Your search keyword '"ciliated cells"' showing total 243 results

1. Transcriptomic Analysis of Air–Liquid Interface Culture in Human Lung Organoids Reveals Regulators of Epithelial Differentiation.

Author

Kim, Jieun, Eo, Eun-Young, Kim, Bokyong, Lee, Heetak, Kim, Jihoon, Koo, Bon-Kyoung, Kim, Hyung-Jun, Cho, Sukki, Kim, Jinho, and Cho, Young-Jae

Subjects

*CELL differentiation, *RNA sequencing, *EPITHELIAL cells, *CELL culture, *EPITHELIUM, *LUNGS

Abstract

To develop in vitro respiratory models, it is crucial to identify the factors involved in epithelial cell differentiation. In this study, we comprehensively analyzed the effects of air–liquid interface (ALI) culture on epithelial cell differentiation using single-cell RNA sequencing (scRNA-seq). ALI culture induced a pronounced shift in cell composition, marked by a fivefold increase in ciliated cells and a reduction of more than half in basal cells. Transcriptional signatures associated with epithelial cell differentiation, analyzed using iPathwayGuide software, revealed the downregulation of VEGFA and upregulation of CDKN1A as key signals for epithelial differentiation. Our findings highlight the efficacy of the ALI culture for replicating the human lung airway epithelium and provide valuable insights into the crucial factors that influence human ciliated cell differentiation. [ABSTRACT FROM AUTHOR]

Published

2024

2. Tropism of adeno-associated virus serotypes in mouse lungs via intratracheal instillation

Author

Haoyu Wu, Ailing Zhao, Ye Bu, Weiping Yang, Lang He, Yujian Zhong, Dong Yao, Huapeng Li, and Wenguang Yin

Subjects

Adeno-associated virus, Tropism, Club cells, Ciliated cells, Alveolar epithelial cells, Infectious and parasitic diseases, RC109-216

Abstract

Abstract Background Gene therapy holds great potential for treating various acquired and inherited pulmonary diseases. Adeno-associated viral (AAV) vectors have been thought to be primary candidates for gene delivery in patients with pulmonary diseases. However, the tropism of AAVs in the lungs remains largely unknown. Results Here, we investigate the tropism of twenty serotypes of AAVs by examining AAV-packed vector expression of the enhanced green fluorescent protein (eGFP) in mice. AAV1, AAV4, AAV5, AAV6, AAV6.2, AAV-PHP.B, and AAV-PHP.S exhibit high transduction rates in the airway epithelium. AAV1, AAV4, AAV5, AAV6, and AAV6.2 highly infect club cells. AAV1, AAV4, AAV5, AAV6, AAV6.2, and AAV-PHP.B efficiently infect ciliated cells. AAV8 and AAVrh10 can infect a few alveolar type I cells. AAV1, AAV5, AAV6, AAV6.2, AAV9, and AAVie can infect alveolar type II cells. AAV1, AAV5, AAVie, AAV-PHP.B, AAV-PHP.eB, and AAV-PHP.S can infect a few endothelial cells. However, none of these AAVs can efficiently infect neuroendocrine or smooth muscle cells. Conclusions Our findings provide comprehensive information about the tropism of AAVs in pulmonary epithelium in mice, which might be helpful in developing efficient AAV-mediated gene therapy strategies for pulmonary disease treatment.

Published

2024

3. Single-cell transcriptomics reveals e-cigarette vapor-induced airway epithelial remodeling and injury

Author

Weitao Cao, Jia Li, Li Che, Ruixue Yang, Zehong Wu, Guoping Hu, Weifeng Zou, Zehang Zhao, Yumin Zhou, Xingtao Jiang, Tiejun Zhang, Wenguang Yin, and Pixin Ran

Subjects

E-cigarette, COPD, Ciliated cells, Cilia, Notch signaling, Diseases of the respiratory system, RC705-779

Abstract

Abstract Background In recent years, e-cigarettes have been used as alternatives among adult smokers. However, the impact of e-cigarette use on human bronchial epithelial (HBE) cells remains controversial. Methods We collected primary HBE cells of healthy nonsmokers and chronic obstructive pulmonary disease (COPD) smokers, and analyzed the impact of e- cigarette vapor extract (ECE) or cigarette smoke extract (CSE) on HBE cell differentiation and injury by single-cell RNA sequencing, immunostaining, HE staining, qPCR and ELISA. We obtained serum and sputum from healthy non- smokers, smokers and e-cigarette users, and analyzed cell injury markers and mucin proteins. Results ECE treatment led to a distinct differentiation program of ciliated cells and unique patterns of their cell–cell communications compared with CSE. ECE treatment caused increased Notch signaling strength in a ciliated cell subpopulation, and HBE cell remodeling and injury including hypoplasia of ciliated cells and club cells, and shorter cilia. ECE-induced hypoplasia of ciliated cells and shorter cilia were ameliorated by the Notch signaling inhibition. Conclusions This study reveals distinct characteristics in e-cigarette vapor-induced airway epithelial remodeling, pointing to Notch signaling pathway as a potential targeted intervention for e-cigarette vapor-caused ciliated cell differentiation defects and cilia injury. In addition, a decrease in SCGB1A1 proteins is associated with e- cigarette users, indicating a potential lung injury marker for e-cigarette users.

Published

2024

4. Tropism of adeno-associated virus serotypes in mouse lungs via intratracheal instillation.

Author

Wu, Haoyu, Zhao, Ailing, Bu, Ye, Yang, Weiping, He, Lang, Zhong, Yujian, Yao, Dong, Li, Huapeng, and Yin, Wenguang

Subjects

GREEN fluorescent protein, LUNG diseases, ADENO-associated virus, GENE therapy, EPITHELIAL cells, VIRAL tropism

Abstract

Background: Gene therapy holds great potential for treating various acquired and inherited pulmonary diseases. Adeno-associated viral (AAV) vectors have been thought to be primary candidates for gene delivery in patients with pulmonary diseases. However, the tropism of AAVs in the lungs remains largely unknown. Results: Here, we investigate the tropism of twenty serotypes of AAVs by examining AAV-packed vector expression of the enhanced green fluorescent protein (eGFP) in mice. AAV1, AAV4, AAV5, AAV6, AAV6.2, AAV-PHP.B, and AAV-PHP.S exhibit high transduction rates in the airway epithelium. AAV1, AAV4, AAV5, AAV6, and AAV6.2 highly infect club cells. AAV1, AAV4, AAV5, AAV6, AAV6.2, and AAV-PHP.B efficiently infect ciliated cells. AAV8 and AAVrh10 can infect a few alveolar type I cells. AAV1, AAV5, AAV6, AAV6.2, AAV9, and AAVie can infect alveolar type II cells. AAV1, AAV5, AAVie, AAV-PHP.B, AAV-PHP.eB, and AAV-PHP.S can infect a few endothelial cells. However, none of these AAVs can efficiently infect neuroendocrine or smooth muscle cells. Conclusions: Our findings provide comprehensive information about the tropism of AAVs in pulmonary epithelium in mice, which might be helpful in developing efficient AAV-mediated gene therapy strategies for pulmonary disease treatment. [ABSTRACT FROM AUTHOR]

Published

2024

5. Airway epithelium damage in acute respiratory distress syndrome.

Author

Gerard, Ludovic, Lecocq, Marylene, Detry, Bruno, Bouzin, Caroline, Hoton, Delphine, Pinto Pereira, Joao, Carlier, François, Plante-Bordeneuve, Thomas, Gohy, Sophie, Lacroix, Valérie, Laterre, Pierre-François, and Pilette, Charles

