to mechanical stress, changes in transepidermal water loss, or inflammatory infiltrates in Dnase1l2 −/− Dnase2 Δep mice. The results of this study suggest that cornification of epidermal keratinocytes depends on the cooperation of DNase1L2 and DNase2 and indicate that parakeratosis per se does not suffice to cause skin pathologies.

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Section: Discussionmentioning

confidence: 99%

Inactivation of DNase1L2 and DNase2 in keratinocytes suppresses DNA degradation during epidermal cornification and results in constitutive parakeratosis

Fischer

Buchberger

Napirei

et al. 2017

Sci Rep

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“…We could exclude that this degradation depends on DNase1, which is also expressed in differentiating keratinocytes 23 . Other candidate contributors to cornification-associated DNA fragmentation include, but are not limited to, caspase-activated DNase (CAD), also known as DNA fragmentation factor B 24 and the exonuclease TREX2 10,25,26 . Like in suppression of DNA breakdown during programmed cell death of hair and nail keratinocytes 14 and sebocytes 15 , the blockade of DNA degradation by deletion of DNase1L2 and DNase2 prevented the complete removal of histone H3, a component of nucleosomes, whereas the inter-nucleosomal histone H1 and a nuclear protein without DNA interaction, lamin A/C, were degraded.…”

Section: Discussionmentioning

confidence: 99%

079 Inactivation of DNase1L2 and DNase2 in keratinocytes suppresses DNA degradation during epidermal cornification and results in constitutive parakeratosis

Fischer

Buchberger

Tschachler

et al. 2017

Journal of Investigative Dermatology

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“…The exonuclease TREX2 is the epidermis‐associated homolog of TREX1, which suppresses inflammation by controlling endogenous retroelements . Both TREX enzymes are expressed in the epidermis, but only TREX2 is upregulated during normal keratinocyte differentiation . Knockout of TREX2 is associated with the aberrant presence of DNA fragments in the cytoplasm of cornifying keratinocytes but not with inflammation .…”

Section: Epidermal Keratinocytes Suppress Inflammation During Normal mentioning

confidence: 99%

“…Knockout of TREX2 is associated with the aberrant presence of DNA fragments in the cytoplasm of cornifying keratinocytes but not with inflammation . TREX2 and AIM2, a sensor of cytoplasmic DNA, are induced in psoriasis . DNase1L2 is another DNA‐degrading enzyme that is specifically expressed in cornifying keratinocytes where it cooperates both with TREX2 and DNase 2 .…”

Section: Epidermal Keratinocytes Suppress Inflammation During Normal mentioning

confidence: 99%

Control of cell death‐associated danger signals during cornification prevents autoinflammation of the skin

Eckhart

Tschachler

2018

Experimental Dermatology

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The function of the skin as a barrier to the environment is mainly achieved by the outermost layers of the epidermis. In the granular layer, epidermal keratinocytes undergo the last steps of their terminal differentiation program resulting in cornification. The coordinated conversion of living keratinocytes into corneocytes, the building blocks of the cornified layer, represents a unique form of programmed cell death. Recent studies have identified numerous genes that are specifically expressed in terminally differentiated keratinocytes and, surprisingly, this genetic program does not only include mediators of cornification but also suppressors of pyroptosis, another mode of programmed cell death. Pyroptosis is activated by inflammasomes, leads to the release of interleukin-1 (IL-1) family cytokines, and thereby activates inflammation. In addition, inhibitors of potentially pro-inflammatory proteases and enzymes removing danger-associated cytoplasmic DNA are expressed in differentiated keratinocytes. We propose the concept of cornification as an inherently hazardous process in which damaging side effects are actively suppressed by protective mechanisms. In support of this hypothesis, loss-of-function mutations in epidermal protease inhibitors and IL-1 family antagonists suffice to induce autoinflammation. Similarly, exogenous disturbances of either cornification or its accompanying control mechanisms may be starting points for skin inflammation. Further studies into the relationship between cornification, pyroptosis and other forms of cell death will help to define the initiation phase of inflammatory skin diseases and offer new targets for disease prevention and therapy.

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The Exonuclease Trex2 Shapes Psoriatic Phenotype

Cited by 18 publications

References 72 publications

Inactivation of DNase1L2 and DNase2 in keratinocytes suppresses DNA degradation during epidermal cornification and results in constitutive parakeratosis

Inactivation of DNase1L2 and DNase2 in keratinocytes suppresses DNA degradation during epidermal cornification and results in constitutive parakeratosis

079 Inactivation of DNase1L2 and DNase2 in keratinocytes suppresses DNA degradation during epidermal cornification and results in constitutive parakeratosis

Control of cell death‐associated danger signals during cornification prevents autoinflammation of the skin

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