Your search keyword '"Zepp JA"' showing total 35 results

1. Emergence of inflammatory fibroblasts with aging in Hermansky-Pudlak syndrome associated pulmonary fibrosis.

Author

Banaschewski BJH, Michki SN, Sitaraman S, Pan R, Wang JY, Stewart D, Goldy MK, Lin SM, Cantu E, Katzen JB, Basil MC, Emtiazjoo AM, Todd JL, Gokey JJ, Kropski JA, Frank DB, Zepp JA, and Young LR

Subjects

Humans, Male, Female, Animals, Mice, Mice, Inbred C57BL, Aging, Single-Cell Gene Expression Analysis, Disease Models, Animal, Macrophages immunology, Intestines immunology, Fibroblasts metabolism, Pulmonary Fibrosis genetics, Pulmonary Fibrosis immunology, Pulmonary Fibrosis metabolism, Pulmonary Fibrosis psychology, Hermanski-Pudlak Syndrome complications, Hermanski-Pudlak Syndrome genetics, Hermanski-Pudlak Syndrome immunology, Hermanski-Pudlak Syndrome metabolism, Inflammation genetics, Inflammation metabolism

Abstract

The longitudinal cellular interactions that drive pulmonary fibrosis are not well understood. To investigate the disease underpinnings associated with fibrosis onset and progression, we generated a scRNA-seq atlas of lungs from young and aged mouse models of multiple subtypes of Hermansky-Pudlak syndrome (HPS), a collection of rare autosomal recessive diseases associated with albinism, platelet dysfunction, and pulmonary fibrosis. We have identified an age-dependent increase in SAA3 + inflammatory lung fibroblasts in HPS mice, including in double-mutant HPS1-2 mice which develop spontaneous fibrosis. HPS1 fibroblasts show increased expression of IL-1R1, whereas alveolar type II epithelial cells from HPS2 mice induce the inflammatory gene signature in co-cultured fibroblasts. scRNA-seq of lung tissue from three HPS1 patients similarly shows the presence of inflammatory fibroblasts and increased IL1R1 expression on fibroblasts. These data posit complex interactions between dysfunctional epithelial cells, inflammatory fibroblasts, and recruited immune cells, suggesting potential opportunities for mitigation of the fibrotic cascade., Competing Interests: Competing interests: B.J.B. reports equity in MannKind Corporation. JLT acknowledges grants to the institution from the National Institute of Health, AstraZeneca, Boehringer Ingelheim, and Care Dx; and advisory board participation for Avalyn and Sanofi. E.C. reports consulting fees from CSL Behring and United Therapeutics, and meeting travel support from Pulmocide Ltd. E.C. also reports board participation for the International Society of Heart and Lung Transplantation, regional representative role for the UNOS Lung Committee, and as a consultant for device group for the FDA. J.A.K. reports grants from Boehringer Ingelheim and scientific advisory board membership at APIE and ARDA. L.R.Y. reports scientific advisory board participation for Boehringer Ingelheim and Sanofi and royalties from Wolters Kluwer for UpToDate authorship. All conflicts of interest reported are outside the scope of the submitted work., (© 2025. The Author(s).)

Published

2025

2. Dysregulated alveolar epithelial cell progenitor function and identity in Hermansky-Pudlak syndrome.

Author

Wang JY, Michki SN, Sitaraman S, Banaschewski BJ, Jamal R, Gokey JJ, Lin SM, Katzen JB, Basil MC, Cantu E, Kropski JA, Zepp JA, Frank DB, and Young LR

Subjects

Animals, Mice, Humans, Stem Cells metabolism, Pulmonary Fibrosis pathology, Pulmonary Fibrosis genetics, Pulmonary Fibrosis metabolism, Tumor Suppressor Protein p53 metabolism, Tumor Suppressor Protein p53 genetics, Lung pathology, Lung metabolism, Hermanski-Pudlak Syndrome genetics, Hermanski-Pudlak Syndrome metabolism, Hermanski-Pudlak Syndrome pathology, Alveolar Epithelial Cells metabolism, Alveolar Epithelial Cells pathology, Disease Models, Animal, Cell Differentiation

Abstract

Hermansky-Pudlak syndrome (HPS) is a genetic disorder of endosomal protein trafficking associated with pulmonary fibrosis in specific subtypes, including HPS-1 and HPS-2. Single-mutant HPS1 and HPS2 mice display increased fibrotic sensitivity while double-mutant HPS1/2 mice exhibit spontaneous fibrosis with aging, which has been attributed to HPS mutations in alveolar epithelial type II (AT2) cells. We utilized HPS mouse models and human lung tissue to investigate mechanisms of AT2 cell dysfunction driving fibrotic remodeling in HPS. Starting at 8 weeks of age, HPS mice exhibited progressive loss of AT2 cell numbers. HPS AT2 cell function was impaired ex vivo and in vivo. Incorporating AT2 cell lineage tracing in HPS mice, we observed aberrant differentiation with increased AT2-derived alveolar epithelial type I cells. Transcriptomic analysis of HPS AT2 cells revealed elevated expression of genes associated with aberrant differentiation and p53 activation. Lineage-tracing and organoid-modeling studies demonstrated that HPS AT2 cells were primed to persist in a Keratin-8-positive reprogrammed transitional state, mediated by p53 activity. Intrinsic AT2 progenitor cell dysfunction and p53 pathway dysregulation are mechanisms of disease in HPS-related pulmonary fibrosis, with the potential for early targeted intervention before the onset of fibrotic lung disease.

Published

2024

3. Dysregulated alveolar epithelial cell progenitor function and identity in Hermansky-Pudlak syndrome.

Author

Wang JY, Michki SN, Sitaraman S, Banaschewski BJ, Jamal R, Gokey JJ, Lin SM, Katzen JB, Basil MC, Cantu E, Kropski JA, Zepp JA, Frank DB, and Young LR

Abstract

Hermansky-Pudlak syndrome (HPS) is a genetic disorder of endosomal protein trafficking associated with pulmonary fibrosis in specific subtypes, including HPS-1 and HPS-2. Single mutant HPS1 and HPS2 mice display increased fibrotic sensitivity while double mutant HPS1/2 mice exhibit spontaneous fibrosis with aging, which has been attributed to HPS mutations in alveolar epithelial type II (AT2) cells. We utilized HPS mouse models and human lung tissue to investigate mechanisms of AT2 cell dysfunction driving fibrotic remodeling in HPS. Starting at 8 weeks of age, HPS mice exhibited progressive loss of AT2 cell numbers. HPS AT2 cell function was impaired ex vivo and in vivo . Incorporating AT2 cell lineage tracing in HPS mice, we observed aberrant differentiation with increased AT2-derived alveolar epithelial type I cells. Transcriptomic analysis of HPS AT2 cells revealed elevated expression of genes associated with aberrant differentiation and p53 activation. Lineage tracing and organoid modeling studies demonstrated that HPS AT2 cells were primed to persist in a Krt8 + reprogrammed transitional state, mediated by p53 activity. Intrinsic AT2 progenitor cell dysfunction and p53 pathway dysregulation are novel mechanisms of disease in HPS-related pulmonary fibrosis, with the potential for early targeted intervention before the onset of fibrotic lung disease.

Published

2024

4. Spatiotemporal dynamics of primary and motile cilia throughout lung development.

Author

Spurgin S, Nguimtsop AM, Chaudhry FN, Michki SN, Salvador J, Iruela-Arispe ML, Zepp JA, Mukhopadhyay S, and Cleaver O

Abstract

Cilia are specialized structures found on a variety of mammalian cells, with variable roles in the transduction of mechanical and biological signals (by primary cilia, PC), as well as the generation of fluid flow (by motile cilia). Their critical role in the establishment of a left-right axis in early development is well described, as is the innate immune function of multiciliated upper airway epithelium. By contrast, the dynamics of ciliary status during organogenesis and postnatal development is largely unknown. In this study, we define the progression of ciliary status within the endothelium, epithelium, and mesenchyme of the lung. Remarkably, we find that endothelial cells (ECs) lack PC at all stages of development, except in low numbers in the most proximal portions of the pulmonary arteries. In the lung epithelium, a proximodistal ciliary gradient is established over time, as the uniformly mono-ciliated epithelium transitions into proximal, multiciliated cells, and the distal alveolar epithelium loses its cilia. Mesenchymal cells, interestingly, are uniformly ciliated in early development, but with restriction to PDGFRα+ fibroblasts in the adult alveoli. This dynamic process in multiple cellular populations both challenges prior assertions that PC are found on all cells, and highlights a need to understand their spatiotemporal functions.

