Your search keyword '"Sarkar, Mrinal K."' showing total 18 results

1. Cytokine responses in nonlesional psoriatic skin as clinical predictor to anti-TNF agents.

Author

Tsoi LC, Patrick MT, Shuai S, Sarkar MK, Chi S, Ruffino B, Billi AC, Xing X, Uppala R, Zang C, Fullmer J, He Z, Maverakis E, Mehta NN, Perez White BE, Getsios S, Helfrich Y, Voorhees JJ, Kahlenberg JM, Weidinger S, and Gudjonsson JE

Subjects

Cytokines genetics, Humans, Longitudinal Studies, Psoriasis immunology, RNA-Seq, Severity of Illness Index, Transcriptome, Cytokines biosynthesis, Psoriasis drug therapy, Skin immunology, Tumor Necrosis Factor Inhibitors therapeutic use

Abstract

Background: A major issue with the current management of psoriasis is our inability to predict treatment response., Objective: Our aim was to evaluate the ability to use baseline molecular expression profiling to assess treatment outcome for patients with psoriasis., Methods: We conducted a longitudinal study of 46 patients with chronic plaque psoriasis treated with anti-TNF agent etanercept, and molecular profiles were assessed in more than 200 RNA-seq samples., Results: We demonstrated correlation between clinical response and molecular changes during the course of the treatment, particularly for genes responding to IL-17A/TNF in keratinocytes. Intriguingly, baseline gene expressions in nonlesional, but not lesional, skin were the best marker of treatment response at week 12. We identified USP18, a known regulator of IFN responses, as positively correlated with Psoriasis Area and Severity Index (PASI) improvement (P = 9.8 × 10 -4 ) and demonstrate its role in regulating IFN/TNF responses in keratinocytes. Consistently, cytokine gene signatures enriched in baseline nonlesional skin expression profiles had strong correlations with PASI improvement. Using this information, we developed a statistical model for predicting PASI75 (ie, 75% of PASI improvement) at week 12, achieving area under the receiver-operating characteristic curve value of 0.75 and up to 80% accurate PASI75 prediction among the top predicted responders., Conclusions: Our results illustrate feasibility of assessing drug response in psoriasis using nonlesional skin and implicate involvement of IFN regulators in anti-TNF responses., (Copyright © 2021 American Academy of Allergy, Asthma & Immunology. All rights reserved.)

Published

2022

2. KLK6 expression in skin induces PAR1-mediated psoriasiform dermatitis and inflammatory joint disease.

Author

Billi AC, Ludwig JE, Fritz Y, Rozic R, Swindell WR, Tsoi LC, Gruzska D, Abdollahi-Roodsaz S, Xing X, Diaconu D, Uppala R, Camhi MI, Klenotic PA, Sarkar MK, Husni ME, Scher JU, McDonald C, Kahlenberg JM, Midura RJ, Gudjonsson JE, and Ward NL

Subjects

Animals, Arthritis, Psoriatic genetics, Arthritis, Psoriatic pathology, Dermatitis genetics, Dermatitis pathology, Female, Humans, Kallikreins genetics, Male, Mice, Mice, Transgenic, Receptor, PAR-1 genetics, Skin pathology, Arthritis, Psoriatic metabolism, Dermatitis metabolism, Kallikreins metabolism, Receptor, PAR-1 metabolism, Signal Transduction, Skin metabolism

Abstract

Kallikrein-related peptidase 6 (KLK6) is a secreted serine protease hypothesized to promote inflammation via cleavage of protease-activated receptor 1 (PAR1) and PAR2. KLK6 levels are elevated in multiple inflammatory and autoimmune conditions, but no definitive role in pathogenesis has been established. Here, we show that skin-targeted overexpression of KLK6 causes generalized, severe psoriasiform dermatitis with spontaneous development of debilitating psoriatic arthritis-like joint disease. The psoriatic skin and joint phenotypes are reversed by normalization of skin KLK6 levels and attenuated following genetic elimination of PAR1 but not PAR2. Conservation of this regulatory pathway was confirmed in human psoriasis using vorapaxar, an FDA-approved PAR1 antagonist, on explanted lesional skin from patients with psoriasis. Beyond defining a critical role for KLK6/PAR1 signaling in promoting psoriasis, our results demonstrate that KLK6/PAR1-mediated inflammation in the skin alone is sufficient to drive inflammatory joint disease. Further, we identify PAR1 as a promising cytokine-independent target in therapy of psoriasis and psoriatic arthritis.

Published

2020

3. Staphylococcus aureus Colonization Is Increased on Lupus Skin Lesions and Is Promoted by IFN-Mediated Barrier Disruption.