Abstract

Background: The airway epithelium (AE) fulfils multiple functions to maintain pulmonary homeostasis, among which ensuring adequate barrier function, cell differentiation and polarization, and actively transporting immunoglobulin A (IgA), the predominant mucosal immunoglobulin in the airway lumen, via the polymeric immunoglobulin receptor (pIgR). Morphological changes of the airways have been reported in ARDS, while their detailed features, impact for mucosal immunity, and causative mechanisms remain unclear. Therefore, this study aimed to assess epithelial alterations in the distal airways of patients with ARDS. Methods: We retrospectively analyzed lung tissue samples from ARDS patients and controls to investigate and quantify structural and functional changes in the small airways, using multiplex fluorescence immunostaining and computer-assisted quantification on whole tissue sections. Additionally, we measured markers of mucosal immunity, IgA and pIgR, alongside with other epithelial markers, in the serum and the broncho-alveolar lavage fluid (BALF) prospectively collected from ARDS patients and controls. Results: Compared to controls, airways of ARDS were characterized by increased epithelial denudation (p = 0.0003) and diffuse epithelial infiltration by neutrophils (p = 0.0005). Quantitative evaluation of multiplex fluorescence immunostaining revealed a loss of ciliated cells (p = 0.0317) a trend towards decreased goblet cells (p = 0.056), and no change regarding cell progenitors (basal and club cells), indicating altered mucociliary differentiation. Increased epithelial permeability was also shown in ARDS with a significant decrease of tight (p < 0.0001) and adherens (p = 0.025) junctional proteins. Additionally, we observed a significant decrease of the expression of pIgR, (p < 0.0001), indicating impaired mucosal IgA immunity. Serum concentrations of secretory component (SC) and S-IgA were increased in ARDS (both p < 0.0001), along other lung-derived proteins (CC16, SP-D, sRAGE). However, their BALF concentrations remained unchanged, suggesting a spillover of airway and alveolar proteins through a damaged AE. Conclusion: The airway epithelium from patients with ARDS exhibits multifaceted alterations leading to altered mucociliary differentiation, compromised defense functions and increased permeability with pneumoproteinemia. [ABSTRACT FROM AUTHOR]

Published

2024

6. Single-cell transcriptomics reveals e-cigarette vapor-induced airway epithelial remodeling and injury.

Author

Cao, Weitao, Li, Jia, Che, Li, Yang, Ruixue, Wu, Zehong, Hu, Guoping, Zou, Weifeng, Zhao, Zehang, Zhou, Yumin, Jiang, Xingtao, Zhang, Tiejun, Yin, Wenguang, and Ran, Pixin

Subjects

NOTCH signaling pathway, CHRONIC obstructive pulmonary disease, SMOKING, E-cigarette or vaping product use-associated lung injuries, ELECTRONIC cigarettes

Abstract

Background: In recent years, e-cigarettes have been used as alternatives among adult smokers. However, the impact of e-cigarette use on human bronchial epithelial (HBE) cells remains controversial. Methods: We collected primary HBE cells of healthy nonsmokers and chronic obstructive pulmonary disease (COPD) smokers, and analyzed the impact of e- cigarette vapor extract (ECE) or cigarette smoke extract (CSE) on HBE cell differentiation and injury by single-cell RNA sequencing, immunostaining, HE staining, qPCR and ELISA. We obtained serum and sputum from healthy non- smokers, smokers and e-cigarette users, and analyzed cell injury markers and mucin proteins. Results: ECE treatment led to a distinct differentiation program of ciliated cells and unique patterns of their cell–cell communications compared with CSE. ECE treatment caused increased Notch signaling strength in a ciliated cell subpopulation, and HBE cell remodeling and injury including hypoplasia of ciliated cells and club cells, and shorter cilia. ECE-induced hypoplasia of ciliated cells and shorter cilia were ameliorated by the Notch signaling inhibition. Conclusions: This study reveals distinct characteristics in e-cigarette vapor-induced airway epithelial remodeling, pointing to Notch signaling pathway as a potential targeted intervention for e-cigarette vapor-caused ciliated cell differentiation defects and cilia injury. In addition, a decrease in SCGB1A1 proteins is associated with e- cigarette users, indicating a potential lung injury marker for e-cigarette users. [ABSTRACT FROM AUTHOR]

Published

2024

7. Cell type-specific regulation of CFTR trafficking—on the verge of progress.

Author

Farinha, Carlos M., Santos, Lúcia, and Ferreira, João F.

Subjects

CYSTIC fibrosis transmembrane conductance regulator, CELLULAR control mechanisms, TRAFFIC regulations, CELL membranes

Abstract

Trafficking of the Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) protein is a complex process that starts with its biosynthesis and folding in the endoplasmic reticulum. Exit from the endoplasmic reticulum (ER) is coupled with the acquisition of a compact structure that can be processed and traffic through the secretory pathway. Once reaching its final destination—the plasma membrane, CFTR stability is regulated through interaction with multiple protein partners that are involved in its post-translation modification, connecting the channel to several signaling pathways. The complexity of the process is further boosted when analyzed in the context of the airway epithelium. Recent advances have characterized in detail the different cell types that compose the surface epithelium and shifted the paradigm on which cells express CFTR and on their individual and combined contribution to the total expression (and function) of this chloride/bicarbonate channel. Here we review CFTR trafficking and its relationship with the knowledge on the different cell types of the airway epithelia. We explore the crosstalk between these two areas and discuss what is still to be clarified and how this can be used to develop more targeted therapies for CF. [ABSTRACT FROM AUTHOR]

Published

2024

8. Ciliated Cells in Ovarian Cancer Decrease with Increasing Tumor Grade and Disease Progression

Author

Richardson, Michael T, Recouvreux, Maria Sol, Karlan, Beth Y, Walts, Ann E, and Orsulic, Sandra

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Ovarian Cancer, Women's Health, Rare Diseases, Cancer, Humans, Female, Ovarian Neoplasms, Carcinoma, Ovarian Epithelial, Epithelial Cells, Fallopian Tubes, Disease Progression, fallopian tube, ciliated cells, secretory cells, ovarian cancer, serous, mucinous, endometrioid, clear cell, CAPS, FOXJ1, Biological sciences, Biomedical and clinical sciences

Abstract

Ciliated cell markers expressed in epithelial ovarian cancers (EOC) are associated with improved survival. We examined the distribution of cells expressing ciliated cell markers in various EOC histologies and stages. Immunohistochemistry and/or multiplex immunofluorescence were used to determine the expression of FOXJ1 and/or CAPS (ciliated cell markers) in tissue microarrays including 4 normal fallopian tubes, 6 normal endometria, 16 cystadenomas, 25 borderline tumors, 21 low-grade carcinomas, and 118 high-grade carcinomas (HGSOC) (46 serous, 29 endometrioid, 30 clear cell, 13 mucinous). CAPS+ cells were observed in normal fallopian tubes and endometria and in ~85% of serous benign and borderline tumors and low-grade carcinomas but only in

Published

2022

9. Single-Cell RNA-Seq Analysis Reveals Lung Epithelial Cell Type-Specific Responses to HDM and Regulation by Tet1

Author

Zhu, Tao, Brown, Anthony P, Cai, Lucy P, Quon, Gerald, and Ji, Hong

Subjects

Biological Sciences, Genetics, Human Genome, Lung, Social Determinants of Health, Health Effects of Indoor Air Pollution, 2.1 Biological and endogenous factors, Respiratory, Inflammatory and immune system, Animals, Asthma, DNA-Binding Proteins, Epithelial Cell Adhesion Molecule, Epithelial Cells, Mice, Mice, Knockout, Pneumonia, Proto-Oncogene Proteins, Pyroglyphidae, Sequence Analysis, RNA, Single-Cell Analysis, allergic lung inflammation, Tet1, single-cell RNA-seq, alveolar type 2 (AT2) cells, ciliated cells

Abstract

Tet1 protects against house dust mite (HDM)-induced lung inflammation in mice and alters the lung methylome and transcriptome. In order to explore the role of Tet1 in individual lung epithelial cell types in HDM-induced inflammation, we established a model of HDM-induced lung inflammation in Tet1 knockout and littermate wild-type mice, then studied EpCAM+ lung epithelial cells using single-cell RNA-seq analysis. We identified eight EpCAM+ lung epithelial cell types, among which AT2 cells were the most abundant. HDM challenge altered the relative abundance of epithelial cell types and resulted in cell type-specific transcriptomic changes. Bulk and cell type-specific analysis also showed that loss of Tet1 led to the altered expression of genes linked to augmented HDM-induced lung inflammation, including alarms, detoxification enzymes, oxidative stress response genes, and tissue repair genes. The transcriptomic regulation was accompanied by alterations in TF activities. Trajectory analysis supports that HDM may enhance the differentiation of AP and BAS cells into AT2 cells, independent of Tet1. Collectively, our data showed that lung epithelial cells had common and unique transcriptomic signatures of allergic lung inflammation. Tet1 deletion altered transcriptomic networks in various lung epithelial cells, which may promote allergen-induced lung inflammation.

