Photosensitivity and type I IFN responses in cutaneous lupus are driven by epidermal-derived interferon kappa

Sarkar, Mrinal K.; Hile, Grace A.; Tsoi, Lam C.; Xing, Xianying; Liu, Jianhua; Liang, Yun; Berthier, Céline C.; Swindell, William R.; Patrick, Matthew; Shao, Shuai; Tsou, Pei‐Suen; Uppala, Rattapon; Beamer, Maria A.; Srivastava, Anshika; Bielas, Stephanie; Harms, Paul W.; Getsios, Spiro; Elder, James T.; Voorhees, John J.; Guðjónsson, Jóhann E.; Kahlenberg, J. Michelle

doi:10.1136/annrheumdis-2018-213197

Cited by 199 publications

(222 citation statements)

References 44 publications

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“…1A). Similar to a previous report using ex vivo samples (Sarkar et al, 2018), we detected a modest (~2-fold) and transient (6 hr) IFN-κ expression in the skin (not shown). Early induction in cutaneous expression of all the tested ISG was strikingly higher in female than in male mice, and the greater fold-induction of some ISG in female skin persisted at 24hr (Ifit3 and Ifif44) and 48hr (Ifit3 and Irf7) after UVB exposure ( Fig.…”

Section: Resultssupporting

confidence: 91%

“…In vitro and ex vivo studies reported that UVB and UVC light-mediated cell damage induced IFN-I in keratinocytes and other cell types (Gehrke et al, 2013;Sarkar et al, 2018), possibly aided by the downregulation of ULK-1, a STING inhibitor (Kemp et al, 2015). We and others observed that repeated exposure to low doses of UVB light (100mJ/cm 2 per day for 5 days) caused a modest upregulation in ISG expression in the skin of normal mice (Sontheimer et al, 2017;Wolf et al, 2019).…”

Section: Resultsmentioning

confidence: 71%

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The early local and systemic Type I interferon responses to ultraviolet B light exposure are cGAS dependent

Skopelja-Gardner

Tai

et al. 2019

Preprint

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AbstractMost systemic lupus erythematosus (SLE) patients are photosensitive and ultraviolet B light (UVB) exposure worsens cutaneous disease and precipitates systemic flares of disease. The pathogenic link between skin disease and systemic exacerbations in SLE remains elusive. In an acute model of UVB-triggered inflammation, we observed that a single UV exposure triggered a striking IFN-I signature not only in the skin, but also in the blood and kidneys. The early IFN-I signature was significantly higher in female compared to male mice. The early IFN-I response in the skin was almost entirely, and in the blood partly, dependent on the presence of cGAS, as was skin inflammatory cell infiltration. Inhibition of cGAMP hydrolysis augmented the UVB-triggered IFN-I response. UVB skin exposure leads to cGAS-activation and both local and systemic IFN-I signature and could contribute to acute flares of disease in susceptible subjects such as patients with SLE.

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Section: Resultssupporting

confidence: 91%

Section: Resultsmentioning

confidence: 71%

The early local and systemic Type I interferon responses to ultraviolet B light exposure are cGAS dependent

Skopelja-Gardner

Tai

et al. 2019

Preprint

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“…To examine the effects of VGLL3 that were driving this lupus-like cutaneous phenotype, we evaluated WT mice and robustly expressing transgenic mice by qRT-PCR for transcript levels of a panel of proinflammatory and lupus-related factors. Many of these transcripts showed significant elevation in transgenic mice (Figure 2A and Supplemental Figure 2A), including Tnfsf13b (encoding BAFF); IFN-κ (Ifnk), the predominant type I IFN in cutaneous lupus (5); and Cxcl13, a biomarker of early-onset SLE, heightened disease activity, and renal involvement (6). IF studies of key VGLL3-regulated factors ( Figure 2B) corroborated our qRT-PCR findings.…”

Section: Resultssupporting

confidence: 74%

The female-biased factor VGLL3 drives cutaneous and systemic autoimmunity

Billi¹,

Gharaee−Kermani

Fullmer³

et al. 2019

JCI Insight

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“…While we found that neutrophil-mediated kidney inflammation in response to UV light does not cause clinical disease in healthy mice, such a mechanism may contribute to LN flares in photosensitive lupus patients in multiple ways: Fc receptor engagement by immune complexes could enhance neutrophil recruitment resulting in ROS and protease release 105,106 ; the heightened capacity of lupus neutrophils and LDGs to produce NETs, which in SLE patients are not cleared efficiently 107,108 , could lead to release of tissue-damaging proteases 109,110 , propagation of the IFN-I response 85,86 , or direct damage to the kidney endothelium by creating vascular damage and leakage 14,111 . Moreover, the underlying differences in lupus skin, such as enhanced IFN-I signaling 7,112,113 and defects in protective Langerhans cell population 114 could inform the extent and nature of neutrophil-mediated systemic responses. The exact mechanism might in addition be influenced by the neutrophil/LDG phenotype, as heterogeneity within these populations has become more apparent in SLE 65 .…”

Section: Discussionmentioning

confidence: 99%

Neutrophils Mediate Kidney Inflammation Following Acute Skin Exposure to UVB Light

Skopelja-Gardner

Tai

Sun

et al. 2020

Preprint

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Photosensitivity to ultraviolet (UV) light affects up to ~80% of lupus patients and can exacerbate local skin disease as well as systemic disease, including lupus nephritis. While neutrophils have been implicated in local tissue injury in lupus in response to immune complex deposition, whether and how they play a role in photosensitivity induced systemic disease is unknown. Here, we show that following skin exposure to UV light, neutrophils migrate not only to the skin, but also to the kidney, in an IL-17A-dependent manner. Kidney infiltrating neutrophils produced reactive oxygen species and their presence was associated with upregulation of endothelial adhesion molecules and inflammatory cytokines as well as the induction of kidney injury markers, including transient proteinuria. Neutrophils were responsible for inflammation and renal injury as demonstrated by experiments that inhibited neutrophil mobilization. Exploiting a mouse model containing photoactivatable immune cells, we observed that a subset of neutrophils found in the kidney had transited through UV light-exposed skin suggesting reverse transmigration. These findings demonstrate that neutrophils mediate transient kidney injury following skin exposure to UV light and, coupled with observations identifying similar neutrophil phenotypes in human lupus, could provide a mechanistic link to explain sun-induced systemic lupus flares.

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Photosensitivity and type I IFN responses in cutaneous lupus are driven by epidermal-derived interferon kappa

Abstract: Collectively, our data identify IFN-κ as a critical IFN in CLE pathology via promotion of enhanced IFN responses and photosensitivity. IFN-κ is a potential novel target for UVB prophylaxis and CLE-directed therapy.

Cited by 199 publications

References 44 publications

The early local and systemic Type I interferon responses to ultraviolet B light exposure are cGAS dependent

The early local and systemic Type I interferon responses to ultraviolet B light exposure are cGAS dependent

The female-biased factor VGLL3 drives cutaneous and systemic autoimmunity

Neutrophils Mediate Kidney Inflammation Following Acute Skin Exposure to UVB Light

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