Author

Sirobhushanam S, Parsa N, Reed TJ, Berthier CC, Sarkar MK, Hile GA, Tsoi LC, Banfield J, Dobry C, Horswill AR, Gudjonsson JE, and Kahlenberg JM

Subjects

Adult, Cell Adhesion, Cell Movement, Cells, Cultured, Female, Filaggrin Proteins, Humans, Interferon Type I metabolism, Interferon-gamma metabolism, Intermediate Filament Proteins genetics, Intermediate Filament Proteins metabolism, Lupus Erythematosus, Systemic microbiology, Male, Membrane Proteins genetics, Membrane Proteins metabolism, Microarray Analysis, Middle Aged, Pregnancy, Sequence Analysis, RNA, Skin microbiology, Skin pathology, Staphylococcal Infections microbiology, Keratinocytes physiology, Lupus Erythematosus, Systemic immunology, Skin immunology, Staphylococcal Infections immunology, Staphylococcus aureus physiology

Abstract

Cutaneous inflammation is recurrent in systemic lupus erythematosus (SLE), yet mechanisms that drive cutaneous inflammation in SLE are not well defined. Type I IFNs are elevated in nonlesional SLE skin and promote inflammatory responses. Staphylococcus aureus, known to induce IFN production, could play a role in cutaneous inflammation in SLE. We show here that active cutaneous lupus erythematosus lesions are highly colonized (∼50%) by S. aureus. To define the impact of IFNs on S. aureus colonization, we examined the effects of type I and type II IFNs on S. aureus adherence and invasion. An increase in adherent S. aureus was observed after exposure to both IFN-α and -γ, whereas IFN-γ appeared to inhibit invasion of S. aureus. Cutaneous lupus erythematosus lesional skin microarray data and RNA sequencing data from SLE keratinocytes identified repression of barrier gene expression, such as filaggrin and loricrin, and SLE keratinocytes exhibited increased S. aureus-binding integrins. These SLE-associated changes could be replicated by IFN treatment of keratinocytes. Further, SLE keratinocytes exhibited increased binding to S. aureus. Together, these data suggest that chronic exposure to IFNs induces barrier disruption that allows for higher S. aureus colonization in SLE skin., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2020

4. Atopic Dermatitis Is an IL-13-Dominant Disease with Greater Molecular Heterogeneity Compared to Psoriasis.

Author

Tsoi LC, Rodriguez E, Degenhardt F, Baurecht H, Wehkamp U, Volks N, Szymczak S, Swindell WR, Sarkar MK, Raja K, Shao S, Patrick M, Gao Y, Uppala R, Perez White BE, Getsios S, Harms PW, Maverakis E, Elder JT, Franke A, Gudjonsson JE, and Weidinger S

Subjects

Cohort Studies, Dermatitis, Atopic genetics, Gene Expression Profiling, Humans, Interleukin-13 genetics, Interleukin-4 metabolism, Psoriasis genetics, RNA, Long Noncoding genetics, Sequence Analysis, RNA, Signal Transduction, Skin pathology, Transcriptome, Dermatitis, Atopic immunology, Interleukin-13 metabolism, Organ Specificity genetics, Psoriasis immunology, RNA genetics, Skin metabolism, Th2 Cells immunology

Abstract

Atopic dermatitis (AD) affects up to 20% of children and adults worldwide. To gain a deeper understanding of the pathophysiology of AD, we conducted a large-scale transcriptomic study of AD with deeply sequenced RNA-sequencing samples using long (126-bp) paired-end reads. In addition to the comparisons against previous transcriptomic studies, we conducted in-depth analysis to obtain a high-resolution view of the global architecture of the AD transcriptome and contrasted it with that of psoriasis from the same cohort. By using 147 RNA samples in total, we found striking correlation between dysregulated genes in lesional psoriasis and lesional AD skin with 81% of AD dysregulated genes being shared with psoriasis. However, we described disease-specific molecular and cellular features, with AD skin showing dominance of IL-13 pathways, but with near undetectable IL-4 expression. We also demonstrated greater disease heterogeneity and larger proportion of dysregulated long noncoding RNAs in AD, and illustrated the translational impact, including skin-type classification and drug-target prediction. This study is by far the largest study comparing the AD and psoriasis transcriptomes using RNA sequencing and demonstrating the shared inflammatory components, as well as specific discordant cytokine signatures of these two skin diseases., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2019

5. RNA-seq identifies a diminished differentiation gene signature in primary monolayer keratinocytes grown from lesional and uninvolved psoriatic skin.