Published

2024

5. Dynamic Hippo pathway activity underlies mesenchymal differentiation during lung alveolar morphogenesis.

Author

Chaudhry FN, Michki NS, Shirmer DL, McGrath-Morrow S, Young LR, Frank DB, and Zepp JA

Subjects

Animals, Mice, Mesoderm metabolism, Adaptor Proteins, Signal Transducing metabolism, Adaptor Proteins, Signal Transducing genetics, Lung metabolism, Organogenesis genetics, Gene Expression Regulation, Developmental, Cell Differentiation, Hippo Signaling Pathway, Myofibroblasts metabolism, Myofibroblasts cytology, YAP-Signaling Proteins metabolism, YAP-Signaling Proteins genetics, Pulmonary Alveoli metabolism, Pulmonary Alveoli cytology, Signal Transduction, Protein Serine-Threonine Kinases metabolism, Protein Serine-Threonine Kinases genetics, Morphogenesis genetics

Abstract

Alveologenesis, the final stage in lung development, substantially remodels the distal lung, expanding the alveolar surface area for efficient gas exchange. Secondary crest myofibroblasts (SCMF) exist transiently in the neonatal distal lung and are crucial for alveologenesis. However, the pathways that regulate SCMF function, proliferation and temporal identity remain poorly understood. To address this, we purified SCMFs from reporter mice, performed bulk RNA-seq and found dynamic changes in Hippo-signaling components during alveologenesis. We deleted the Hippo effectors Yap/Taz from Acta2-expressing cells at the onset of alveologenesis, causing a significant arrest in alveolar development. Using single cell RNA-seq, we identified a distinct cluster of cells in mutant lungs with altered expression of marker genes associated with proximal mesenchymal cell types, airway smooth muscle and alveolar duct myofibroblasts. In vitro studies confirmed that Yap/Taz regulates myofibroblast-associated gene signature and contractility. Together, our findings show that Yap/Taz is essential for maintaining functional myofibroblast identity during postnatal alveologenesis., Competing Interests: Competing interests The authors declare no competing or financial interests., (© 2024. Published by The Company of Biologists Ltd.)

Published

2024

6. Circadian regulation of lung repair and regeneration.

Author

Naik A, Forrest KM, Paul O, Issah Y, Valekunja UK, Tang SY, Reddy AB, Hennessy EJ, Brooks TG, Chaudhry F, Babu A, Morley M, Zepp JA, Grant GR, FitzGerald GA, Sehgal A, Worthen GS, Frank DB, Morrisey EE, and Sengupta S

Published

2024

7. Circadian regulation of lung repair and regeneration.

Author

Naik A, Forrest KM, Paul O, Issah Y, Valekunja UK, Tang SY, Reddy AB, Hennessy EJ, Brooks TG, Chaudhry F, Babu A, Morley M, Zepp JA, Grant GR, FitzGerald GA, Sehgal A, Worthen GS, Frank DB, Morrisey EE, and Sengupta S

Subjects

Lung metabolism, Alveolar Epithelial Cells, Circadian Rhythm, Regeneration, Circadian Clocks genetics, Influenza A virus physiology

Abstract

Optimal lung repair and regeneration are essential for recovery from viral infections, including influenza A virus (IAV). We have previously demonstrated that acute inflammation and mortality induced by IAV is under circadian control. However, it is not known whether the influence of the circadian clock persists beyond the acute outcomes. Here, we utilize the UK Biobank to demonstrate an association between poor circadian rhythms and morbidity from lower respiratory tract infections, including the need for hospitalization and mortality after discharge; this persists even after adjusting for common confounding factors. Furthermore, we use a combination of lung organoid assays, single-cell RNA sequencing, and IAV infection in different models of clock disruption to investigate the role of the circadian clock in lung repair and regeneration. We show that lung organoids have a functional circadian clock and the disruption of this clock impairs regenerative capacity. Finally, we find that the circadian clock acts through distinct pathways in mediating lung regeneration - in tracheal cells via the Wnt/β-catenin pathway and through IL-1β in alveolar epithelial cells. We speculate that adding a circadian dimension to the critical process of lung repair and regeneration will lead to novel therapies and improve outcomes.

Published

2023

8. Engineering and Modeling the Lung Mesenchyme.

Author

Snitow ME, Chaudhry FN, and Zepp JA

Subjects

Mice, Animals, Fibroblasts, Intercellular Signaling Peptides and Proteins metabolism, Mesoderm metabolism, Mammals, Lung metabolism, Extracellular Matrix physiology

Abstract

The structure of the mammalian lung controls the flow of air through the airways and into the distal alveolar region where gas exchange occurs. Specialized cells in the lung mesenchyme produce the extracellular matrix (ECM) and growth factors required for lung structure. Historically, characterizing the mesenchymal cell subtypes was challenging due to their ambiguous morphology, overlapping expression of protein markers, and limited cell-surface molecules needed for isolation. The recent development of single-cell RNA sequencing (scRNA-seq) complemented with genetic mouse models demonstrated that the lung mesenchyme comprises transcriptionally and functionally heterogeneous cell-types. Bioengineering approaches that model tissue structure clarify the function and regulation of mesenchymal cell types. These experimental approaches demonstrate the unique abilities of fibroblasts in mechanosignaling, mechanical force generation, ECM production, and tissue regeneration. This chapter will review the cell biology of the lung mesenchyme and experimental approaches to study their function., (© 2023. The Author(s), under exclusive license to Springer Nature Switzerland AG.)

Published

2023

9. CXCL12 defines lung endothelial heterogeneity and promotes distal vascular growth.

Author

Chandrasekaran P, Negretti NM, Sivakumar A, Liberti DC, Wen H, Peers de Nieuwburgh M, Wang JY, Michki NS, Chaudhry FN, Kaur S, Lu M, Jin A, Zepp JA, Young LR, Sucre JMS, and Frank DB

Subjects

Mice, Pregnancy, Animals, Female, Morphogenesis, Mice, Transgenic, Embryonic Development, Lung, Endothelium, Vascular metabolism

Abstract

There is a growing amount of data uncovering the cellular diversity of the pulmonary circulation and mechanisms governing vascular repair after injury. However, the molecular and cellular mechanisms contributing to the morphogenesis and growth of the pulmonary vasculature during embryonic development are less clear. Importantly, deficits in vascular development lead to significant pediatric lung diseases, indicating a need to uncover fetal programs promoting vascular growth. To address this, we used a transgenic mouse reporter for expression of Cxcl12, an arterial endothelial hallmark gene, and performed single-cell RNA sequencing on isolated Cxcl12-DsRed+ endothelium to assess cellular heterogeneity within pulmonary endothelium. Combining cell annotation with gene ontology and histological analysis allowed us to segregate the developing artery endothelium into functionally and spatially distinct subpopulations. Expression of Cxcl12 is highest in the distal arterial endothelial subpopulation, a compartment enriched in genes for vascular development. Accordingly, disruption of CXCL12 signaling led to, not only abnormal branching, but also distal vascular hypoplasia. These data provide evidence for arterial endothelial functional heterogeneity and reveal conserved signaling mechanisms essential for pulmonary vascular development., Competing Interests: Competing interests L.R.Y. declares grants paid to her institution from the National Institutes of Health and the Orphan Disease Center at the University of Pennsylvania; royalties from UpToDate; consultancy fees and fees for participation on the Steering Committee of the InPedILD trial from Boehringer Ingelheim; and consultancy fees from Roche and Sanofi., (© 2022. Published by The Company of Biologists Ltd.)

Published

2022

10. A census of the lung: CellCards from LungMAP.

Author

Sun X, Perl AK, Li R, Bell SM, Sajti E, Kalinichenko VV, Kalin TV, Misra RS, Deshmukh H, Clair G, Kyle J, Crotty Alexander LE, Masso-Silva JA, Kitzmiller JA, Wikenheiser-Brokamp KA, Deutsch G, Guo M, Du Y, Morley MP, Valdez MJ, Yu HV, Jin K, Bardes EE, Zepp JA, Neithamer T, Basil MC, Zacharias WJ, Verheyden J, Young R, Bandyopadhyay G, Lin S, Ansong C, Adkins J, Salomonis N, Aronow BJ, Xu Y, Pryhuber G, Whitsett J, and Morrisey EE

Subjects

Cell Differentiation genetics, Databases as Topic, Humans, Lung metabolism, Regeneration genetics, Single-Cell Analysis methods, Lung cytology, Lung physiology

Abstract

The human lung plays vital roles in respiration, host defense, and basic physiology. Recent technological advancements such as single-cell RNA sequencing and genetic lineage tracing have revealed novel cell types and enriched functional properties of existing cell types in lung. The time has come to take a new census. Initiated by members of the NHLBI-funded LungMAP Consortium and aided by experts in the lung biology community, we synthesized current data into a comprehensive and practical cellular census of the lung. Identities of cell types in the normal lung are captured in individual cell cards with delineation of function, markers, developmental lineages, heterogeneity, regenerative potential, disease links, and key experimental tools. This publication will serve as the starting point of a live, up-to-date guide for lung research at https://www.lungmap.net/cell-cards/. We hope that Lung CellCards will promote the community-wide effort to establish, maintain, and restore respiratory health., Competing Interests: Declaration of interests X.S. and E.E.M. are members of the advisory board for Developmental Cell., (Copyright © 2021 Elsevier Inc. All rights reserved.)