Published

2022

10. Cell type-specific regulation of CFTR trafficking—on the verge of progress

Author

Carlos M. Farinha, Lúcia Santos, and João F. Ferreira

Subjects

CFTR, protein trafficking, airway epithelium, ionocytes, ciliated cells, basal cells, Biology (General), QH301-705.5

Abstract

Trafficking of the Cystic Fibrosis Transmembrane Conductance Regulator (CFTR) protein is a complex process that starts with its biosynthesis and folding in the endoplasmic reticulum. Exit from the endoplasmic reticulum (ER) is coupled with the acquisition of a compact structure that can be processed and traffic through the secretory pathway. Once reaching its final destination—the plasma membrane, CFTR stability is regulated through interaction with multiple protein partners that are involved in its post-translation modification, connecting the channel to several signaling pathways. The complexity of the process is further boosted when analyzed in the context of the airway epithelium. Recent advances have characterized in detail the different cell types that compose the surface epithelium and shifted the paradigm on which cells express CFTR and on their individual and combined contribution to the total expression (and function) of this chloride/bicarbonate channel. Here we review CFTR trafficking and its relationship with the knowledge on the different cell types of the airway epithelia. We explore the crosstalk between these two areas and discuss what is still to be clarified and how this can be used to develop more targeted therapies for CF.

Published

2024

11. The Path from Nasal Tissue to Nasal Mucosa on Chip: Part 1—Establishing a Nasal In Vitro Model for Drug Delivery Testing Based on a Novel Cell Line.

Author

Bendas, Sebastian, Koch, Eugen Viktor, Nehlsen, Kristina, May, Tobias, Dietzel, Andreas, and Reichl, Stephan

Subjects

*NASAL mucosa, *CELL lines, *DRUG delivery systems, *DRUG registration, *DRUG absorption, *CELL culture

Abstract

In recent years, there has been a significant increase in the registration of drugs for nasal application with systemic effects. Previous preclinical in vitro test systems for transmucosal drug absorption studies have mostly been based on primary cells or on tumor cell lines such as RPMI 2650, but both approaches have disadvantages. Therefore, the aim of this study was to establish and characterize a novel immortalized nasal epithelial cell line as the basis for an improved 3D cell culture model of the nasal mucosa. First, porcine primary cells were isolated and transfected. The P1 cell line obtained from this process was characterized in terms of its expression of tissue-specific properties, namely, mucus expression, cilia formation, and epithelial barrier formation. Using air–liquid interface cultivation, it was possible to achieve both high mucus formation and the development of functional cilia. Epithelial integrity was expressed as both transepithelial electrical resistance and mucosal permeability, which was determined for sodium fluorescein, rhodamine B, and FITC-dextran 4000. We noted a high comparability of the novel cell culture model with native excised nasal mucosa in terms of these measures. Thus, this novel cell line seems to offer a promising approach for developing 3D nasal mucosa tissues that exhibit favorable characteristics to be used as an in vitro system for testing drug delivery systems. [ABSTRACT FROM AUTHOR]

Published

2023

12. Generation of Complete Multi-Cell Type Lung Organoids From Human Embryonic and Patient-Specific Induced Pluripotent Stem Cells for Infectious Disease Modeling and Therapeutics Validation.

Author

Leibel, Sandra, McVicar, Rachael, Winquist, Alicia, Niles, Walter, and Snyder, Evan

Subjects

SARS-CoV-2 viral infection, ciliated cells, differentiation, endoderm, human pluripotent stem cells, lung development, lung organoid, pulmonary disease modeling, smooth muscle, surfactant, type 1 alveolar cells, type 2 alveolar cells, Betacoronavirus, COVID-19, Cell Culture Techniques, Cell Differentiation, Coronavirus Infections, Endoderm, Human Embryonic Stem Cells, Humans, Induced Pluripotent Stem Cells, Lung, Models, Biological, Organoids, Pandemics, Patient-Specific Modeling, Pneumonia, Viral, Respiratory Tract Infections, SARS-CoV-2, Time-Lapse Imaging

Abstract

The normal development of the pulmonary system is critical to transitioning from placental-dependent fetal life to alveolar-dependent newborn life. Human lung development and disease have been difficult to study due to the lack of an in vitro model system containing cells from the large airways and distal alveolus. This article describes a system that allows human embryonic stem cells (hESCs) and induced pluripotent stem cells (hiPSCs) to differentiate and form three-dimensional (3D) structures that emulate the development, cytoarchitecture, and function of the lung (organoids), containing epithelial and mesenchymal cell populations, and including the production of surfactant and presence of ciliated cells. The organoids can also be invested with mesoderm derivatives, differentiated from the same human pluripotent stem cells, such as alveolar macrophages and vasculature. Such lung organoids may be used to study the impact of environmental modifiers and perturbagens (toxins, microbial or viral pathogens, alterations in microbiome) or the efficacy and safety of drugs, biologics, and gene transfer. © 2020 Wiley Periodicals LLC. Basic Protocol: hESC/hiPSC dissection, definitive endoderm formation, and lung progenitor cell induction.

Published

2020

13. Evaluation of chronic cigarette smoke exposure in human bronchial epithelial cultures.

Author

Tyrrell, Jean, Ghosh, Arunava, Manzo, Nicholas D., Randell, Scott H., and Tarran, Robert

Subjects

CIGARETTE smoke, SMOKING, MUCOCILIARY system, TOBACCO products, TOBACCO smoke, LIQUID surfaces, PERFUSION

Abstract

Cigarette smoke (CS) exposure induces both cytotoxicity and inflammation, and often causes COPD, a growing cause of morbidity and mortality. CS also inhibits the CFTR Cl‐ channel, leading to airway surface liquid dehydration, which is predicated to impair clearance of inhaled pathogens and toxicants. Numerous in vitro studies have been performed that utilize acute (≤24 h) CS exposures. However, CS exposure is typically chronic. We evaluated the feasibility of using British‐American Tobacco (BAT)‐designed CS exposure chambers for chronically exposing human bronchial epithelial cultures (HBECs) to CS. HBECs are polarized and contain mucosal and serosal sides. In vivo, inhaled CS interacts with mucosal membranes, and BAT chambers are designed to direct CS to HBEC mucosal surfaces while keeping CS away from serosal surfaces via a perfusion system. We found that serosal perfusion was absolutely required to maintain HBEC viability over time following chronic CS exposure. Indeed, with this system, we found that CS increased inflammation and mucin levels, while decreasing CFTR function. Without this serosal perfusion, CS was extremely toxic within 24 h. We therefore propose that 5‐ and 10‐day CS exposures with serosal perfusion are suitable for measuring chronic CS exposure and can be used for monitoring new and emerging tobacco products. Cigarette smoke (CS) exposure induces cytotoxicity and inflammation. We chronically exposed human bronchial epithelial cultures (HBECs) to CS. HBECs remained viable for 10 days. However, serosal perfusion with a physiologically‐relevant buffer during smoke exposure was critical for maintaining HBEC viability, and without this perfusion, CS was extremely toxic within 24 h. We propose that serosal perfusion is absolutely required when measuring chronic CS exposure and that this technique can be used for monitoring new and emerging tobacco products. [ABSTRACT FROM AUTHOR]

Published

2023

14. Immunohistochemical identification of epithelial cell types in the isthmus of bovine oviduct: Comparison with the ampulla

Author

Sayaka ITO, Yuna YAMAGUCHI, Sayaka KUBOTA, Yuki YAMAMOTO, and Koji KIMURA

Subjects

characterization, ciliated cells, cow, isthmic oviductal epithelium, proliferation, Reproduction, QH471-489, Internal medicine, RC31-1245

Abstract

The oviductal epithelium consists of ciliated and non-ciliated cells, and their numbers vary depending on the segment of the oviduct and stage of the estrous cycle. Compared with the ampulla, fewer cyclic changes in the number of the two types of cells occur in the isthmus. Recently, we have reported that the epithelium in the ampullary oviduct is composed of many types of cells during different translational/transcriptional states, and their numbers change during the estrous cycle. However, detailed information regarding the epithelial cell subtypes lining the isthmic oviductal epithelium has not yet been reported. In this study, we aimed to identify the epithelial subtypes in the isthmus of the oviduct using immunohistochemistry. Some similarities and differences were observed between the ampulla and isthmus. As observed in the ampulla, epithelial cells of the isthmus expressed either FOXJ1 (ciliogenesis marker) or PAX8 (non-ciliated cell marker). The estrous cycle affected the number of Ki67+ cells but not that of ciliated cells. A relatively high rate of Ki67+ cells (60%) was observed at 1–4 days after the ovulation. Interestingly, unlike the ampulla, Ki67+/FOXJ1+ cells (12.6 ± 1.1%) were discovered in the isthmus. Double staining for Ki67 with FOXJ1, PAX8, or Centrin-1 (a centriole marker) revealed that Centrin-1 was localized on the apical surface of some Ki67+/FOXJ1+ cells. In conclusion, some epithelial cell subtypes exist in the isthmus of the oviduct and isthmus-specific cell subtypes have been identified. These region-specific cells may provide functional and morphological differences between the ampulla and isthmus of the oviduct.