Author

Swindell WR, Sarkar MK, Liang Y, Xing X, Baliwag J, Elder JT, Johnston A, Ward NL, and Gudjonsson JE

Subjects

Adult, Female, Gene Expression, Gene Expression Profiling, Humans, Keratinocytes pathology, Male, Middle Aged, Psoriasis metabolism, Psoriasis pathology, Sequence Analysis, RNA, Skin pathology, Transcriptome, Keratinocytes metabolism, Psoriasis genetics, Skin metabolism

Abstract

Keratinocyte (KC) hyper-proliferation and epidermal thickening are characteristic features of psoriasis lesions, but the specific contributions of KCs to plaque formation are not fully understood. This study used RNA-seq to investigate the transcriptome of primary monolayer KC cultures grown from lesional (PP) and non-lesional (PN) biopsies of psoriasis patients and control subjects (NN). Whole skin biopsies from the same subjects were evaluated concurrently. RNA-seq analysis of whole skin identified a larger number of psoriasis-increased differentially expressed genes (DEGs), but analysis of KC cultures identified more PP- and PN-decreased DEGs. These latter DEG sets overlapped more strongly with genes near loci identified by psoriasis genome-wide association studies and were enriched for genes associated with epidermal differentiation. Consistent with this, the frequency of AP-1 motifs was elevated in regions upstream of PN-KC-decreased DEGs. A subset of these genes belonged to the same co-expression module, mapped to the epidermal differentiation complex, and exhibited differentiation-dependent expression. These findings demonstrate a decreased differentiation gene signature in PP/PN-KCs that had not been identified by pre-genomic studies of patient-derived monolayers. This may reflect intrinsic defects limiting psoriatic KC differentiation capacity, which may contribute to compromised barrier function in normal-appearing uninvolved psoriatic skin.

Published

2017

6. Psoriasis: a mixed autoimmune and autoinflammatory disease.

Author

Liang Y, Sarkar MK, Tsoi LC, and Gudjonsson JE

Subjects

Adaptive Immunity genetics, Genetic Predisposition to Disease, Humans, Immunity, Innate genetics, Autoimmunity, Inflammation, Psoriasis immunology, Skin immunology

Abstract

In recent years marked progress has been made in our understanding of the critical biologic and immunologic pathways involved in psoriasis. Genetic studies have demonstrated that susceptibility to psoriasis involves components of both the adaptive and innate immune system and not surprisingly activation of both of these arms of the immune system is found in psoriatic skin. While adaptive immune responses predominate in chronic plaque psoriasis, innate and autoinflammatory responses dominate in pustular forms of psoriasis, with other clinical subtypes extending on a spectrum between plaque and pustular psoriasis. This makes psoriasis a unique disease where both autoimmune and autoinflammatory responses co-exist, with the balance between the two being critical in shaping its clinical presentation., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

7. Imiquimod has strain-dependent effects in mice and does not uniquely model human psoriasis.

Author

Swindell WR, Michaels KA, Sutter AJ, Diaconu D, Fritz Y, Xing X, Sarkar MK, Liang Y, Tsoi A, Gudjonsson JE, and Ward NL

Subjects

Animals, Female, Humans, Imiquimod, Interleukin-17 genetics, Male, Mice, Psoriasis metabolism, Sequence Analysis, RNA, Sex Factors, Skin metabolism, Species Specificity, Aminoquinolines pharmacology, Disease Models, Animal, Gene Expression Regulation, Mice, Inbred Strains, Psoriasis genetics, Skin drug effects

Abstract

Background: Imiquimod (IMQ) produces a cutaneous phenotype in mice frequently studied as an acute model of human psoriasis. Whether this phenotype depends on strain or sex has never been systematically investigated on a large scale. Such effects, however, could lead to conflicts among studies, while further impacting study outcomes and efforts to translate research findings., Methods: RNA-seq was used to evaluate the psoriasiform phenotype elicited by 6 days of Aldara (5% IMQ) treatment in both sexes of seven mouse strains (C57BL/6 J (B6), BALB/cJ, CD1, DBA/1 J, FVB/NJ, 129X1/SvJ, and MOLF/EiJ)., Results: In most strains, IMQ altered gene expression in a manner consistent with human psoriasis, partly due to innate immune activation and decreased homeostatic gene expression. The response of MOLF males was aberrant, however, with decreased expression of differentiation-associated genes (elevated in other strains). Key aspects of the IMQ response differed between the two most commonly studied strains (BALB/c and B6). Compared with BALB/c, the B6 phenotype showed increased expression of genes associated with DNA replication, IL-17A stimulation, and activated CD8+ T cells, but decreased expression of genes associated with interferon signaling and CD4+ T cells. Although IMQ-induced expression shifts mirrored psoriasis, responses in BALB/c, 129/SvJ, DBA, and MOLF mice were more consistent with other human skin conditions (e.g., wounds or infections). IMQ responses in B6 mice were most consistent with human psoriasis and best replicated expression patterns specific to psoriasis lesions., Conclusions: These findings demonstrate strain-dependent aspects of IMQ dermatitis in mice. We have shown that IMQ does not uniquely model psoriasis but in fact triggers a core set of pathways active in diverse skin diseases. Nonetheless, our findings suggest that B6 mice provide a better background than other strains for modeling psoriasis disease mechanisms.

