An ENU Mutagenesis-Derived Mouse Model with a Dominant Jak1 Mutation Resembling Phenotypes of Systemic Autoimmune Disease

Sabrautzki, Sibylle; Janas, Eva; Lorenz‐Depiereux, Bettina; Calzada‐Wack, Julia; Aguilar-Pimentel, Juan Antonio; Rathkolb, Birgit; Adler, Thure; Cohrs, Christian M.; Hans, Wolfgang; Diener, Susanne; Fuchs, Helmut; Gailus‐Durner, Valérie; Busch, Dirk H.; Höfler, Heinz; Ollert, Markus; Strom, Tim M.; Wolf, Eckhard; Neff, Frauke; Angelis, Martin Hrabé de

doi:10.1016/j.ajpath.2013.04.027

Cited by 25 publications

(36 citation statements)

References 87 publications

(75 reference statements)

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“…Nonetheless, WT BM cells transferred into Spade-mutant jci.org Volume 126 Number 6 June 2016 mice should be a useful model to investigate the presymptomatic pathological changes in the skin under emollient treatment, which is difficult to investigate in humans. While the present article was in preparation, Sabrauski et al reported that a missense point mutation (S645P) in the pseudokinase domain of the Jak1 gene resulted in dermatitis accompanied by STAT3 activation (41). However, there are important differences between our results and theirs with respect to disease onset and phenotype.…”

Section: Discussioncontrasting

confidence: 63%

Hyperactivation of JAK1 tyrosine kinase induces stepwise, progressive pruritic dermatitis

Yasuda¹,

Fukada²,

Nishida³

et al. 2016

Journal of Clinical Investigation

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Section: Discussioncontrasting

confidence: 63%

Hyperactivation of JAK1 tyrosine kinase induces stepwise, progressive pruritic dermatitis

Yasuda¹,

Fukada²,

Nishida³

et al. 2016

Journal of Clinical Investigation

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“…This could explain the earlier failure of the JAK3/SYK blocking agent R333 in a clinical CLE study (45). A central role for JAK1 in CLE-associated immune signaling also is supported by recent findings of mice developing CLE-like skin lesions due to JAK1-hyperactivation (46). Currently, a phase II clinical trial investigates the efficacy of orally administered JAK1 inhibitor filgotinib in female patients with active CLE (NCT03134222).…”

Section: Discussionmentioning

confidence: 91%

Selective Janus Kinase 1 Inhibition Is a Promising Therapeutic Approach for Lupus Erythematosus Skin Lesions

et al. 2020

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Background: Cutaneous lupus erythematosus (CLE) is an interferon (IFN)-driven autoimmune skin disease characterized by an extensive cytotoxic lesional inflammation with activation of different innate immune pathways. Aim of our study was to investigate the specific role of Janus kinase 1 (JAK1) activation in this disease and the potential benefit of selective JAK1 inhibitors as targeted therapy in a preclinical CLE model. Methods: Lesional skin of patients with different CLE subtypes and healthy controls (N = 31) were investigated on JAK1 activation and expression of IFN-associated mediators via immunohistochemistry and gene expression analyses. The functional role of JAK1 and efficacy of inhibition was evaluated in vitro using cultured keratinocytes stimulated with endogenous nucleic acids. Results were confirmed in vivo using an established lupus-prone mouse model. Results: Proinflammatory immune pathways, including JAK/STAT signaling, are significantly upregulated within inflamed CLE skin. Here, lesional keratinocytes and dermal immune cells strongly express activated phospho-JAK1. Selective pharmacological JAK1 inhibition significantly reduces the expression of typical proinflammatory mediators such as CXCL chemokines, BLyS, TRAIL, and AIM2 in CLE in vitro models and also improves skin lesions in lupus-prone TREX1 −/−-mice markedly. Conclusion: IFN-associated JAK/STAT activation plays a crucial role in the pathophysiology of CLE. Selective inhibition of JAK1 leads to a decrease of cytokine expression, reduced immune activation, and decline of keratinocyte cell death. Topical treatment with a JAK1-specific inhibitor significantly improves CLE-like skin lesions in a lupus-prone TREX1 −/−-mouse model and appears to be a promising therapeutic approach for CLE patients.

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“…These targets may include TRP channels, as previous studies have demonstrated, these proteins can be phosphorylated to modulate neuronal activity . Strikingly, recent studies in both mice and humans have identified activating mutations in JAK1 that result in pruritic dermatoses . Bone marrow transplantation with wild‐type bone marrow into mutant JAK1 mice, as well as potent systemic immunosuppression in patients with activated mutant JAK1, did not resolve the aberrant inflammation and chronic itch.…”

Section: Effects Of the Immune System On The Sensory Nervous Systemmentioning

confidence: 99%

Interactions of the immune and sensory nervous systems in atopy

Oetjen

Kim

2018

The FEBS Journal

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A striking feature underlying all atopic disorders, such as asthma, atopic dermatitis, and food allergy, is the presence of pathologic sensory responses, reflexes, and behaviors. These symptoms, exemplified by chronic airway irritation and cough, chronic itch and scratching, as well as gastrointestinal discomfort and dysfunction, are often cited as the most debilitating aspects of atopic disorders. Emerging studies have highlighted how the immune system shapes the scope and intensity of sensory responses by directly modulating the sensory nervous system. Additionally, factors produced by neurons have demonstrated novel functions in propagating atopic inflammation at barrier surfaces. In this review, we highlight new studies that have changed our understanding of atopy through advances in characterizing the reciprocal interactions between the immune and sensory nervous systems.

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An ENU Mutagenesis-Derived Mouse Model with a Dominant Jak1 Mutation Resembling Phenotypes of Systemic Autoimmune Disease

Cited by 25 publications

References 87 publications

Hyperactivation of JAK1 tyrosine kinase induces stepwise, progressive pruritic dermatitis

Hyperactivation of JAK1 tyrosine kinase induces stepwise, progressive pruritic dermatitis

Selective Janus Kinase 1 Inhibition Is a Promising Therapeutic Approach for Lupus Erythematosus Skin Lesions

Interactions of the immune and sensory nervous systems in atopy

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