Published

2022

11. Genomic, epigenomic, and biophysical cues controlling the emergence of the lung alveolus.

Author

Zepp JA, Morley MP, Loebel C, Kremp MM, Chaudhry FN, Basil MC, Leach JP, Liberti DC, Niethamer TK, Ying Y, Jayachandran S, Babu A, Zhou S, Frank DB, Burdick JA, and Morrisey EE

Subjects

Alveolar Epithelial Cells cytology, Alveolar Epithelial Cells metabolism, Animals, Cells, Cultured, Cues, Epigenomics, Humans, Mice, Mice, Transgenic, Myofibroblasts cytology, Myofibroblasts metabolism, Pulmonary Alveoli cytology, Pulmonary Alveoli metabolism, RNA-Seq methods, Signal Transduction, Single-Cell Analysis, Transcriptome, Cell Lineage genetics, Epigenesis, Genetic, Pulmonary Alveoli embryology

Abstract

The lung alveolus is the functional unit of the respiratory system required for gas exchange. During the transition to air breathing at birth, biophysical forces are thought to shape the emerging tissue niche. However, the intercellular signaling that drives these processes remains poorly understood. Applying a multimodal approach, we identified alveolar type 1 (AT1) epithelial cells as a distinct signaling hub. Lineage tracing demonstrates that AT1 progenitors align with receptive, force-exerting myofibroblasts in a spatial and temporal manner. Through single-cell chromatin accessibility and pathway expression (SCAPE) analysis, we demonstrate that AT1-restricted ligands are required for myofibroblasts and alveolar formation. These studies show that the alignment of cell fates, mediated by biophysical and AT1-derived paracrine signals, drives the extensive tissue remodeling required for postnatal respiration., (Copyright © 2021 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.)

Published

2021

12. p16 INK4a and the Alveolar Niche Take Center Stage in Bronchopulmonary Dysplasia.

Author

Chao CM, Bellusci S, and Zepp JA

Subjects

Cyclin-Dependent Kinase Inhibitor p16, Humans, Infant, Newborn, Regeneration, Bronchopulmonary Dysplasia, Carcinoma, Squamous Cell

Published

2020

13. STAT3-BDNF-TrkB signalling promotes alveolar epithelial regeneration after lung injury.

Author

Paris AJ, Hayer KE, Oved JH, Avgousti DC, Toulmin SA, Zepp JA, Zacharias WJ, Katzen JB, Basil MC, Kremp MM, Slamowitz AR, Jayachandran S, Sivakumar A, Dai N, Wang P, Frank DB, Eisenlohr LC, Cantu E 3rd, Beers MF, Weitzman MD, Morrisey EE, and Worthen GS

Subjects

Alveolar Epithelial Cells metabolism, Animals, Brain-Derived Neurotrophic Factor genetics, Female, Humans, Lung Injury etiology, Lung Injury pathology, Male, Membrane Glycoproteins genetics, Protein-Tyrosine Kinases genetics, Receptor, trkB genetics, STAT3 Transcription Factor genetics, Alveolar Epithelial Cells cytology, Brain-Derived Neurotrophic Factor metabolism, Lung Injury prevention & control, Membrane Glycoproteins metabolism, Protein-Tyrosine Kinases metabolism, Receptor, trkB metabolism, Regeneration, STAT3 Transcription Factor metabolism

Abstract

Alveolar epithelial regeneration is essential for recovery from devastating lung diseases. This process occurs when type II alveolar pneumocytes (AT2 cells) proliferate and transdifferentiate into type I alveolar pneumocytes (AT1 cells). We used genome-wide analysis of chromatin accessibility and gene expression following acute lung injury to elucidate repair mechanisms. AT2 chromatin accessibility changed substantially following injury to reveal STAT3 binding motifs adjacent to genes that regulate essential regenerative pathways. Single-cell transcriptome analysis identified brain-derived neurotrophic factor (Bdnf) as a STAT3 target gene with newly accessible chromatin in a unique population of regenerating AT2 cells. Furthermore, the BDNF receptor tropomyosin receptor kinase B (TrkB) was enriched on mesenchymal alveolar niche cells (MANCs). Loss or blockade of AT2-specific Stat3, Bdnf or mesenchyme-specific TrkB compromised repair and reduced Fgf7 expression by niche cells. A TrkB agonist improved outcomes in vivo following lung injury. These data highlight the biological and therapeutic importance of the STAT3-BDNF-TrkB axis in orchestrating alveolar epithelial regeneration.

Published

2020

14. Nanoparticle Delivery of Angiogenic Gene Therapy. Save the Vessels, Save the Lung!

Author

Zepp JA and Alvira CM

Subjects

Genetic Therapy, Humans, Infant, Newborn, Lung, Transcription Factors, Hyperoxia, Nanoparticles

Published

2020

15. Defining the role of pulmonary endothelial cell heterogeneity in the response to acute lung injury.

Author

Niethamer TK, Stabler CT, Leach JP, Zepp JA, Morley MP, Babu A, Zhou S, and Morrisey EE

Subjects

Animals, Endothelium pathology, Endothelium, Vascular cytology, Endothelium, Vascular pathology, Female, Flow Cytometry, Lung pathology, Mice, Mice, Inbred C57BL, Neovascularization, Physiologic, Orthomyxoviridae Infections pathology, Pulmonary Alveoli cytology, Pulmonary Alveoli pathology, Single-Cell Analysis, Acute Lung Injury pathology, Endothelium cytology, Lung cytology

Abstract

Pulmonary endothelial cells (ECs) are an essential component of the gas exchange machinery of the lung alveolus. Despite this, the extent and function of lung EC heterogeneity remains incompletely understood. Using single-cell analytics, we identify multiple EC populations in the mouse lung, including macrovascular endothelium (maEC), microvascular endothelium (miECs), and a new population we have termed Car4 -high ECs. Car4 -high ECs express a unique gene signature, and ligand-receptor analysis indicates they are primed to receive reparative signals from alveolar type I cells. After acute lung injury, they are preferentially localized in regenerating regions of the alveolus. Influenza infection reveals the emergence of a population of highly proliferative ECs that likely arise from multiple miEC populations and contribute to alveolar revascularization after injury. These studies map EC heterogeneity in the adult lung and characterize the response of novel EC subpopulations required for tissue regeneration after acute lung injury., Competing Interests: TN, CS, JL, JZ, MM, AB, SZ No competing interests declared, EM Reviewing editor, eLife, (© 2020, Niethamer et al.)

Published

2020

16. Dnmt1 is required for proximal-distal patterning of the lung endoderm and for restraining alveolar type 2 cell fate.

Author

Liberti DC, Zepp JA, Bartoni CA, Liberti KH, Zhou S, Lu M, Morley MP, and Morrisey EE

Subjects

Animals, Cell Differentiation genetics, Cell Lineage physiology, Cell Polarity, Cell Proliferation genetics, DNA (Cytosine-5-)-Methyltransferase 1 physiology, DNA Methylation genetics, Endoderm metabolism, Epigenesis, Genetic genetics, Epithelial Cells cytology, Epithelial-Mesenchymal Transition, Female, Gene Expression Regulation, Developmental, Lung cytology, Lung metabolism, Lung pathology, Male, Mice, Morphogenesis, Organogenesis physiology, Signal Transduction physiology, Transcription Factors metabolism, Alveolar Epithelial Cells metabolism, DNA (Cytosine-5-)-Methyltransferase 1 genetics, DNA (Cytosine-5-)-Methyltransferase 1 metabolism

Abstract

Lung endoderm development occurs through a series of finely coordinated transcriptional processes that are regulated by epigenetic mechanisms. However, the role of DNA methylation in regulating lung endoderm development remains poorly understood. We demonstrate that DNA methyltransferase 1 (Dnmt1) is required for early branching morphogenesis of the lungs and for restraining epithelial fate specification. Loss of Dnmt1 leads to an early branching defect, a loss of epithelial polarity and proximal endodermal cell differentiation, and an expansion of the distal endoderm compartment. Dnmt1 deficiency also disrupts epithelial-mesenchymal crosstalk and leads to precocious distal endodermal cell differentiation with premature expression of alveolar type 2 cell restricted genes. These data reveal an important requirement for Dnmt1 mediated DNA methylation in early lung development to promote proper branching morphogenesis, maintain proximal endodermal cell fate, and suppress premature activation of the distal epithelial fate., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

17. Cellular crosstalk in the development and regeneration of the respiratory system.

Author

Zepp JA and Morrisey EE

Subjects

Animals, Humans, Oxygen Consumption physiology, Cell Communication physiology, Cell Differentiation physiology, Homeostasis physiology, Regeneration, Respiratory Physiological Phenomena, Respiratory System embryology

Abstract

The respiratory system, including the peripheral lungs, large airways and trachea, is one of the most recently evolved adaptations to terrestrial life. To support the exchange of respiratory gases, the respiratory system is interconnected with the cardiovascular system, and this interconnective nature requires a complex interplay between a myriad of cell types. Until recently, this complexity has hampered our understanding of how the respiratory system develops and responds to postnatal injury to maintain homeostasis. The advent of new single-cell sequencing technologies, developments in cellular and tissue imaging and advances in cell lineage tracing have begun to fill this gap. The view that emerges from these studies is that cellular and functional heterogeneity of the respiratory system is even greater than expected and also highly adaptive. In this Review, we explore the cellular crosstalk that coordinates the development and regeneration of the respiratory system. We discuss both the classic cell and developmental biology studies and recent single-cell analysis to provide an integrated understanding of the cellular niches that control how the respiratory system develops, interacts with the external environment and responds to injury.