Published

2017

8. A gene network regulated by the transcription factor VGLL3 as a promoter of sex-biased autoimmune diseases.

Author

Liang Y, Tsoi LC, Xing X, Beamer MA, Swindell WR, Sarkar MK, Berthier CC, Stuart PE, Harms PW, Nair RP, Elder JT, Voorhees JJ, Kahlenberg JM, and Gudjonsson JE

Subjects

Adult, Aged, Aged, 80 and over, Cells, Cultured, Female, Gene Expression Profiling, Genetic Association Studies, Genome-Wide Association Study, Humans, Male, Middle Aged, Quantitative Trait Loci, Transcription Factors genetics, Transcriptome, Young Adult, Gene Regulatory Networks, Keratinocytes physiology, Lupus Erythematosus, Cutaneous genetics, Scleroderma, Systemic genetics, Sex Factors, Sjogren's Syndrome genetics, Skin pathology, Transcription Factors metabolism

Abstract

Autoimmune diseases affect 7.5% of the US population, and they are among the leading causes of death and disability. A notable feature of many autoimmune diseases is their greater prevalence in females than in males, but the underlying mechanisms of this have remained unclear. Through the use of high-resolution global transcriptome analyses, we demonstrated a female-biased molecular signature associated with susceptibility to autoimmune disease and linked this to extensive sex-dependent co-expression networks. This signature was independent of biological age and sex-hormone regulation and was regulated by the transcription factor VGLL3, which also had a strong female-biased expression. On a genome-wide level, VGLL3-regulated genes had a strong association with multiple autoimmune diseases, including lupus, scleroderma and Sjögren's syndrome, and had a prominent transcriptomic overlap with inflammatory processes in cutaneous lupus. These results identified a VGLL3-regulated network as a previously unknown inflammatory pathway that promotes female-biased autoimmunity. They demonstrate the importance of studying immunological processes in females and males separately and suggest new avenues for therapeutic development., Competing Interests: Competing Financial Interests. The authors declare no competing financial interests.

Published

2017

9. IL-17 Responses Are the Dominant Inflammatory Signal Linking Inverse, Erythrodermic, and Chronic Plaque Psoriasis.

Author

Xing X, Liang Y, Sarkar MK, Wolterink L, Swindell WR, Voorhees JJ, Harms PW, Kahlenberg JM, Johnston A, and Gudjonsson JE

Subjects

Chronic Disease, Humans, Oxidative Phosphorylation, Paraffin Embedding, Receptors, Glucocorticoid metabolism, Signal Transduction, Skin pathology, TOR Serine-Threonine Kinases metabolism, Tissue Array Analysis, Ubiquitination, Dermatitis, Exfoliative immunology, Inflammation Mediators metabolism, Interleukin-17 metabolism, Mitochondria metabolism, Psoriasis immunology, Skin metabolism

Abstract

Competing Interests: Dr. Johann E. Gudjonsson has received research support from Amgen, AbbVie and Novartis.

Published

2016

10. Analysis of long non-coding RNAs highlights tissue-specific expression patterns and epigenetic profiles in normal and psoriatic skin.

Author

Tsoi LC, Iyer MK, Stuart PE, Swindell WR, Gudjonsson JE, Tejasvi T, Sarkar MK, Li B, Ding J, Voorhees JJ, Kang HM, Nair RP, Chinnaiyan AM, Abecasis GR, and Elder JT

Subjects

Cluster Analysis, Computational Biology, Enhancer Elements, Genetic, Gene Expression Profiling, Genomics methods, High-Throughput Nucleotide Sequencing, Humans, Molecular Sequence Annotation, Promoter Regions, Genetic, Psoriasis pathology, Epigenesis, Genetic, Gene Expression Regulation, Psoriasis genetics, RNA, Long Noncoding genetics, Skin metabolism, Transcriptome