Published

2022

15. Functional Alteration and Differential Expression of the Bitter Taste Receptor T2R38 in Human Paranasal Sinus in Patients with Chronic Rhinosinusitis.

Author

Takemoto, Kota, Lomude, Luga Santo, Takeno, Sachio, Kawasumi, Tomohiro, Okamoto, Yukako, Hamamoto, Takao, Ishino, Takashi, Ando, Yuki, Ishikawa, Chie, and Ueda, Tsutomu

Subjects

*NASAL mucosa, *TASTE receptors, *BITTERNESS (Taste), *GENE expression, *PARANASAL sinuses, *SINGLE nucleotide polymorphisms

Abstract

The bitter taste receptors (T2Rs) expressed in human sinonasal mucosae are known to elicit innate immune responses involving the release of nitric oxide (NO). We investigated the expression and distribution of two T2Rs, T2R14 and T2R38, in patients with chronic rhinosinusitis (CRS) and correlated the results with fractional exhaled NO (FeNO) levels and genotype of the T2R38 gene (TAS2R38). Using the Japanese Epidemiological Survey of Refractory Eosinophilic Chronic Rhinosinusitis (JESREC) phenotypic criteria, we identified CRS patients as either eosinophilic (ECRS, n = 36) or non-eosinophilic (non-ECRS, n = 56) patients and compared these groups with 51 non-CRS subjects. Mucosal specimens from the ethmoid sinus, nasal polyps, and inferior turbinate were collected from all subjects, together with blood samples, for RT-PCR analysis, immunostaining, and single nucleotide polymorphism (SNP) typing. We observed significant downregulation of T2R38 mRNA levels in the ethmoid mucosa of non-ECRS patients and in the nasal polyps of ECRS patients. No significant differences in T2R14 or T2R38 mRNA levels were found among the inferior turbinate mucosae of the three groups. Positive T2R38 immunoreactivity was localized mainly in epithelial ciliated cells, whereas secretary goblet cells generally showed lack of staining. The patients in the non-ECRS group showed significantly lower oral and nasal FeNO levels compared with the control group. There was a trend towards higher CRS prevalence in the PAV/AVI and AVI/AVI genotype groups as compared to the PAV/PAV group. Our findings reveal complex but important roles of T2R38 function in ciliated cells associated with specific CRS phenotypes, suggesting the T2R38 pathway as a potential therapeutic target for promotion of endogenous defense mechanisms. [ABSTRACT FROM AUTHOR]

Published

2023

16. Immunohistochemical identification of epithelial cell types in the isthmus of bovine oviduct: Comparison with the ampulla.

Author

Sayaka ITO, Yuna YAMAGUCHI, Sayaka KUBOTA, Yuki YAMAMOTO, and Koji KIMURA

Subjects

IMMUNOHISTOCHEMISTRY, SPERMATOZOA, EPITHELIUM, ESTRUS, OVIDUCT

Abstract

The oviductal epithelium consists of ciliated and non-ciliated cells, and their numbers vary depending on the segment of the oviduct and stage of the estrous cycle. Compared with the ampulla, fewer cyclic changes in the number of the two types of cells occur in the isthmus. Recently, we have reported that the epithelium in the ampullary oviduct is composed of many types of cells during different translational/transcriptional states, and their numbers change during the estrous cycle. However, detailed information regarding the epithelial cell subtypes lining the isthmic oviductal epithelium has not yet been reported. In this study, we aimed to identify the epithelial subtypes in the isthmus of the oviduct using immunohistochemistry. Some similarities and differences were observed between the ampulla and isthmus. As observed in the ampulla, epithelial cells of the isthmus expressed either FOXJ1 (ciliogenesis marker) or PAX8 (non-ciliated cell marker). The estrous cycle affected the number of Ki67+ cells but not that of ciliated cells. A relatively high rate of Ki67+ cells (60%) was observed at 1–4 days after the ovulation. Interestingly, unlike the ampulla, Ki67+/FOXJ1+ cells (12.6 ± 1.1%) were discovered in the isthmus. Double staining for Ki67 with FOXJ1, PAX8, or Centrin-1 (a centriole marker) revealed that Centrin-1 was localized on the apical surface of some Ki67+/FOXJ1+ cells. In conclusion, some epithelial cell subtypes exist in the isthmus of the oviduct and isthmus-specific cell subtypes have been identified. These region-specific cells may provide functional and morphological differences between the ampulla and isthmus of the oviduct. [ABSTRACT FROM AUTHOR]

Published

2023

17. Mutational Signatures as Sensors of Environmental Exposures: Analysis of Smoking-Induced Lung Tissue Remodeling.

Author

Kim, Yoo-Ah, Hodzic, Ermin, Amgalan, Bayarbaatar, Saslafsky, Ariella, Wojtowicz, Damian, and Przytycka, Teresa M.

Subjects

*LUNGS, *TISSUE remodeling, *ENVIRONMENTAL exposure, *LUNG diseases, *GENE expression, *DETECTORS

Abstract

Smoking is a widely recognized risk factor in the emergence of cancers and other lung diseases. Studies of non-cancer lung diseases typically investigate the role that smoking has in chronic changes in lungs that might predispose patients to the diseases, whereas most cancer studies focus on the mutagenic properties of smoking. Large-scale cancer analysis efforts have collected expression data from both tumor and control lung tissues, and studies have used control samples to estimate the impact of smoking on gene expression. However, such analyses may be confounded by tumor-related micro-environments as well as patient-specific exposure to smoking. Thus, in this paper, we explore the utilization of mutational signatures to study environment-induced changes of gene expression in control lung tissues from lung adenocarcinoma samples. We show that a joint computational analysis of mutational signatures derived from sequenced tumor samples, and the gene expression obtained from control samples, can shed light on the combined impact that smoking and tumor-related micro-environments have on gene expression and cell-type composition in non-neoplastic (control) lung tissue. The results obtained through such analysis are both supported by experimental studies, including studies utilizing single-cell technology, and also suggest additional novel insights. We argue that the study provides a proof of principle of the utility of mutational signatures to be used as sensors of environmental exposures not only in the context of the mutational landscape of cancer, but also as a reference for changes in non-cancer lung tissues. It also provides an example of how a database collected with the purpose of understanding cancer can provide valuable information for studies not directly related to the disease. [ABSTRACT FROM AUTHOR]

Published

2022

18. 猪链球菌在呼吸道上皮细胞中感染特性的研究.

Author

张浩 and 杨巍

Subjects

EPITHELIAL cells, SCANNING electron microscopy, CILIA & ciliary motion, RESPIRATORY organs, EPITHELIUM, BRONCHI

Abstract

Copyright of Chinese Journal of Preventive Veterinary Medicine / Zhongguo Yufang Shouyi Xuebao is the property of Chinese Journal of Preventive Veterinary Medicine Editorial Office and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2022

19. Morphological features of endometrial pinopodia formation during the luteal phase in women with previous unsuccessful implantation

Author

Y.G. Antypkin, O.O. Lytvak, O.G. Kuryk, G.P. Pasichnyk, and Y.M. Bondarenko

Subjects

infertility, pinopodia, endometrium, ciliated cells, secretory cells, Gynecology and obstetrics, RG1-991

Abstract

Pinopodia of the receptive endometrium is one of the prerequisites for successful embryo implantation. Study objective: to analyze the morphological changes of the endometrium in infertile women, in particular to investigate the apical surface of epithelial cells and pinopodia formation. Materials and methods. 12 patients with a history of previous implantation failure were examined. Patients underwent hysteroscopy with biopsy under intravenous anesthesia on 20–24th day of the menstrual cycle. Morphological structure of pinopodia on the surface of the endometrial epithelium was evaluated by scanning electron microscopy. Results. Apical surface of epitheliocytes was damaged in 16.7% studied biopsies. Morphological picture and maturity of the endometrial glands did not correspond to the actual day of the menstrual cycle in 41.7% biopsies. Degree of glands maturity in these patients was low, so there was a delay in the menstrual cycle. Ultrastructural examination showed clear changes in the structure of secretory and ciliary cells in 33.3%. On the apical surface of the secretory cells there was no or small number of microvilli; cilia of eyelashes were shortened or sometimes fused together. Pinopodia as a one of the most important components of implantation was detected in only 50% of patients. Only in 33.3% of participants visualized fully developed, mature pinopodia. Conclusions. Analysis of own data showed that in the endometrium of women with previous unsuccessful implantation there are certain morphological changes, which are physiologically manifested by a delay in the luteinizing phase of the menstrual cycle and, possibly, as a result mismatch of endometrial structure and embryo maturity. Time of pinopodia onset in participants varied from 20 to 24 days of the menstrual cycle. It is necessary to improve the design and conduct further research to study the association between the expression of receptivity markers and ultrastructural structure.