Published

2019

18. Early lineage specification defines alveolar epithelial ontogeny in the murine lung.

Author

Frank DB, Penkala IJ, Zepp JA, Sivakumar A, Linares-Saldana R, Zacharias WJ, Stolz KG, Pankin J, Lu M, Wang Q, Babu A, Li L, Zhou S, Morley MP, Jain R, and Morrisey EE

Subjects

Animals, Cell Differentiation, Female, In Situ Hybridization, Fluorescence, Mice, Pregnancy, Transcriptome, Cell Lineage, Lung cytology, Pulmonary Alveoli cytology

Abstract

During the stepwise specification and differentiation of tissue-specific multipotent progenitors, lineage-specific transcriptional networks are activated or repressed to orchestrate cell specification. The gas-exchange niche in the lung contains two major epithelial cell types, alveolar type 1 (AT1) and AT2 cells, and the timing of lineage specification of these cells is critical for the correct formation of this niche and postnatal survival. Integrating cell-specific lineage tracing studies, spatially specific mRNA transcript and protein expression, and single-cell RNA-sequencing analysis, we demonstrate that specification of alveolar epithelial cell fate begins concomitantly with the proximal-distal specification of epithelial progenitors and branching morphogenesis earlier than previously appreciated. By using a newly developed dual-lineage tracing system, we show that bipotent alveolar cells that give rise to AT1 and AT2 cells are a minor contributor to the alveolar epithelial population. Furthermore, single-cell assessment of the transcriptome identifies specified AT1 and AT2 progenitors rather than bipotent cells during sacculation. These data reveal a paradigm of organ formation whereby lineage specification occurs during the nascent stages of development coincident with broad tissue-patterning processes, including axial patterning of the endoderm and branching morphogenesis., Competing Interests: The authors declare no conflict of interest.

Published

2019

19. Regeneration of the lung alveolus by an evolutionarily conserved epithelial progenitor.

Author

Zacharias WJ, Frank DB, Zepp JA, Morley MP, Alkhaleel FA, Kong J, Zhou S, Cantu E, and Morrisey EE

Subjects

Acute Lung Injury pathology, Acute Lung Injury surgery, Animals, Antigens, Surface metabolism, Axin Protein metabolism, Biomarkers metabolism, Cell Cycle, Cell Lineage, Chromatin genetics, Chromatin metabolism, Epigenomics, Epithelial Cells metabolism, Female, Fibroblast Growth Factors metabolism, Humans, Male, Mice, Neoplasm Proteins metabolism, Organoids cytology, Organoids metabolism, Stem Cells metabolism, Transcriptome, Wnt Signaling Pathway, Epithelial Cells cytology, Evolution, Molecular, Pulmonary Alveoli cytology, Regeneration, Stem Cells cytology

Abstract

Functional tissue regeneration is required for the restoration of normal organ homeostasis after severe injury. Some organs, such as the intestine, harbour active stem cells throughout homeostasis and regeneration; more quiescent organs, such as the lung, often contain facultative progenitor cells that are recruited after injury to participate in regeneration. Here we show that a Wnt-responsive alveolar epithelial progenitor (AEP) lineage within the alveolar type 2 cell population acts as a major facultative progenitor cell in the distal lung. AEPs are a stable lineage during alveolar homeostasis but expand rapidly to regenerate a large proportion of the alveolar epithelium after acute lung injury. AEPs exhibit a distinct transcriptome, epigenome and functional phenotype and respond specifically to Wnt and Fgf signalling. In contrast to other proposed lung progenitor cells, human AEPs can be directly isolated by expression of the conserved cell surface marker TM4SF1, and act as functional human alveolar epithelial progenitor cells in 3D organoids. Our results identify the AEP lineage as an evolutionarily conserved alveolar progenitor that represents a new target for human lung regeneration strategies.

Published

2018

20. IL-17A-Induced PLET1 Expression Contributes to Tissue Repair and Colon Tumorigenesis.

Author

Zepp JA, Zhao J, Liu C, Bulek K, Wu L, Chen X, Hao Y, Wang Z, Wang X, Ouyang W, Kalady MF, Carman J, Yang WP, Zhu J, Blackburn C, Huang YH, Hamilton TA, Su B, and Li X

Subjects

Animals, Azoxymethane, Carcinogenesis, Cells, Cultured, Clustered Regularly Interspaced Short Palindromic Repeats, Colitis chemically induced, Colon pathology, Colonic Neoplasms chemically induced, Dextran Sulfate, Gene Expression Regulation, Neoplastic, Interleukin-17 genetics, Mice, Mice, Inbred C57BL, Mice, Knockout, Pregnancy Proteins genetics, Receptors, Interleukin genetics, Wound Healing, Colitis immunology, Colon metabolism, Colonic Neoplasms immunology, Epithelial Cells immunology, Interleukin-17 metabolism, Pregnancy Proteins metabolism

Abstract

This study identifies a novel mechanism linking IL-17A with colon tissue repair and tumor development. Abrogation of IL-17A signaling in mice attenuated tissue repair of dextran sulfate sodium (DSS)-induced damage in colon epithelium and markedly reduced tumor development in an azoxymethane/DSS model of colitis-associated cancer. A novel IL-17A target gene, PLET1 (a progenitor cell marker involved in wound healing), was highly induced in DSS-treated colon tissues and tumors in an IL-17RC-dependent manner. PLET1 expression was induced in LGR5 + colon epithelial cells after DSS treatment. LGR5 + PLET1 + marks a highly proliferative cell population with enhanced expression of IL-17A target genes. PLET1 deficiency impaired tissue repair of DSS-induced damage in colon epithelium and reduced tumor formation in an azoxymethane/DSS model of colitis-associated cancer. Our results suggest that IL-17A-induced PLET1 expression contributes to tissue repair and colon tumorigenesis., (Copyright © 2017 by The American Association of Immunologists, Inc.)

Published

2017

21. Distinct Mesenchymal Lineages and Niches Promote Epithelial Self-Renewal and Myofibrogenesis in the Lung.

Author

Zepp JA, Zacharias WJ, Frank DB, Cavanaugh CA, Zhou S, Morley MP, and Morrisey EE

Subjects

Algorithms, Animals, Epithelial Cells metabolism, Fibrosis metabolism, Gene Expression Profiling, Lung pathology, Lung physiology, Lung Injury pathology, Mice, Organoids cytology, Paracrine Communication, Regeneration, Signal Transduction, Single-Cell Analysis, Stem Cells metabolism, Lung cytology, Mesoderm cytology

Abstract

The lung is an architecturally complex organ comprising a heterogeneous mixture of various epithelial and mesenchymal lineages. We use single-cell RNA sequencing and signaling lineage reporters to generate a spatial and transcriptional map of the lung mesenchyme. We find that each mesenchymal lineage has a distinct spatial address and transcriptional profile leading to unique niche regulatory functions. The mesenchymal alveolar niche cell is Wnt responsive, expresses Pdgfrα, and is critical for alveolar epithelial cell growth and self-renewal. In contrast, the Axin2+ myofibrogenic progenitor cell preferentially generates pathologically deleterious myofibroblasts after injury. Analysis of the secretome and receptome of the alveolar niche reveals functional pathways that mediate growth and self-renewal of alveolar type 2 progenitor cells, including IL-6/Stat3, Bmp, and Fgf signaling. These studies define the cellular and molecular framework of lung mesenchymal niches and reveal the functional importance of developmental pathways in promoting self-renewal versus a pathological response to tissue injury., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

22. Emergence of a Wave of Wnt Signaling that Regulates Lung Alveologenesis by Controlling Epithelial Self-Renewal and Differentiation.