Abstract

Background: Although analysis pipelines have been developed to use RNA-seq to identify long non-coding RNAs (lncRNAs), inference of their biological and pathological relevance remains a challenge. As a result, most transcriptome studies of autoimmune disease have only assessed protein-coding transcripts., Results: We used RNA-seq data from 99 lesional psoriatic, 27 uninvolved psoriatic, and 90 normal skin biopsies, and applied computational approaches to identify and characterize expressed lncRNAs. We detect 2,942 previously annotated and 1,080 novel lncRNAs which are expected to be skin specific. Notably, over 40% of the novel lncRNAs are differentially expressed and the proportions of differentially expressed transcripts among protein-coding mRNAs and previously-annotated lncRNAs are lower in psoriasis lesions versus uninvolved or normal skin. We find that many lncRNAs, in particular those that are differentially expressed, are co-expressed with genes involved in immune related functions, and that novel lncRNAs are enriched for localization in the epidermal differentiation complex. We also identify distinct tissue-specific expression patterns and epigenetic profiles for novel lncRNAs, some of which are shown to be regulated by cytokine treatment in cultured human keratinocytes., Conclusions: Together, our results implicate many lncRNAs in the immunopathogenesis of psoriasis, and our results provide a resource for lncRNA studies in other autoimmune diseases.

Published

2015

11. Single cell and spatial sequencing define processes by which keratinocytes and fibroblasts amplify inflammatory responses in psoriasis.

Author

Ma, Feiyang, Plazyo, Olesya, Billi, Allison C, Tsoi, Lam C, Xing, Xianying, Wasikowski, Rachael, Gharaee-Kermani, Mehrnaz, Hile, Grace, Jiang, Yanyun, Harms, Paul W, Xing, Enze, Kirma, Joseph, Xi, Jingyue, Hsu, Jer-En, Sarkar, Mrinal K, Chung, Yutein, Di Domizio, Jeremy, Gilliet, Michel, Ward, Nicole L, Maverakis, Emanual, Klechevsky, Eynav, Voorhees, John J, Elder, James T, Lee, Jun Hee, Kahlenberg, J Michelle, Pellegrini, Matteo, Modlin, Robert L, and Gudjonsson, Johann E

Subjects

Fibroblasts, Keratinocytes, Skin, Humans, Psoriasis, Epidermal Cells, Clinical Research, Rare Diseases, Autoimmune Disease, 2.1 Biological and endogenous factors, Aetiology, Inflammatory and immune system

Abstract

The immunopathogenesis of psoriasis, a common chronic inflammatory disease of the skin, is incompletely understood. Here we demonstrate, using a combination of single cell and spatial RNA sequencing, IL-36 dependent amplification of IL-17A and TNF inflammatory responses in the absence of neutrophil proteases, which primarily occur within the supraspinous layer of the psoriatic epidermis. We further show that a subset of SFRP2+ fibroblasts in psoriasis contribute to amplification of the immune network through transition to a pro-inflammatory state. The SFRP2+ fibroblast communication network involves production of CCL13, CCL19 and CXCL12, connected by ligand-receptor interactions to other spatially proximate cell types: CCR2+ myeloid cells, CCR7+ LAMP3+ dendritic cells, and CXCR4 expressed on both CD8+ Tc17 cells and keratinocytes, respectively. The SFRP2+ fibroblasts also express cathepsin S, further amplifying inflammatory responses by activating IL-36G in keratinocytes. These data provide an in-depth view of psoriasis pathogenesis, which expands our understanding of the critical cellular participants to include inflammatory fibroblasts and their cellular interactions.

Published

2023

12. Noninvasive Tape-Stripping with High-Resolution RNA Profiling Effectively Captures a Preinflammatory State in Nonlesional Psoriatic Skin

Author

Tsoi, Lam C, Xing, Xianying, Xing, Enze, Wasikowski, Rachael, Shao, Shuai, Zeng, Chang, Plazyo, Olesya, Kirma, Joseph, Jiang, Yanyung, Billi, Allison C, Sarkar, Mrinal K, Turnier, Jessica L, Uppala, Ranjitha, Smith, Kathleen M, Helfrich, Yolanda, Voorhees, John J, Maverakis, Emanual, Modlin, Robert L, Kahlenberg, J Michelle, Scott, Victoria E, and Gudjonsson, Johann E

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Psoriasis, Autoimmune Disease, Clinical Research, Genetics, Skin, Epidermis, Gene Expression Profiling, Humans, RNA, Oncology and Carcinogenesis, Dermatology & Venereal Diseases, Clinical sciences