Published

2021

20. Spatial characterization of proteins in reproductive tissues : Insights into health and disease states

Author

Hikmet Noraddin, Feria and Hikmet Noraddin, Feria

Abstract

The molecular building blocks of human cells have been increasingly mapped in large-scale projects by emerging high-throughput antibody profiling and sequencing methods. These transformational efforts have shown remarkable progress in resolving the expression levels and spatial locations of proteins in many human cells. This thesis aimed to characterize the spatial protein expression at the single-cell level in human reproductive tissues, testis and fallopian tube (FT), and additionally study how aberrantly expressed testis-proteins repurposed in non-small cell lung cancer (NSCLC) affect the immune microenvironment. In Paper I, more than 500 proteins with elevated RNA expression levels in the testis were profiled in eight different cell types with immunohistochemistry (IHC). Several poorly characterized proteins, so-called “missing proteins,” were localized at the cell-type level at various stages of spermatogenesis, providing novel insights into their possible function. In Paper II, a spatiotemporal map of human spermatogenesis was created by combining single-cell transcriptomics and multiplex IHC. High-throughput image analysis determined the cell state-specific protein expression for almost 500 proteins. By examining RNA and protein correlation dynamics, we highlighted the complex spatiotemporal landscape of the human testis. These proteins serve as targets for functional studies. In Paper III, protein-coding genes elevated in FT based on RNA levels were profiled by IHC, and most proteins were functionally related to cilia motility, a mechanism necessary for creating the tubal flow essential for fertilization. Of 133 proteins annotated at the cell-type level, most were exclusive to ciliated cells, including several proteins previously not described in motile cilia. In Paper IV, cancer-testis antigens (CTA) were characterized by IHC on more than 300 immunophenotyped NSCLC patients. CTAs are typically expressed in the testis and harbor immunogenic properties that m

Published

2024

21. Goblet Cell Hyperplasia Increases SARS-CoV-2 Infection in Chronic Obstructive Pulmonary Disease

Author

Jaspreet Osan, Sattya N. Talukdar, Friederike Feldmann, Beth Ann DeMontigny, Kailey Jerome, Kristina L. Bailey, Heinz Feldmann, and Masfique Mehedi

Subjects

SARS-CoV-2, COVID-19, goblet cells, ciliated cells, COPD, airway epithelium, Microbiology, QR1-502

Abstract

ABSTRACT Chronic obstructive pulmonary disease (COPD) is one of the underlying conditions in adults of any age that place them at risk for developing severe illnesses associated with COVID-19. To determine whether SARS-CoV-2’s cellular tropism plays a critical role in severe pathophysiology in the lung, we investigated its host cell entry receptor distribution in the bronchial airway epithelium of healthy adults and high-risk adults (those with COPD). We found that SARS-CoV-2 preferentially infects goblet cells in the bronchial airway epithelium, as mostly goblet cells harbor the entry receptor angiotensin-converting enzyme 2 (ACE2) and its cofactor transmembrane serine protease 2 (TMPRSS2). We also found that SARS-CoV-2 replication was substantially increased in the COPD bronchial airway epithelium, likely due to COPD-associated goblet cell hyperplasia. Likewise, SARS-CoV and Middle East respiratory syndrome (MERS-CoV) infection increased disease pathophysiology (e.g., syncytium formation) in the COPD bronchial airway epithelium. Our results reveal that goblet cells play a critical role in SARS-CoV-2-induced pathophysiology in the lung. IMPORTANCE SARS-CoV-2 or COVID-19’s first case was discovered in December 2019 in Wuhan, China, and by March 2020 it was declared a pandemic by the WHO. It has been shown that various underlying conditions can increase the chance of having severe COVID-19. COPD, which is the third leading cause of death worldwide, is one of the conditions listed by the CDC which can increase the chance of severe COVID-19. The present study uses a healthy and COPD-derived bronchial airway epithelial model to study the COVID-19 and host factors which could explain the reason for COPD patients developing severe infection due to COVID-19.

Published

2022

22. Ciliated (FOXJ1 +) Cells Display Reduced Ferritin Light Chain in the Airways of Idiopathic Pulmonary Fibrosis Patients.

Author

Wijk, Sofia C., Prabhala, Pavan, Löfdahl, Anna, Nybom, Annika, Lang, Stefan, Brunnström, Hans, Bjermer, Leif, Westergren-Thorsson, Gunilla, and Magnusson, Mattias

Subjects

*IDIOPATHIC pulmonary fibrosis, *CILIA & ciliary motion, *FERRITIN, *CELL physiology, *PROTEIN microarrays, *RNA sequencing, *CELL populations

Abstract

Cell-based therapies hold great promise in re-establishing organ function for many diseases, including untreatable lung diseases such as idiopathic pulmonary fibrosis (IPF). However, many hurdles still remain, in part due to our lack of knowledge about the disease-driving mechanisms that may affect the cellular niche and thereby possibly hinder the function of any transplanted cells by imposing the disease phenotype onto the newly generated progeny. Recent findings have demonstrated increased ciliation of lung cells from IPF patients, but how this affects ciliated cell function and the airway milieu is not well-known. Here, we performed single-cell RNA sequencing on primary ciliated (FOXJ1+) cells isolated from IPF patients and from healthy control donors. The sequencing identified multiple biological processes, such as cilium morphogenesis and cell signaling, that were significantly changed between IPF and healthy ciliated cells. Ferritin light chain (FTL) was downregulated in IPF, which suggests that iron metabolism may be affected in the IPF ciliated cells. The RNA expression was confirmed at the protein level with histological localization in lung tissue, prompting future functional assays to reveal the potential role of FTL. Taken together, our data demonstrate the importance of careful analyses in pure cell populations to better understand the IPF disease mechanism. [ABSTRACT FROM AUTHOR]

Published

2022

23. Histo-morphological features of the efferent ductules of the African strawcoloured fruit bat (Eidolon helium).

Author

Abiaezute, C. N. and Uwagie-Ero, E. A.

Subjects

STRAW-colored fruit bat, POLLINATORS, ZOONOSES, EPIDIDYMIS, REPRODUCTION

Abstract

Introduction: The African straw-coloured fruit bat plays important roles as pollinators, seed dispersers and important carrier of zoonotic diseases. It is a non-hibernating seasonal breeder whose reproductive biology had received little attention. The aim was to study the histomorphology of the efferent ductules of Eidolon helvum using 10 adult male bats. Methods: The efferent ductules were obtained from the adult bats, fixed by immersion in neutral-buffered formalin and prepared for histology and histochemistry. Results: The result showed that the entire epididymis was enclosed by the thick dense regular connective tissue, tunica albuginea. Within the connective tissue, tubules of efferent ductules occurred in lobules. These lobules were separated from each other by connective tissue trabeculae. The efferent ductules are tiny tubules that connect the rete testis to the initial segments of the epididymis. Each efferent ductule was lined by a simple columnar epithelium of two cell types, containing the ciliated and the non-ciliated cells. The non-ciliated cells were more numerous exhibiting oval shapes, basally located euchromatic nuclei with prominent nucleoli. The ciliated cells were fewer and appeared as dark cells with oval to elongated, centrally or apically located heterochromatic nuclei. Cilia projected from the apical surfaces of the ciliated cells into the lumen. PAS/Alcian blue staining showed presence of PAS positive secretions in the apical cytoplasm of the non-ciliated cells. Significance: These findings indicate that the morphology of efferent ductules of the African straw-coloured fruit bat have similar morphology with most mammals but differ from those of insectivorous bats. [ABSTRACT FROM AUTHOR]

Published

2021

24. The embryonic epidermis of Xenopus tropialis: developing a model system for the study of mucociliary epithelia

Author

Dubaissi, Eamon and Papalopulu, Nancy

Subjects

571.53, Ciliated cells, Goblet cells, Ionocytes, Serous acinar cells, Foxi1e, v1a, ca12, mucociliary epithelia, Xenopus, epidermis

Abstract

Mucociliary epithelia are found in the human airways and act as the first line of defence against inhaled foreign agents. Mucus traps potentially damaging particles and the cilia transport the mucus away from the airways to remove the threat. Modelling mucociliary epithelia for research purposes is challenging. This is because the airways are enclosed and are thus difficult to study directly. Instead, tissue is extracted or in vitro techniques are employed. Whilst these systems are useful, there is a need for accessible in vivo models to complement them. In this thesis I assess a new model system for studying mucociliary epithelia. This system is the larval epidermis of the amphibian, Xenopus tropicalis. Its epidermis comprises multi-ciliated cells that beat in a polarised direction reminiscent of those found in the human airways. It is also proposed to have a number of other cell types including mucus-secreting cells, but very little is known about them. The epidermis is open and accessible to manipulation meaning that it has great potential to be used in the study of mucociliary epithelia in live, native conditions. Such a system would be a valuable addition to the current models employed. However, the epidermis has not been thoroughly characterized before so its utility as a model system remains speculative.To develop and evaluate this new model, I fully characterize the epidermis, showing that it has five distinguishable cell types. This includes a population of cells called ionocytes that are shown to be essential for the health and function of the epidermis. I also test for the presence of mucins, the structural component of mucus, secreted from the epidermis in order to evaluate the proposal that mucus-secreting cells are present in the epidermis. A mucin-like protein called otogelin is identified. After characterizing the epidermal cell types, I compare them to the human mucociliary epithelium and consider potential applications and future perspectives for this model.