Author

Frank DB, Peng T, Zepp JA, Snitow M, Vincent TL, Penkala IJ, Cui Z, Herriges MJ, Morley MP, Zhou S, Lu MM, and Morrisey EE

Subjects

Animals, Axin Protein metabolism, Cell Lineage, Cell Proliferation, Clone Cells, Epithelial Cells metabolism, Epithelium embryology, Genes, Reporter, Integrases metabolism, Mice, Models, Biological, Organoids, Pulmonary Alveoli cytology, Cell Differentiation, Cell Self Renewal, Epithelial Cells cytology, Lung embryology, Organogenesis genetics, Pulmonary Alveoli embryology, Wnt Signaling Pathway genetics

Abstract

Alveologenesis is the culmination of lung development and involves the correct temporal and spatial signals to generate the delicate gas exchange interface required for respiration. Using a Wnt-signaling reporter system, we demonstrate the emergence of a Wnt-responsive alveolar epithelial cell sublineage, which arises during alveologenesis, called the axin2+ alveolar type 2 cell, or AT2 Axin2 . The number of AT2 Axin2 cells increases substantially during late lung development, correlating with a wave of Wnt signaling during alveologenesis. Transcriptome analysis, in vivo clonal analysis, and ex vivo lung organoid assays reveal that AT2s Axin2 promote enhanced AT2 cell growth during generation of the alveolus. Activating Wnt signaling results in the expansion of AT2s, whereas inhibition of Wnt signaling inhibits AT2 cell development and shunts alveolar epithelial development toward the alveolar type 1 cell lineage. These findings reveal a wave of Wnt-dependent AT2 expansion required for lung alveologenesis and maturation., (Copyright © 2016 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2016

23. T cell-intrinsic ASC critically promotes T(H)17-mediated experimental autoimmune encephalomyelitis.

Author

Martin BN, Wang C, Zhang CJ, Kang Z, Gulen MF, Zepp JA, Zhao J, Bian G, Do JS, Min B, Pavicic PG Jr, El-Sanadi C, Fox PL, Akitsu A, Iwakura Y, Sarkar A, Wewers MD, Kaiser WJ, Mocarski ES, Rothenberg ME, Hise AG, Dubyak GR, Ransohoff RM, and Li X

Subjects

Adenosine Triphosphate pharmacology, Animals, Apoptosis Regulatory Proteins genetics, Apoptosis Regulatory Proteins metabolism, CARD Signaling Adaptor Proteins, CD4-Positive T-Lymphocytes immunology, CD4-Positive T-Lymphocytes metabolism, Carrier Proteins genetics, Carrier Proteins immunology, Carrier Proteins metabolism, Caspase 8 genetics, Caspase 8 immunology, Caspase 8 metabolism, Cell Survival genetics, Cell Survival immunology, Cells, Cultured, Encephalomyelitis, Autoimmune, Experimental genetics, Encephalomyelitis, Autoimmune, Experimental metabolism, Flow Cytometry, Gene Expression immunology, Immunoblotting, Inflammasomes genetics, Inflammasomes immunology, Inflammasomes metabolism, Interleukin-17 genetics, Interleukin-17 immunology, Interleukin-17 metabolism, Interleukin-1beta genetics, Interleukin-1beta immunology, Interleukin-1beta metabolism, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, NLR Family, Pyrin Domain-Containing 3 Protein, Reverse Transcriptase Polymerase Chain Reaction, Signal Transduction genetics, Signal Transduction immunology, T-Lymphocytes drug effects, T-Lymphocytes metabolism, Th17 Cells drug effects, Th17 Cells metabolism, Apoptosis Regulatory Proteins immunology, Encephalomyelitis, Autoimmune, Experimental immunology, T-Lymphocytes immunology, Th17 Cells immunology

Abstract

Interleukin 1β (IL-1β) is critical for the in vivo survival, expansion and effector function of IL-17-producing helper T (T(H)17) cells during autoimmune responses, including experimental autoimmune encephalomyelitis (EAE). However, the spatiotemporal role and cellular source of IL-1β during EAE pathogenesis are poorly defined. In the present study, we uncovered a T cell-intrinsic inflammasome that drives IL-1β production during T(H)17-mediated EAE pathogenesis. Activation of T cell antigen receptors induced expression of pro-IL-1β, whereas ATP stimulation triggered T cell production of IL-1β via ASC-NLRP3-dependent caspase-8 activation. IL-1R was detected on T(H)17 cells but not on type 1 helper T (T(H)1) cells, and ATP-treated T(H)17 cells showed enhanced survival compared with ATP-treated T(H)1 cells, suggesting autocrine action of T(H)17-derived IL-1β. Together these data reveal a critical role for IL-1β produced by a T(H)17 cell-intrinsic ASC-NLRP3-caspase-8 inflammasome during inflammation of the central nervous system.

Published

2016

24. Human Colon Tumors Express a Dominant-Negative Form of SIGIRR That Promotes Inflammation and Colitis-Associated Colon Cancer in Mice.

Author

Zhao J, Bulek K, Gulen MF, Zepp JA, Karagkounis G, Martin BN, Zhou H, Yu M, Liu X, Huang E, Fox PL, Kalady MF, Markowitz SD, and Li X

Subjects

Animals, Azoxymethane, Cell Membrane metabolism, Colitis chemically induced, Colitis genetics, Colitis pathology, Colon pathology, Colonic Neoplasms chemically induced, Colonic Neoplasms genetics, Colonic Neoplasms pathology, Cytosol metabolism, Dextran Sulfate, Gene Expression Profiling methods, Gene Expression Regulation, Neoplastic, Genetic Predisposition to Disease, Glycosylation, HeLa Cells, Humans, Inflammation Mediators metabolism, Intestinal Mucosa pathology, Mice, 129 Strain, Mice, Inbred C57BL, Mice, Transgenic, Mutation, Oligonucleotide Array Sequence Analysis, Phenotype, Protein Processing, Post-Translational, RNA, Messenger metabolism, Receptors, Interleukin-1 genetics, Signal Transduction, Tissue Culture Techniques, Transfection, Colitis metabolism, Colon metabolism, Colonic Neoplasms metabolism, Genes, Dominant, Intestinal Mucosa metabolism, Receptors, Interleukin-1 metabolism

Abstract

Background & Aims: Single immunoglobulin and toll-interleukin 1 receptor (SIGIRR), a negative regulator of the Toll-like and interleukin-1 receptor (IL-1R) signaling pathways, controls intestinal inflammation and suppresses colon tumorigenesis in mice. However, the importance of SIGIRR in human colorectal cancer development has not been determined. We investigated the role of SIGIRR in development of human colorectal cancer., Methods: We performed RNA sequence analyses of pairs of colon tumor and nontumor tissues, each collected from 68 patients. Immunoblot and immunofluorescence analyses were used to determine levels of SIGIRR protein in primary human colonic epithelial cells, tumor tissues, and colon cancer cell lines. We expressed SIGIRR and mutant forms of the protein in Vaco cell lines. We created and analyzed mice that expressed full-length (control) or a mutant form of Sigirr (encoding SIGIRR(N86/102S), which is not glycosylated) specifically in the intestinal epithelium. Some mice were given azoxymethane (AOM) and dextran sulfate sodium to induce colitis-associated cancer. Intestinal tissues were collected and analyzed by immunohistochemical and gene expression profile analyses., Results: RNA sequence analyses revealed increased expression of a SIGIRR mRNA isoform, SIGIRR(ΔE8), in colorectal cancer tissues compared to paired nontumor tissues. SIGIRR(ΔE8) is not modified by complex glycans and is therefore retained in the cytoplasm-it cannot localize to the cell membrane or reduce IL1R signaling. SIGIRR(ΔE8) interacts with and has a dominant-negative effect on SIGIRR, reducing its glycosylation, localization to the cell surface, and function. Most SIGIRR detected in human colon cancer tissues was cytoplasmic, whereas in nontumor tissues it was found at the cell membrane. Mice that expressed SIGIRR(N86/102S) developed more inflammation and formed larger tumors after administration of azoxymethane and dextran sulfate sodium than control mice; colon tissues from these mutant mice expressed higher levels of the inflammatory cytokines IL-17A and IL-6 had activation of the transcription factors STAT3 and NFκB. SIGIRR(N86/102S) expressed in colons of mice did not localize to the epithelial cell surface., Conclusion: Levels of SIGIRR are lower in human colorectal tumors, compared with nontumor tissues; tumors contain the dominant-negative isoform SIGIRR(ΔE8). This mutant protein blocks localization of full-length SIGIRR to the surface of colon epithelial cells and its ability to downregulate IL1R signaling. Expression of SIGIRR(N86/102S) in the colonic epithelium of mice increases expression of inflammatory cytokines and formation and size of colitis-associated tumors., (Copyright © 2015 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published