Abstract

Tape stripping is a minimally invasive, nonscarring method that can be utilized to assess gene expression in the skin but is infrequently used given technical constraints. By comparing different tape stripping technologies and full-thickness skin biopsy results of lesional and nonlesional psoriatic skin from the same patients, we demonstrate that tape stripping with optimized high-resolution transcriptomic profiling can be used to effectively assess and characterize inflammatory responses in the skin. Upon comparison with single-cell RNA-sequencing data from psoriatic full-thickness skin biopsies, we illustrate that tape-stripping efficiently captures the transcriptome of the upper layers of the epidermis with sufficient resolution to assess the molecular components of the feed-forward immune amplification pathway in psoriasis. Notably, nonlesional psoriatic skin sampled by tape stripping demonstrates activated, proinflammatory changes when compared to healthy control skin, suggesting a prepsoriatic state, which is not captured on full-thickness skin biopsy transcriptome profiling. This work illustrates an approach to assess inflammatory response in the epidermis by combining noninvasive sampling with high throughput RNA-sequencing, providing a foundation for biomarker discoveries and mechanism of action studies for inflammatory skin conditions.

Published

2022

13. Phospholipase A2 enzymes represent a shared pathogenic pathway in psoriasis and pityriasis rubra pilaris

Author

Shao, Shuai, Chen, Jiaoling, Swindell, William R, Tsoi, Lam C, Xing, Xianying, Ma, Feiyang, Uppala, Ranjitha, Sarkar, Mrinal K, Plazyo, Olesya, Billi, Allison C, Wasikowski, Rachael, Smith, Kathleen M, Honore, Prisca, Scott, Victoria E, Maverakis, Emanual, Kahlenberg, J Michelle, Wang, Gang, Ward, Nicole L, Harms, Paul W, and Gudjonsson, Johann E

Subjects

Genetics, Psoriasis, Autoimmune Disease, 2.1 Biological and endogenous factors, Aetiology, Skin, Animals, Humans, Mice, Phospholipases A2, Pityriasis Rubra Pilaris, Autoimmune diseases, Dermatology, Immunology, Innate immunity

Abstract

Altered epidermal differentiation along with increased keratinocyte proliferation is a characteristic feature of psoriasis and pityriasis rubra pilaris (PRP). However, despite this large degree of overlapping clinical and histologic features, the molecular signatures these skin disorders share are unknown. Using global transcriptomic profiling, we demonstrate that plaque psoriasis and PRP skin lesions have high overlap, with all differentially expressed genes in PRP relative to normal skin having complete overlap with those in psoriasis. The major common pathway shared between psoriasis and PRP involves the phospholipases PLA2G2F, PLA2G4D, and PLA2G4E, which were found to be primarily expressed in the epidermis. Gene silencing each of the 3 PLA2s led to reduction in immune responses and epidermal thickness both in vitro and in vivo in a mouse model of psoriasis, establishing their proinflammatory roles. Lipidomic analyses demonstrated that PLA2s affect mobilization of a phospholipid-eicosanoid pool, which is altered in psoriatic lesions and functions to promote immune responses in keratinocytes. Taken together, our results highlight the important role of PLA2s as regulators of epidermal barrier homeostasis and inflammation, identify PLA2s as a shared pathogenic mechanism between PRP and psoriasis, and as potential therapeutic targets for both diseases.

Published

2021

14. IRAK2 Has a Critical Role in Promoting Feed-Forward Amplification of Epidermal Inflammatory Responses

Author

Shao, Shuai, Tsoi, Lam C, Swindell, William R, Chen, Jiaoling, Uppala, Ranjitha, Billi, Allison C, Xing, Xianying, Zeng, Chang, Sarkar, Mrinal K, Wasikowski, Rachael, Jiang, Yanyun, Kirma, Joseph, Sun, Jingru, Plazyo, Olesya, Wang, Gang, Harms, Paul W, Voorhees, John J, Ward, Nicole L, Ma, Feiyang, Pellegrini, Matteo, Merleev, Alexander, Perez White, Bethany E, Modlin, Robert L, Andersen, Bogi, Maverakis, Emanual, Weidinger, Stephan, Kahlenberg, J Michelle, and Gudjonsson, Johann E

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Autoimmune Disease, Psoriasis, Eczema / Atopic Dermatitis, Skin, Inflammatory and immune system, Cell Differentiation, Cells, Cultured, Dermatitis, Atopic, Epidermis, Humans, Inflammation, Interleukin-1 Receptor-Associated Kinases, NF-kappa B, Severity of Illness Index, Signal Transduction, Transcription Factors, Tumor Suppressor Proteins, Oncology and Carcinogenesis, Dermatology & Venereal Diseases, Clinical sciences

Abstract

Many inflammatory skin diseases are characterized by altered epidermal differentiation. Whether this altered differentiation promotes inflammatory responses has been unknown. Here, we show that IRAK2, a member of the signaling complex downstream of IL-1 and IL-36, correlates positively with disease severity in both atopic dermatitis and psoriasis. Inhibition of epidermal IRAK2 normalizes differentiation and inflammation in two mouse models of psoriasis- and atopic dermatitis-like inflammation. Specifically, we demonstrate that IRAK2 ties together proinflammatory and differentiation-dependent responses and show that this function of IRAK2 is specific to keratinocytes and acts through the differentiation-associated transcription factor ZNF750. Taken together, our findings suggest that IRAK2 has a critical role in promoting feed-forward amplification of inflammatory responses in skin through modulation of differentiation pathways and inflammatory responses.