Published

2011

25. Heterogeneous expression of the SARS-Coronavirus-2 receptor ACE2 in the human respiratory tract

Author

Miguel E. Ortiz, Andrew Thurman, Alejandro A. Pezzulo, Mariah R. Leidinger, Julia A. Klesney-Tait, Philip H. Karp, Ping Tan, Christine Wohlford-Lenane, Paul B. McCray, Jr., and David K. Meyerholz

Subjects

Lung, Expression, Alveolar type II cells, Ciliated cells, Immunohistochemistry, Medicine, Medicine (General), R5-920

Abstract

Background: Zoonotically transmitted coronaviruses are responsible for three disease outbreaks since 2002, including the current COVID-19 pandemic, caused by SARS-CoV-2. Its efficient transmission and range of disease severity raise questions regarding the contributions of virus-receptor interactions. ACE2 is a host ectopeptidase and the receptor for SARS-CoV-2. Numerous reports describe ACE2 mRNA abundance and tissue distribution; however, mRNA abundance is not always representative of protein levels. Currently, there is limited data evaluating ACE2 protein and its correlation with other SARS-CoV-2 susceptibility factors. Materials and methods: We systematically examined the human upper and lower respiratory tract using single-cell RNA sequencing and immunohistochemistry to determine receptor expression and evaluated its association with risk factors for severe COVID-19. Findings: Our results reveal that ACE2 protein is highest within regions of the sinonasal cavity and pulmonary alveoli, sites of presumptive viral transmission and severe disease development, respectively. In the lung parenchyma, ACE2 protein was found on the apical surface of a small subset of alveolar type II cells and colocalized with TMPRSS2, a cofactor for SARS-CoV2 entry. ACE2 protein was not increased by pulmonary risk factors for severe COVID-19. Additionally, ACE2 protein was not reduced in children, a demographic with a lower incidence of severe COVID-19. Interpretation: These results offer new insights into ACE2 protein localization in the human respiratory tract and its relationship with susceptibility factors to COVID-19.

Published

2020

26. Finely tuned ciliary alignment and coordinated beating generate continuous water flow across the external gills in Pleurodeles waltl larvae.

Author

Ichikawa, Reico and Toyoizumi, Ryuji

Subjects

*HYDRAULICS, *GILLS, *CELL motility, *AMPHIBIAN larvae, *LARVAE

Abstract

Urodelan amphibian larvae develop three pairs of branching external gills on both sides of the pharyngeal region, and this study focuses on motile cilia on the gill surface. High-speed camera was used to observe ciliary strokes on the surface of the external gills of Pleurodeles waltl larvae. We found that the directionality of ciliary beating is position-dependent on the gill surface, and this rule is applicable to all the samples examined. For visualizing water flow around the external gills, we used bead suspensions. We revealed continuous anterior-to-posterior water flow generated by coordinated ciliary beating. Around the frontal surface of the gill stem (gill rachis), water flows countercurrent to the bloodstream beneath the gill epidermis. These results suggest that ciliary beating in each ciliated cell is coordinated, which cooperatively generates continuous and directional ciliary flow. We next visualized the overall distribution of ciliated cells on the gill surface by immunostaining of acetylated alpha-tubulin. Our results showed that the fine branches of external gills (fimbriae) have a circumferential distribution of cilia aligned orthogonal to the longitudinal axes of fimbriae, which facilitates water flow from proximal to the distal part of the fimbriae through the gills. This ciliary distribution pattern and directionality of cilia-driven flow are shared among five urodelan and two anuran species. Taken together, our findings suggest that the distribution and motility of ciliated cells on the surface of external gills is finely controlled, and this might support efficient respiration by the gills in urodeles. [ABSTRACT FROM AUTHOR]

Published

2020

27. Single-cell analysis reveals insights into epithelial abnormalities in ovarian endometriosis.

Author

Yan, Jia, Zhou, Ling, Liu, Mengya, Zhu, Honglan, Zhang, Xin, Cai, E., Xu, Xueqiang, Chen, Tinghan, Cheng, Hongyan, Liu, Jun'e, Wang, Shang, Dai, Lin, Chang, Xiaohong, and Tang, Fuchou

Abstract

Ovarian endometriosis is characterized by the growth of endometrial tissue within the ovary, causing infertility and chronic pain. However, its pathophysiology remains unclear. Utilizing high-precision single-cell RNA sequencing, we profile the normal, eutopic, and ectopic endometrium from 34 individuals across proliferative and secretory phases. We observe an increased proportion of ciliated cells in both eutopic and ectopic endometrium, characterized by a diminished expression of estrogen sulfotransferase, which likely confers apoptosis resistance. After translocating to ectopic lesions, endometrial epithelium upregulates nicotinamide N-methyltransferase expression that inhibits apoptosis by promoting deacetylation and subsequent nuclear exclusion of transcription factor forkhead box protein O1, thereby leading to the downregulation of the apoptotic gene BIM. Moreover, epithelial cells in ectopic lesions elevate HLA class II complex expression, which stimulates CD4+ T cells and consequently contributes to chronic inflammation. Altogether, our study provides a comprehensive atlas of ovarian endometriosis and highlights potential therapeutic targets for modulating apoptosis and inflammation. [Display omitted] • Eutopic and ectopic endometrium upregulate the percentage of ciliated cells • The ciliated cells in patients exhibit decreased SULT1E1 expression • Epithelial cells in endometriotic lesions resist apoptosis through NNMT-FOXO1-BIM pathway • Epithelial cells in endometriotic lesions stimulate CD4+ T cells via HLA class II complex Yan et al. generated a single-cell endometriosis atlas and revealed that ciliated cells in eutopic and ectopic endometrium suppress apoptosis through reduced estrogen sulfotransferase expression. In ectopic lesions, epithelial cells further adapted to survive by resisting apoptosis via NNMT and driving chronic inflammation through the HLA class II complex. [ABSTRACT FROM AUTHOR]

Published

2024

28. Rhinovirus C targets ciliated airway epithelial cells

Author

Theodor F. Griggs, Yury A. Bochkov, Sarmila Basnet, Thomas R. Pasic, Rebecca A. Brockman-Schneider, Ann C. Palmenberg, and James E. Gern

Subjects

Rhinovirus C, Air-liquid interface, Ciliated cells, CDHR3, Bronchial epithelium, Diseases of the respiratory system, RC705-779

Abstract

Abstract Background The Rhinovirus C (RV-C), first identified in 2006, produce high symptom burdens in children and asthmatics, however, their primary target host cell in the airways remains unknown. Our primary hypotheses were that RV-C target ciliated airway epithelial cells (AECs), and that cell specificity is determined by restricted and high expression of the only known RV-C cell-entry factor, cadherin related family member 3 (CDHR3). Methods RV-C15 (C15) infection in differentiated human bronchial epithelial cell (HBEC) cultures was assessed using immunofluorescent and time-lapse epifluorescent imaging. Morphology of C15-infected differentiated AECs was assessed by immunohistochemistry. Results C15 produced a scattered pattern of infection, and infected cells were shed from the epithelium. The percentage of cells infected with C15 varied from 1.4 to 14.7% depending on cell culture conditions. Infected cells had increased staining for markers of ciliated cells (acetylated-alpha-tubulin [aat], p

Published

2017

29. Transient integumentary structures in Boana riojana (Anura, Hylidae) tadpoles.

Author

Quinzio, Silvia Inés and Goldberg, Javier

Subjects

*HYLIDAE, *TADPOLES, *ANURA

Abstract

Few studies focusing on embryos and/or tadpole skin morphology have described sensory transient organs whose morphological variation could indicate some taxonomical or functional correlations. We explore here some integumentary features of Boana riojana larvae that are rarely mentioned in tadpole descriptions. We provide histomorphological and SEM descriptions of the lateral line system, a series of evenly distributed unpigmented spots, and some symmetrical paired structures dorsal to the oral disc. The latter are previously unreported in any tadpole. Our descriptions reveal that the: 1) the number of lateral lines resembles those for most tadpoles, but with an unusual arrangement of stitches; 2) paired lateral spots are formed by ciliated cells dispersed in clusters unrelated to the lateral line system; and 3) upper-lip related structures are histomorphologically similar to the unpigmented spots. We discuss and suggest that integumentary transient structures in B. riojana represent traits that should be taken into account when describing tadpoles. This new information may help diagnose species and advance our understanding of tadpole ecomorphology and evolution. [ABSTRACT FROM AUTHOR]

Published

2019

30. Ultrastructural and histological characteristics of the endometrium during early embryo development in mares.

Author

Camozzato, G.C., Martinez, M.N., Bastos, H.B.A., Fiala-Rechsteiner, S., Meikle, A., Jobim, M.I.M., Gregory, R.M., and Mattos, R.C.