2015

25. A novel IL-17 signaling pathway controlling keratinocyte proliferation and tumorigenesis via the TRAF4-ERK5 axis.

Author

Wu L, Chen X, Zhao J, Martin B, Zepp JA, Ko JS, Gu C, Cai G, Ouyang W, Sen G, Stark GR, Su B, Vines CM, Tournier C, Hamilton TA, Vidimos A, Gastman B, Liu C, and Li X

Subjects

Adaptor Proteins, Signal Transducing genetics, Adaptor Proteins, Signal Transducing metabolism, Animals, Carcinoma, Squamous Cell metabolism, Carcinoma, Squamous Cell pathology, Cell Proliferation genetics, Feedback, Physiological, Humans, Interleukin-17 genetics, MAP Kinase Kinase Kinase 3 genetics, MAP Kinase Kinase Kinase 3 metabolism, Membrane Proteins genetics, Membrane Proteins metabolism, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Mitogen-Activated Protein Kinase 7 genetics, Phosphoproteins genetics, Phosphoproteins metabolism, Receptors, Interleukin-17 genetics, Receptors, Interleukin-17 metabolism, Signal Transduction, Skin Neoplasms metabolism, Skin Neoplasms pathology, TNF Receptor-Associated Factor 4 genetics, Trans-Activators genetics, Trans-Activators metabolism, Interleukin-17 metabolism, Keratinocytes metabolism, Keratinocytes pathology, Mitogen-Activated Protein Kinase 7 metabolism, TNF Receptor-Associated Factor 4 metabolism

Abstract

Although IL-17 is emerging as an important cytokine in cancer promotion and progression, the underlining molecular mechanism remains unclear. Previous studies suggest that IL-17 (IL-17A) sustains a chronic inflammatory microenvironment that favors tumor formation. Here we report a novel IL-17-mediated cascade via the IL-17R-Act1-TRAF4-MEKK3-ERK5 positive circuit that directly stimulates keratinocyte proliferation and tumor formation. Although this axis dictates the expression of target genes Steap4 (a metalloreductase for cell metabolism and proliferation) and p63 (a transcription factor for epidermal stem cell proliferation), Steap4 is required for the IL-17-induced sustained expansion of p63(+) basal cells in the epidermis. P63 (a positive transcription factor for the Traf4 promoter) induces TRAF4 expression in keratinocytes. Thus, IL-17-induced Steap4-p63 expression forms a positive feedback loop through p63-mediated TRAF4 expression, driving IL-17-dependent sustained activation of the TRAF4-ERK5 axis for keratinocyte proliferation and tumor formation., (© 2015 Wu et al.)

Published

2015

26. A novel IL-25 signaling pathway through STAT5.

Author

Wu L, Zepp JA, Qian W, Martin BN, Ouyang W, Yin W, Bunting KD, Aronica M, Erzurum S, and Li X

Subjects

Animals, Cell Line, Connexin 43 metabolism, Cytokines metabolism, Epithelial Cells drug effects, Epithelial Cells metabolism, Humans, Ligands, Mice, Mice, Transgenic, Models, Biological, Peptide Fragments metabolism, Protein Binding, Receptors, Interleukin metabolism, Receptors, Interleukin-17 metabolism, Th2 Cells drug effects, Th2 Cells immunology, Th2 Cells metabolism, Interleukins metabolism, STAT5 Transcription Factor metabolism, Signal Transduction

Abstract

IL-25 is a member of the IL-17 family of cytokines that promotes Th2 cell-mediated inflammatory responses. IL-25 signals through a heterodimeric receptor (IL-25R) composed of IL-17RA and IL-17RB, which recruits the adaptor molecule Act1 for downstream signaling. Although the role of IL-25 in potentiating type 2 inflammation is well characterized by its ability to activate the epithelium as well as T cells, the components of its signaling cascade remain largely unknown. In this study, we found that IL-25 can directly activate STAT5 independently of Act1. Furthermore, conditional STAT5 deletion in T cells or epithelial cells led to a defective IL-25-initiated Th2 polarization as well as defective IL-25 enhancement of Th2 responses. Finally, we found that STAT5 is recruited to the IL-25R in a ligand-dependent manner through unique tyrosine residues on IL-17RB. Together, these findings reveal a novel Act1-independent IL-25 signaling pathway through STAT5 activation., (Copyright © 2015 by The American Association of Immunologists, Inc.)

Published

2015

27. TRAF4-SMURF2-mediated DAZAP2 degradation is critical for IL-25 signaling and allergic airway inflammation.

Author

Zepp JA, Wu L, Qian W, Ouyang W, Aronica M, Erzurum S, and Li X

Subjects

Animals, Carrier Proteins genetics, Carrier Proteins metabolism, Cells, Cultured, HEK293 Cells, Humans, Immunoblotting, Inflammation genetics, Inflammation metabolism, Interleukins immunology, Interleukins pharmacology, Mice, Inbred C57BL, Mice, Knockout, Models, Immunological, Mutation, Proteolysis, RNA Interference, RNA-Binding Proteins, Receptors, Interleukin genetics, Receptors, Interleukin metabolism, Receptors, Interleukin-17 deficiency, Receptors, Interleukin-17 genetics, Receptors, Interleukin-17 immunology, Respiratory System metabolism, Respiratory System pathology, Signal Transduction immunology, TNF Receptor-Associated Factor 4 deficiency, TNF Receptor-Associated Factor 4 genetics, Tyrosine genetics, Tyrosine immunology, Tyrosine metabolism, Ubiquitin-Protein Ligases deficiency, Ubiquitin-Protein Ligases genetics, Carrier Proteins immunology, Inflammation immunology, Receptors, Interleukin immunology, Respiratory System immunology, TNF Receptor-Associated Factor 4 immunology, Ubiquitin-Protein Ligases immunology

Abstract

IL-25 promotes type 2 immunity by inducing the expression of Th2-associated cytokines. Although it is known that the IL-25R (IL-17RB) recruits the adaptor protein ACT1, the IL-25R signaling mechanism remains poorly understood. While screening for IL-25R components, we found that IL-25 responses were impaired in Traf4 (-/-) cells. Administering IL-25 to Traf4 (-/-) mice resulted in blunted airway eosinophilia and Th2 cytokine production. Notably, IL-25R recruitment of TRAF4 was required for the ACT1/IL-25R interaction. Mechanistically, TRAF4 recruited the E3-ligase SMURF2, to degrade the IL-25R-inhibitory molecule DAZAP2. Silencing Dazap2 increased ACT1/IL-25R interaction and IL-25 responsiveness. Moreover, a tyrosine within the IL-25R elicited DAZAP2 interference. This study indicates that TRAF4-SMURF2-mediated DAZAP2 degradation is a crucial initiating event for the IL-25 response., (Copyright © 2015 by The American Association of Immunologists, Inc.)

Published

2015

28. IL-32 promotes angiogenesis.

Author

Nold-Petry CA, Rudloff I, Baumer Y, Ruvo M, Marasco D, Botti P, Farkas L, Cho SX, Zepp JA, Azam T, Dinkel H, Palmer BE, Boisvert WA, Cool CD, Taraseviciene-Stewart L, Heinhuis B, Joosten LA, Dinarello CA, Voelkel NF, and Nold MF

Subjects

Activins metabolism, Animals, Apoptosis physiology, Cells, Cultured, Endostatins metabolism, Familial Primary Pulmonary Hypertension, Glioblastoma embryology, Glioblastoma pathology, Human Umbilical Vein Endothelial Cells, Humans, Hypertension, Pulmonary metabolism, Hypertension, Pulmonary pathology, Integrin alphaVbeta3 metabolism, Interferon-gamma metabolism, Interleukin-8 metabolism, Matrix Metalloproteinase 9 metabolism, Mice, Nitrogen Oxides metabolism, Receptors, Vascular Endothelial Growth Factor antagonists & inhibitors, Receptors, Vascular Endothelial Growth Factor metabolism, Transforming Growth Factor beta1 metabolism, Vascular Endothelial Growth Factor A metabolism, Interleukins metabolism, Neovascularization, Pathologic metabolism, Neovascularization, Pathologic pathology

Abstract

IL-32 is a multifaceted cytokine with a role in infections, autoimmune diseases, and cancer, and it exerts diverse functions, including aggravation of inflammation and inhibition of virus propagation. We previously identified IL-32 as a critical regulator of endothelial cell (EC) functions, and we now reveal that IL-32 also possesses angiogenic properties. The hyperproliferative ECs of human pulmonary arterial hypertension and glioblastoma multiforme exhibited a markedly increased abundance of IL-32, and, significantly, the cytokine colocalized with integrin αVβ3. Vascular endothelial growth factor (VEGF) receptor blockade, which resulted in EC hyperproliferation, increased IL-32 three-fold. Small interfering RNA-mediated silencing of IL-32 negated the 58% proliferation of ECs that occurred within 24 h in scrambled-transfected controls. Reduction of IL-32 neither affected apoptosis (insignificant changes in Bak-1, Bcl-2, Bcl-xL, lactate dehydrogenase, annexin V, and propidium iodide) nor VEGF or TGF-β levels, but siIL-32-transfected adult and neonatal ECs produced up to 61% less NO, IL-8, and matrix metalloproteinase-9, and up to 3-fold more activin A and endostatin. In coculture-based angiogenesis assays, IL-32γ dose-dependently increased tube formation up to 3-fold; an αVβ3 inhibitor prevented this activity and reduced IL-32γ-induced IL-8 by 85%. In matrigel plugs loaded with IL-32γ, VEGF, or vehicle and injected into live mice, we observed the anticipated VEGF-induced increase in neocapillarization (8-fold versus vehicle), but unexpectedly, IL-32γ was equally angiogenic. A second signal such as IFN-γ was required to render cells responsive to exogenous IL-32γ; importantly, this was confirmed using a completely synthetic preparation of IL-32γ. In summary, we add angiogenic properties that are mediated by integrin αVβ3 but VEGF-independent to the portfolio of IL-32, implicating a role for this versatile cytokine in pulmonary arterial hypertension and neoplastic diseases.