Published

2021

15. Progression of acute-to-chronic atopic dermatitis is associated with quantitative rather than qualitative changes in cytokine responses

Author

Tsoi, Lam C, Rodriguez, Elke, Stölzl, Dora, Wehkamp, Ulrike, Sun, Jingru, Gerdes, Sascha, Sarkar, Mrinal K, Hübenthal, Matthias, Zeng, Chang, Uppala, Ranjitha, Xing, Xianying, Thielking, Frederieke, Billi, Allison C, Swindell, William R, Shefler, Alanna, Chen, Jiahan, Patrick, Matthew T, Harms, Paul W, Kahlenberg, J Michelle, Perez White, Bethany E, Maverakis, Emanual, Gudjonsson, Johann E, and Weidinger, Stephan

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Eczema / Atopic Dermatitis, Clinical Research, Genetics, Aetiology, 2.1 Biological and endogenous factors, Inflammatory and immune system, Skin, Acute Disease, Chronic Disease, Cytokines, Dermatitis, Atopic, Female, Humans, Male, Sequence Analysis, RNA, Th1 Cells, Th17 Cells, Th2 Cells, Transcriptome, Atopic dermatitis, RNA-sequencing, nonlesional, chronic AD, acute AD, Immunology, Allergy

Abstract

BackgroundAlthough multiple studies have assessed molecular changes in chronic atopic dermatitis (AD) lesions, little is known about the transition from acute to chronic disease stages, and the factors and mechanisms that shape chronic inflammatory activity.ObjectivesWe sought to assess the global transcriptome changes that characterize the progression from acute to chronic stages of AD.MethodsWe analyzed transcriptome changes in paired nonlesional skin, acute and chronic AD lesions from 11 patients and 38 healthy controls by RNA-sequencing, and conducted in vivo and histological assays to evaluate findings.ResultsOur data demonstrate that approximately 74% of the genes dysregulated in acute lesions remain or are further dysregulated in chronic lesions, whereas only 34% of the genes dysregulated in chronic lesions are altered already in the acute stage. Nonlesional AD skin exhibited enrichment of TNF, TH1, TH2, and TH17 response genes. Acute lesions showed marked dendritic-cell signatures and a prominent enrichment of TH1, TH2, and TH17 responses, along with increased IL-36 and thymic stromal lymphopoietin expression, which were further heightened in chronic lesions. In addition, genes involved in skin barrier repair, keratinocyte proliferation, wound healing, and negative regulation of T-cell activation showed a significant dysregulation in the chronic versus acute comparison. Furthermore, our data show progressive changes in vasculature and maturation of dendritic-cell subsets with chronicity, with FOXK1 acting as immune regulator.ConclusionsOur results show that the changes accompanying the transition from nonlesional to acute to chronic inflammation in AD are quantitative rather than qualitative, with chronic AD having heightened TH2, TH1, TH17, and IL36 responses and skin barrier repair mechanisms. These findings provide novel insights and highlight underappreciated pathways in AD pathogenesis that may be amenable to therapeutic targeting.

Published

2020

16. When bugs and drugs conspire: driving acneiform skin toxicity

Author

Billi, Allison C., Sarkar, Mrinal K., and Gudjonsson, Johann E.

Subjects

Tetracyclines -- Complications and side effects, Acne -- Complications and side effects, Toxicity, Skin, Anakinra -- Complications and side effects, DNA binding proteins, Antineoplastic agents, Rash, Health care industry

Abstract

Therapy with antineoplastic agents that inhibit EGFR and MEK is frequently limited by cutaneous adverse reactions, most commonly acne-like eruptions. In this issue of the JCI, Satoh et al. define a mechanism for acneiform skin toxicity wherein EGFR/MEK inhibitors cooperate with the skin commensal Cutibacterium acnes to induce IL-36[gamma] in keratinocytes via the combined actions of Kruppel-like factor 4 and NF-[kappa]B transcription factors at the IL-36[gamma] promoter, resulting in neutrophil recruitment. In addition to elucidating why EGFR/MEK inhibitor-induced rashes are often pustular and folliculocentric, this mechanism provides justification for the long-standing practice of management with antibiotic therapy., Molecular pathogenesis of acneiform reactions While antineoplastic targeted therapies have revolutionized treatment of oncologic patients, the high incidence of cutaneous adverse reactions requires oncologists and dermatologists to understand the mechanisms, [...]