Subjects

*MARES, *ULTRASTRUCTURE (Biology), *HISTOLOGY, *ENDOMETRIUM, *EMBRYOLOGY, *OVULATION

Abstract

Abstract The aim of this study was to evaluate ultrastructural and histological changes in the endometrium on days 7, 10 and 13 post-ovulation in pregnant and cyclic mares. Mares were routinely examined by transrectal palpation and ultrasonographic examination of the reproductive tract until estrus was detected. In the first cycle, endometrial biopsies from 30 cyclic mares (Cyclic group) were collected on days 7, 10 and 13 post-ovulation. In the second cycle, the same mares were bred by a fertile stallion. At days 7, 10 and 13 post-ovulation intrauterine biopsies were collected. Immediately after sample collection, the mare's uteri were flushed, and those mares with embryo recovery were assigned to the Pregnant group. From ovulation detection until day of uterine biopsy, blood samples to measure Progesterone concentrations were collected daily in cyclic and pregnant mares. A larger blood vessel caliber was observed in pregnant mares than in cyclic from day 7–13. On the 7th day of pregnancy a large loss of ciliated cells was evident in the group of pregnant mares in comparison with the Cyclic group and the superficial cells of the endometrium were more protruded, and a small amount of histotrophic material between the folds was observed. On the 10th day of pregnancy, the glandular histotrophic secretion and the secretion of luminal epithelium became more intense than the secretion of cyclic mares. On the 13th day of pregnancy, a very large amount of histotroph was observed within large glandular openings surrounded by ciliated cells. The concentrations of P4 were affected by day (P < 0.001), but were not affected by group. Changes occurred in the uterine environment thereupon the entry of the embryo into the uterus. In the stroma and in the lumen, these modifications may aid to provide the necessary nutrition for the initial development of the embryo and to promote changes at cellular structures that will interact in the embryonic signaling and future fixation, implantation and placentation. Highlights • A larger blood vessel caliber occurs in pregnant mares than in cyclic since day 7. • A large loss of ciliated cells occurs in pregnant mares than cyclic on day 7. • On the 13th day of pregnancy, a very large amount of histotroph was observed. • Changes occurred in the endometrium thereupon the entry of the embryo into the uterus. [ABSTRACT FROM AUTHOR]

Published

2019

31. Evidence against the mucosal traction theory in cholesteatoma.

Author

Schachern, Patricia, Chole, Richard A., Cureoglu, Sebahattin, Pauna, Henrique F., Monsanto, Rafael C., and Paparella, Michael M.

Abstract

Objectives: To investigate the distribution of ciliated epithelium in the human middle ear and its potential role in the formation of cholesteatoma.Study Design: Comparative human temporal bone study.Methods: We selected temporal bones from 14 donors with a diagnosis of cholesteatoma, 15 with chronic otitis media without retraction pockets, 14 with chronic otitis media with retraction pockets, 14 with cystic fibrosis (CF), and 16 controls. We mapped the distribution of the ciliated cells in the mucosal lining of the middle ear and tympanic membrane using three-dimensional reconstruction analysis, and counted the number of ciliated cells in the middle ear mucosa.Results: Ciliated cells are extremely sparse in the epithelial lining of the lateral surface of the ossicles in the epitympanum and the medial surface of the tympanic membrane. Furthermore, there is a significant decrease in the number of ciliated cells in these areas in temporal bones with cholesteatoma, chronic otitis media, chronic otitis media with retraction pockets, and CF compared to controls. Ciliated cells most commonly are located at the hypotympanum and the Eustachian tube opening but not the tympanic membrane or epitympanum.Conclusion: The paucity of ciliated epithelial cells on the medial side of the tympanic membrane and the lateral surface of the ossicles in the epitympanum in cases with cholesteatoma and/or chronic otitis media do not support the mucosal migration theory of cholesteatoma formation.Level Of Evidence: NA. Laryngoscope, 128:1663-1667, 2018. [ABSTRACT FROM AUTHOR]

Published

2018

32. Variable localization of Toll-like receptors in human fallopian tube epithelial cells.

Author

Amjadi, Fatemehsadat, Zandieh, Zahra, Salehi, Ensieh, Jafari, Reza, Ghasemi, Nasrin, Aflatoonian, Abbas, Fazeli, Alireza, and Aflatoonian, Reza

Subjects

*FALLOPIAN tubes, *EPITHELIAL cells, *TOLL-like receptors, *POLYMERASE chain reaction

Abstract

Objective: To determine the localization, expression, and function of Toll-like receptors (TLRs) in fallopian tube epithelial cells. Methods: The localization of TLRs in fallopian tube epithelial cells was investigated by immunostaining. Surprisingly, the intensity of staining was not equal in the secretory and ciliated cells. After primary cell culture of fallopian tube epithelial cells, ring cloning was used to isolate colonies of ciliated epithelial cells, distinct from non-ciliated epithelial cells. The expression of TLRs 1-10 was examined by quantitative real-time polymerase chain reaction, and protein localization was confirmed by immunostaining. The function of the TLRs was determined by interleukin (IL)-6 and IL-8 production in response to TLR2, TLR3, TLR5, TLR7, and TLR9 ligands. Results: Fallopian tube epithelial cells expressed TLRs 1-10 in a cell-type-specific manner. Exposing fallopian tube epithelial cells to TLR2, TLR3, TLR5, TLR7, and TLR9 agonists induced the secretion of proinflammatory cytokines such as IL-6 and IL-8. Conclusion: Our findings suggest that TLR expression in the fallopian tubes is cell-type-specific. According to our results, ciliated cells may play more effective role than non-ciliated cells in the innate immune defense of the fallopian tubes, and in interactions with gametes and embryos. [ABSTRACT FROM AUTHOR]

Published

2018

33. Ciliated Cells in Ovarian Cancer Decrease with Increasing Tumor Grade and Disease Progression.

Author

Richardson, Michael, Richardson, Michael, Recouvreux, Maria, Walts, Ann, Orsulic, Sandra, Karlan, Beth, Richardson, Michael, Richardson, Michael, Recouvreux, Maria, Walts, Ann, Orsulic, Sandra, and Karlan, Beth

Abstract

Ciliated cell markers expressed in epithelial ovarian cancers (EOC) are associated with improved survival. We examined the distribution of cells expressing ciliated cell markers in various EOC histologies and stages. Immunohistochemistry and/or multiplex immunofluorescence were used to determine the expression of FOXJ1 and/or CAPS (ciliated cell markers) in tissue microarrays including 4 normal fallopian tubes, 6 normal endometria, 16 cystadenomas, 25 borderline tumors, 21 low-grade carcinomas, and 118 high-grade carcinomas (HGSOC) (46 serous, 29 endometrioid, 30 clear cell, 13 mucinous). CAPS+ cells were observed in normal fallopian tubes and endometria and in ~85% of serous benign and borderline tumors and low-grade carcinomas but only in <40% of HGSOC. mRNA data from an independent cohort showed higher FOXJ1 and CAPS expression in serous borderline tumors and low-grade carcinomas compared to HGSOC. In HGSOC, ciliated cell-positive markers were observed in 52% primary tumors compared to 26% of patient-matched synchronous metastases, and 24% metachronous metastases (p = 0.009). mRNA data from an independent HGSOC cohort showed lower levels of CAPS in metastases than in primary tumors (p = 0.03). Overall, the study revealed that ciliated cells were less common in mucinous EOC, the percentage of ciliated cell marker-positive cases decreased with increasing grade, and the percentage of ciliated cells decreased in HGSOC metastases compared to patient-matched primary tumors.

Published

2022

34. Origin of clear cell carcinoma: nature or nurture?

Author

Kolin, David L., Dinulescu, Daniela M., and Crum, Christopher P.