Published

2014

29. The psoriasis-associated D10N variant of the adaptor Act1 with impaired regulation by the molecular chaperone hsp90.

Author

Wang C, Wu L, Bulek K, Martin BN, Zepp JA, Kang Z, Liu C, Herjan T, Misra S, Carman JA, Gao J, Dongre A, Han S, Bunting KD, Ko JS, Xiao H, Kuchroo VK, Ouyang W, and Li X

Subjects

Animals, Cell Line, Connexin 43 genetics, Connexin 43 immunology, Disease Models, Animal, Genetic Predisposition to Disease, Humans, Interleukin-17 metabolism, Mice, Mice, Knockout, Molecular Chaperones genetics, Mutation genetics, Peptide Fragments genetics, Peptide Fragments immunology, Polymorphism, Genetic, Protein Binding genetics, Protein Binding immunology, Psoriasis genetics, Signal Transduction, Connexin 43 metabolism, HSP90 Heat-Shock Proteins metabolism, Molecular Chaperones metabolism, Peptide Fragments metabolism, Psoriasis immunology, Th17 Cells immunology

Abstract

Act1 is an essential adaptor in interleukin 17 (IL-17)-mediated signaling and is recruited to the receptor for IL-17 after stimulation with IL-17. Here we found that Act1 was a 'client' protein of the molecular chaperone hsp90. The D10N variant of Act1 (Act1(D10N)) that is linked to susceptibility to psoriasis was defective in its interaction with hsp90, which resulted in a global loss of Act1 function. Act1-deficient mice modeled the mechanistic link between loss of Act1 function and susceptibility to psoriasis. Although Act1 was necessary for IL-17-mediated inflammation, Act1-deficient mice had a hyperactive response of the T(H)17 subset of helper T cells and developed spontaneous IL-22-dependent skin inflammation. In the absence of IL-17 signaling, IL-22 was the main contributor to skin inflammation, which provides a molecular mechanism for the association of Act1(D10N) with psoriasis susceptibility.

Published

2013

30. Cutting edge: TNF receptor-associated factor 4 restricts IL-17-mediated pathology and signaling processes.

Author

Zepp JA, Liu C, Qian W, Wu L, Gulen MF, Kang Z, and Li X

Subjects

Animals, Encephalomyelitis, Autoimmune, Experimental genetics, HEK293 Cells, HeLa Cells, Humans, Interleukin-17 genetics, Mice, Mice, Inbred C57BL, Mice, Knockout, RNA, Messenger biosynthesis, Signal Transduction genetics, TNF Receptor-Associated Factor 4 deficiency, TNF Receptor-Associated Factor 4 genetics, Th17 Cells immunology, Th17 Cells pathology, Encephalomyelitis, Autoimmune, Experimental immunology, Encephalomyelitis, Autoimmune, Experimental pathology, Interleukin-17 antagonists & inhibitors, Interleukin-17 physiology, Signal Transduction immunology, TNF Receptor-Associated Factor 4 physiology

Abstract

The effector T cell subset, Th17, plays a significant role in the pathogenesis of multiple sclerosis and of other autoimmune diseases. The signature cytokine, IL-17, engages the IL-17R and recruits the E3-ligase NF-κB activator 1 (Act1) upon stimulation. In this study, we examined the role of TNFR-associated factor (TRAF)4 in IL-17 signaling and Th17-mediated autoimmune encephalomyelitis. Primary cells from TRAF4-deficient mice displayed markedly enhanced IL-17-activated signaling pathways and induction of chemokine mRNA. Adoptive transfer of MOG35-55 specific wild-type Th17 cells into TRAF4-deficient recipient mice induced an earlier onset of disease. Mechanistically, we found that TRAF4 and TRAF6 used the same TRAF binding sites on Act1, allowing the competition of TRAF4 with TRAF6 for the interaction with Act1. Taken together, the results of this study reveal the necessity of a unique role of TRAF4 in restricting the effects of IL-17 signaling and Th17-mediated disease.

Published

2012

31. Protection from RNA and DNA viruses by IL-32.

Author

Zepp JA, Nold-Petry CA, Dinarello CA, and Nold MF

Subjects

Animals, Cell Line, Chlorocebus aethiops, Cytopathogenic Effect, Viral immunology, Endothelium, Vascular immunology, Endothelium, Vascular pathology, Endothelium, Vascular virology, Herpes Genitalis immunology, Herpes Genitalis pathology, Herpes Genitalis prevention & control, Humans, Inflammation Mediators therapeutic use, Interleukins therapeutic use, L-Lactate Dehydrogenase, Vero Cells, Vesicular Stomatitis immunology, Vesicular Stomatitis pathology, Vesicular Stomatitis prevention & control, Viral Load immunology, Herpesvirus 2, Human immunology, Herpesvirus 2, Human pathogenicity, Inflammation Mediators physiology, Interleukins physiology, Vesicular stomatitis Indiana virus immunology, Vesicular stomatitis Indiana virus pathogenicity

Abstract

Several studies have documented a proinflammatory role for IL-32, which induces IL-1α, IL-1β, IL-6, TNF, and chemokines via NF-κB, p38MAPK, and AP-1. However, IL-32 also participates in the responses to infection with viruses such as HIV-1 and influenza. In this study, we explored these antiviral properties of IL-32. Vital staining assays demonstrated that low concentrations (5-10 ng/ml) of rIL-32γ protected epithelial WISH cells from vesicular stomatitis virus-induced cell death. By lactate dehydrogenase assays, treatment with IL-32γ resulted in a 3- to 4-fold decrease in viral load. Specific silencing of IL-32 revealed that the antiviral responses triggered by the synthetic analogs of ssRNA viruses (polyuridine) and dsRNA viruses (polyinosinic-polycytidylic acid) were significantly weaker (2- to 3-fold more virus) in WISH cells in the absence of IL-32. Importantly, we discovered that the polyinosinic-polycytidylic acid-induced increase in production of IFN-α in human PBMC was nearly completely abolished when IL-32 was silenced. Moreover, we observed that IL-32 antagonizes the DNA virus HSV-2 in epithelial Vero cells as well as in human umbilical cord endothelial cells, as production of HSV-2 increased 8-fold upon silencing of IL-32 (p < 0.001). Mechanistically, we found that IL-32 used the PKR-eIF-2α as well as the MxA antiviral pathways. Unexpectedly, a considerable part of the antiviral properties of IL-32 was not dependent on IFNs; specific blockade of IFN activity reduced the antiviral properties of IL-32 only moderately. In conclusion, these data suggest a central role for IL-32 in the immune response to RNA and DNA viruses, which may be exploitable for clinical use in the future.

Published

2011

32. IL-37 is a fundamental inhibitor of innate immunity.

Author

Nold MF, Nold-Petry CA, Zepp JA, Palmer BE, Bufler P, and Dinarello CA

Subjects

Animals, Cell Line, Gene Knockdown Techniques, Humans, Interleukin-1 genetics, Mice, Mice, Transgenic, Signal Transduction, Smad3 Protein immunology, Immunity, Innate immunology, Interleukin-1 immunology

Abstract

The function of interleukin 37 (IL-37; formerly IL-1 family member 7) has remained elusive. Expression of IL-37 in macrophages or epithelial cells almost completely suppressed production of pro-inflammatory cytokines, whereas the abundance of these cytokines increased with silencing of endogenous IL-37 in human blood cells. Anti-inflammatory cytokines were unaffected. Mice with transgenic expression of IL-37 were protected from lipopolysaccharide-induced shock, and showed markedly improved lung and kidney function and reduced liver damage after treatment with lipopolysaccharide. Transgenic mice had lower concentrations of circulating and tissue cytokines (72-95% less) than wild-type mice and showed less dendritic cell activation. IL-37 interacted intracellularly with Smad3 and IL-37-expressing cells and transgenic mice showed less cytokine suppression when endogenous Smad3 was depleted. IL-37 thus emerges as a natural suppressor of innate inflammatory and immune responses.