Published

2020

17. Cytokine responses in nonlesional psoriatic skin as clinical predictor to anti-TNF agents

Author

Tsoi, Lam C, Patrick, Matthew T, Shuai, Shao, Sarkar, Mrinal K, Chi, Sunyi, Ruffino, Bethany, Billi, Allison C, Xing, Xianying, Uppala, Ranjitha, Zang, Cheng, Fullmer, Joseph, He, Zhi, Maverakis, Emanual, Mehta, Nehal N, Perez White, Bethany E, Getsios, Spiro, Helfrich, Yolanda, Voorhees, John J, Kahlenberg, J Michelle, Weidinger, Stephan, and Gudjonsson, Johann E

Subjects

drug response prediction, Allergy, Immunology, PASI, Severity of Illness Index, Autoimmune Disease, Clinical Research, Genetics, Humans, Psoriasis, Cytokines, Tumor Necrosis Factor Inhibitors, Longitudinal Studies, RNA-Seq, Transcriptome, etanercept, cytokine response, Skin

Abstract

BackgroundA major issue with the current management of psoriasis is our inability to predict treatment response.ObjectiveOur aim was to evaluate the ability to use baseline molecular expression profiling to assess treatment outcome for patients with psoriasis.MethodsWe conducted a longitudinal study of 46 patients with chronic plaque psoriasis treated with anti-TNF agent etanercept, and molecular profiles were assessed in more than 200 RNA-seq samples.ResultsWe demonstrated correlation between clinical response and molecular changes during the course of the treatment, particularly for genes responding to IL-17A/TNF in keratinocytes. Intriguingly, baseline gene expressions in nonlesional, but not lesional, skin were the best marker of treatment response at week 12. We identified USP18, a known regulator of IFN responses, as positively correlated with Psoriasis Area and Severity Index (PASI) improvement (P= 9.8×10-4) and demonstrate its role in regulating IFN/TNF responses in keratinocytes. Consistently, cytokine gene signatures enriched in baseline nonlesional skin expression profiles had strong correlations with PASI improvement. Using this information, we developed a statistical model for predicting PASI75 (ie, 75% of PASI improvement) at week 12, achieving area under the receiver-operating characteristic curve value of 0.75 and up to 80% accurate PASI75 prediction among the top predicted responders.ConclusionsOur results illustrate feasibility of assessing drug response in psoriasis using nonlesional skin and implicate involvement of IFN regulators in anti-TNF responses.

Published

2022

18. Targeting IL-1 controls refractory pityriasis rubra pilaris.

Author

Schmauch, Eloi, Severin, Yannik, Xianying Xing, Mangold, Aaron, Conrad, Curdin, Johannsen, Pål, Kahlenberg, J. Michelle, Mellett, Mark, Navarini, Alexander, Nobbe, Stefan, Sarkar, Mrinal K., Satyam, Abhigyan, Tsoi, Lam C., French, Lars E., Nilsson, Jakob, Linna-Kuosmanen, Suvi, Kaikkonen, Minna U., Snijder, Berend, Kellis, Manolis, and Gudjonsson, Johann E.

Subjects

*PITYRIASIS rubra, *INTERLEUKIN-1, *SKIN diseases, *SKIN, *ATOPIC dermatitis, *INDIVIDUALIZED medicine, *KERATINIZATION

Abstract

Pityriasis rubra pilaris (PRP) is a rare inflammatory skin disease with a poorly understood pathogenesis. Through a molecularly driven precision medicine approach and an extensive mechanistic pathway analysis in PRP skin samples, compared to psoriasis, atopic dermatitis, healed PRP, and healthy controls, we identified IL-1ß as a key mediator, orchestrating an NF-κB-mediated IL-1ß-CCL20 axis, including activation of CARD14 and NOD2. Treatment of three patients with the IL-1 antagonists anakinra and canakinumab resulted in rapid clinical improvement and reversal of the PRP-associated molecular signature with a 50% improvement in skin lesions after 2 to 3 weeks. This transcriptional signature was consistent with in vitro stimulation of keratinocytes with IL-1ß. With the central role of IL-1ß underscoring its potential as a therapeutic target, our findings propose a redefinition of PRP as an autoinflammatory keratinization disorder. Further clinical trials are needed to validate the efficacy of IL-1ß antagonists in PRP. [ABSTRACT FROM AUTHOR]

Published

2024