Published

2010

33. Increased cytokine production in interleukin-18 receptor alpha-deficient cells is associated with dysregulation of suppressors of cytokine signaling.

Author

Nold-Petry CA, Nold MF, Nielsen JW, Bustamante A, Zepp JA, Storm KA, Hong JW, Kim SH, and Dinarello CA

Subjects

Animals, Cell Line, Tumor, Cytokines genetics, Humans, Interleukin-18 genetics, Interleukin-18 metabolism, Interleukin-18 Receptor alpha Subunit genetics, Mice, Mice, Knockout, Protein Kinases genetics, Protein Kinases metabolism, Suppressor of Cytokine Signaling 1 Protein, Suppressor of Cytokine Signaling 3 Protein, Suppressor of Cytokine Signaling Proteins genetics, Cytokines biosynthesis, Interleukin-18 Receptor alpha Subunit metabolism, MAP Kinase Signaling System physiology, Suppressor of Cytokine Signaling Proteins metabolism

Abstract

Since interleukin (IL)-18 is a proinflammatory cytokine, mice lacking IL-18 or its ligand-binding receptor (IL-18R) should exhibit decreased cytokine and chemokine production. Indeed, production of IL-1alpha, IL-6, and MIP-1alpha was reduced in IL-18 knock-out (ko) mouse embryonic fibroblast (MEF)-like cells. Unexpectedly, we observed a paradoxical 10-fold increase in IL-1beta-induced IL-6 production in MEF cells from mice deficient in the IL-18R alpha-chain (IL-18Ralpha) compared with wild type MEF. Similar increases were observed for IL-1alpha, MIP-1alpha, and prostaglandin E2. Likewise, coincubation with a specific IL-18Ralpha-blocking antibody augmented IL-1beta-induced cytokines in wild type and IL-18 ko MEF. Stable lines of IL-18Ralpha-depleted human A549 cells were generated using shRNA, resulting in an increase of IL-1beta-induced IL-1alpha, IL-6, and IL-8 compared to scrambled small hairpin RNA. In addition, we silenced IL-18Ralpha with small interfering RNA in primary human blood cells and observed up to 4-fold increases in the secretion of lipopolysaccharide- and IL-12/IL-18-induced IL-1beta, IL-6, interferon-gamma, and CD40L. Mechanistically, despite increases in Stat1 and IL-6, induction of SOCS1 and -3 (suppressor of cytokine signaling 1 and 3) was markedly reduced in the absence of IL-18Ralpha. Consistent with these observations, activation of the p38alpha/beta and ERK1/2 MAPKs and of protein kinase B/Akt increased in IL-18Ralpha ko MEF, whereas the negative feedback kinase MSK2 was more active in IL-18 ko cells. These data reveal a role for SOCS1 and -3 in the seemingly paradoxical hyperresponsive state in cells deficient in IL-18Ralpha, supporting the concept that IL-18Ralpha participates in both pro- and anti-inflammatory responses and that an endogenous ligand engages IL-18Ralpha to deliver an inhibitory signal.

Published

2009

34. IL-32-dependent effects of IL-1beta on endothelial cell functions.

Author

Nold-Petry CA, Nold MF, Zepp JA, Kim SH, Voelkel NF, and Dinarello CA

Subjects

Blood Platelets drug effects, Blood Platelets metabolism, Endothelial Cells drug effects, Endothelial Cells enzymology, Gene Expression Profiling, Gene Expression Regulation drug effects, Gene Silencing drug effects, Humans, I-kappa B Kinase metabolism, Intercellular Adhesion Molecule-1 metabolism, Interleukin-1beta pharmacology, Interleukins genetics, Lipopolysaccharides pharmacology, NF-kappa B metabolism, Protein Isoforms genetics, Protein Isoforms metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, RNA, Small Interfering metabolism, Thrombin pharmacology, Thrombomodulin metabolism, Umbilical Veins cytology, Endothelial Cells cytology, Endothelial Cells metabolism, Interleukin-1beta metabolism, Interleukins metabolism

Abstract

Increasing evidence demonstrates that interleukin (IL)-32 is a pro-inflammatory cytokine, inducing IL-1alpha, IL-1beta, IL-6, tumor necrosis factor (TNF)-alpha, and chemokines via nuclear factor (NF)-kappaB, p38 mitogen-activated protein kinase (MAPK), and activating protein (AP)-1 activation. Here we report that IL-32 is expressed and is also functional in human vascular endothelial cells (EC) of various origins. Compared with primary blood monocytes, high levels of IL-32 are constitutively produced in human umbilical vein EC (HUVEC), aortic macrovascular EC, and cardiac as well as pulmonary microvascular EC. At concentrations as low as 0.1 ng/ml, IL-1beta stimulated IL-32 up to 15-fold over constitutive levels, whereas 10 ng/ml of TNFalpha or 100 ng/ml of lipopolysaccharide (LPS) were required to induce similar quantities of IL-32. IL-1beta-induced IL-32 was reduced by inhibition of the IkappaB kinase-beta/NF-kappaB and ERK pathways. In addition to IL-1beta, pro-coagulant concentrations of thrombin or fresh platelets increased IL-32 protein up to 6-fold. IL-1beta and thrombin induced an isoform-switch in steady-state mRNA levels from IL-32alpha/gamma to beta/epsilon. Adult EC responded in a similar fashion. To prove functionality, we silenced endogenous IL-32 with siRNA, decreasing intracellular IL-32 protein levels by 86%. The knockdown of IL-32 resulted in reduction of constitutive as well as IL-1beta-induced intercellular adhesion molecule-1 (ICAM-1) (of 55% and 54%, respectively), IL-1alpha (of 62% and 43%), IL-6 (of 53% and 43%), and IL-8 (of 46% and 42%). In contrast, the anti-inflammatory/anti-coagulant CD141/thrombomodulin increased markedly when IL-32 was silenced. This study introduces IL-32 as a critical regulator of endothelial function, expanding the properties of this cytokine relevant to coagulation, endothelial inflammation, and atherosclerosis.

Published

2009

35. Endogenous IL-32 controls cytokine and HIV-1 production.

Author

Nold MF, Nold-Petry CA, Pott GB, Zepp JA, Saavedra MT, Kim SH, and Dinarello CA

Subjects

Cells, Cultured, Cytokines genetics, DNA metabolism, HIV Core Protein p24 biosynthesis, Humans, Interleukins deficiency, NF-kappa B metabolism, Protein Binding, RNA, Small Interfering genetics, Transcription Factor AP-1 metabolism, Up-Regulation, Anti-HIV Agents metabolism, Cytokines biosynthesis, HIV-1 metabolism, Interleukins metabolism

Abstract

IL-32, a proinflammatory cytokine that activates the p38MAPK and NF-kappaB pathways, induces other cytokines, for example, IL-1beta, IL-6, and TNF-alpha. This study investigated the role of endogenous IL-32 in HIV-1 infection by reducing IL-32 with small interfering (si)RNA in freshly infected PBMC and in the latently infected U1 macrophage cell line. When PBMC were pretreated with siRNA to IL-32 (siIL-32), IL-6, IFN-gamma, and TNF-alpha were reduced by 57, 51, and 36%, respectively, compared with scrambled siRNA. Cotransfection of NF-kappaB and AP-1 reporter constructs with siIL-32 decreased DNA binding of these transcription factors by 42 and 46%, respectively. Cytokine protein array analysis revealed that the inhibitory activity of siIL-32 primarily targeted Th1 and proinflammatory cytokines and chemokines, e.g., MIP-1alpha/beta. Unexpectedly, HIV-1 production (as measured by p24) increased 4-fold in these same PBMC when endogenous IL-32 was reduced. Because IFN-gamma was lower in siIL-32-treated PBMC, we blocked IFN-gamma bioactivity, which enhanced the augmentation of p24 by siIL-32. Furthermore, siIL-32 reduced the natural ligands of the HIV-1 coreceptors CCR5 (MIP-1alpha/beta and RANTES) and CXCR4 (SDF-1). Inhibition of endogenous IL-32 in U1 macrophages also increased HIV-1. When rhIL-32gamma was added to these cells, p24 levels fell by 72%; however, in the same cultures IFN-alpha increased 4-fold. Blockade of IFN-alpha/beta bioactivity in IL-32gamma-stimulated U1 cells revealed that IFN-alpha conveys the anti-HIV-1 effect of rhIL-32gamma. In summary, depletion of endogenous IL-32 reduced the levels of Th1 and proinflammatory cytokines but paradoxically increased p24, proposing IL-32 as a natural inhibitor of HIV-1.

Published

2008