Abstract

Abstract: A rare but serious complication of endometriosis is the development of carcinoma, and clear cell and endometrioid carcinomas of the ovary are the two most common malignancies which arise from endometriosis. They are distinct diseases, characterized by unique morphologies, immunohistochemical profiles, and responses to treatment. However, both arise in endometriosis and can share common mutations. The overlapping mutational profiles of clear cell and endometrioid carcinomas suggest that their varied histologies may be due to a different cell of origin which gives rise to each type of cancer. Cochrane and colleagues address this question in a recent article in this journal. They show that a marker of ovarian clear cell carcinoma, cystathionine gamma lyase, is expressed in ciliated cells. Similarly, they show that markers of secretory cells (estrogen receptor and methylenetetrahydrofolate dehydrogenase 1) are expressed in ovarian endometrioid carcinoma. Taken together, they suggest that endometrioid and clear cell carcinomas arise from cells related to secretory and ciliated cells, respectively. We discuss Cochrane et al's work in the context of other efforts to determine the cell of origin of gynecological malignancies, with an emphasis on recent developments and challenges unique to the area. These limitations complicate our interpretation of tumor differentiation; does it reflect nature imposed by a specific cell of origin or nurture, by either mutation(s) or environment? Copyright © 2017 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2018

35. Scanning ion conductance microscopy for visualizing the three-dimensional surface topography of cells and tissues.

Author

Nakajima, Masato, Mizutani, Yusuke, Iwata, Futoshi, and Ushiki, Tatsuo

Subjects

*MICROSCOPY, *THREE-dimensional imaging in biology, *CELL analysis, *TISSUE analysis, *SURFACE topography, *ULTRASTRUCTURE (Biology), *KIDNEY glomerulus

Abstract

Scanning ion conductance microscopy (SICM), which belongs to the family of scanning probe microscopy, regulates the tip-sample distance by monitoring the ion current through the use of an electrolyte-filled nanopipette as the probing tip. Thus, SICM enables “contact-free” imaging of cell surface topography in liquid conditions. In this paper, we applied hopping mode SICM for obtaining topographical images of convoluted tissue samples such as trachea and kidney in phosphate buffered saline. Some of the SICM images were compared with the images obtained by scanning electron microscopy (SEM) after drying the same samples. We showed that the imaging quality of hopping mode SICM was excellent enough for investigating the three-dimensional surface structure of the soft tissue samples. Thus, SICM is expected to be used for imaging a wide variety of cells and tissues − either fixed or alive- at high resolution under physiologically relevant liquid conditions. [ABSTRACT FROM AUTHOR]

Published

2018

36. Modulation of Wnt signaling is essential for the differentiation of ciliated epithelial cells in human airways.

Author

Schmid, Andreas, Sailland, Juliette, Novak, Lisa, Baumlin, Nathalie, Fregien, Nevis, and Salathe, Matthias

Subjects

*EXFOLIATIVE cytology, *CYTOPROTECTION, *CELL differentiation, *CELL proliferation, *EPITHELIAL cells

Abstract

Wnt signaling is essential for the differentiation of airway epithelial cells during development. Here, we examined the role of Wnt signaling during redifferentiation of ciliated airway epithelial cells in vitro at the air liquid interface as a model of airway epithelial repair. Phases of proliferation and differentiation were defined. Markers of squamous metaplasia and epithelial ciliation were followed while enhancing β-catenin signaling by blocking glycogen synthase kinase 3β with SB216763 and shRNA as well as inhibiting canonical WNT signaling with apical application of Dickkopf 1 (Dkk1). Our findings indicate that enhanced β-catenin signaling decreases the number of ciliated cells and causes squamous changes in the epithelium, whereas treatment with DDk1 leads to an increased number of ciliated cells. [ABSTRACT FROM AUTHOR]

Published

2017

37. Clear cell and endometrioid carcinomas: are their differences attributable to distinct cells of origin?

Author

Cochrane, Dawn R, Tessier‐Cloutier, Basile, Lawrence, Katherine M, Nazeran, Tayyebeh, Karnezis, Anthony N, Salamanca, Clara, Cheng, Angela S, McAlpine, Jessica N, Hoang, Lien N, Gilks, C Blake, and Huntsman, David G

Abstract

Endometrial epithelium is the presumed tissue of origin for both eutopic and endometriosis-derived clear cell and endometrioid carcinomas. We had previously hypothesized that the morphological, biological and clinical differences between these carcinomas are due to histotype-specific mutations. Although some mutations and genomic landscape features are more likely to be found in one of these histotypes, we were not able to identify a single class of mutations that was exclusively present in one histotype and not the other. This lack of genomic differences led us to an alternative hypothesis that these cancers could arise from distinct cells of origin within endometrial tissue, and that it is the cellular context that accounts for their differences. In a proteomic screen, we identified cystathionine γ-lyase (CTH) as a marker for clear cell carcinoma, as it is expressed at high levels in clear cell carcinomas of the ovary and endometrium. In the current study, we analysed normal Müllerian tissues, and found that CTH is expressed in ciliated cells of endometrium (both eutopic endometrium and endometriosis) and fallopian tubes. We then demonstrated that other ciliated cell markers are expressed in clear cell carcinomas, whereas endometrial secretory cell markers are expressed in endometrioid carcinomas. The same differential staining of secretory and ciliated cells was demonstrable in a three-dimensional organoid culture system, in which stem cells were stimulated to differentiate into an admixture of secretory and ciliated cells. These data suggest that endometrioid carcinomas are derived from cells of the secretory cell lineage, whereas clear cell carcinomas are derived from, or have similarities to, cells of the ciliated cell lineage. Copyright © 2017 Pathological Society of Great Britain and Ireland. Published by John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2017

38. Rhinovirus C targets ciliated airway epithelial cells.

Author

Griggs, Theodor F., Bochkov, Yury A., Basnet, Sarmila, Pasic, Thomas R., Brockman-Schneider, Rebecca A., Palmenberg, Ann C., and Gern, James E.

Subjects

ASTHMATICS, AIRWAY (Anatomy), IMMUNOFLUORESCENCE, CELL culture, EXFOLIATIVE cytology

Abstract

Background: The Rhinovirus C (RV-C), first identified in 2006, produce high symptom burdens in children and asthmatics, however, their primary target host cell in the airways remains unknown. Our primary hypotheses were that RV-C target ciliated airway epithelial cells (AECs), and that cell specificity is determined by restricted and high expression of the only known RV-C cell-entry factor, cadherin related family member 3 (CDHR3).Methods: RV-C15 (C15) infection in differentiated human bronchial epithelial cell (HBEC) cultures was assessed using immunofluorescent and time-lapse epifluorescent imaging. Morphology of C15-infected differentiated AECs was assessed by immunohistochemistry.Results: C15 produced a scattered pattern of infection, and infected cells were shed from the epithelium. The percentage of cells infected with C15 varied from 1.4 to 14.7% depending on cell culture conditions. Infected cells had increased staining for markers of ciliated cells (acetylated-alpha-tubulin [aat], p < 0.001) but not markers of goblet cells (wheat germ agglutinin or Muc5AC, p = ns). CDHR3 expression was increased on ciliated epithelial cells, but not other epithelial cells (p < 0.01). C15 infection caused a 27.4% reduction of ciliated cells expressing CDHR3 (p < 0.01). During differentiation of AECs, CDHR3 expression progressively increased and correlated with both RV-C binding and replication.Conclusions: The RV-C only replicate in ciliated AECs in vitro, leading to infected cell shedding. CDHR3 expression positively correlates with RV-C binding and replication, and is largely confined to ciliated AECs. Our data imply that factors regulating differentiation and CDHR3 production may be important determinants of RV-C illness severity. [ABSTRACT FROM AUTHOR]

Published

2017

39. Endothelial Cell Mediated Promotion of Ciliated Cell Differentiation of Human Airway Basal Cells via Insulin and Insulin-Like Growth Factor 1 Receptor Mediated Signaling.

Author

Gomi, Kazunori, Tang, Yongjiang, Arbelaez, Vanessa, Crystal, Ronald, and Walters, Matthew

Subjects

*PROGENITOR cells, *ENDOTHELIAL cells, *CELL differentiation, *SOMATOMEDIN C, *INSULIN, *AIRWAY (Anatomy)

Abstract

Human airway basal cells (BC) function as stem/progenitor cells of the human airway epithelium, capable of differentiating into ciliated and secretory cells during turnover and repair. The positioning of BC along the basement membrane allows for potential paracrine signaling from non-epithelial cells in the mesenchyme to regulate BC function. Based on the knowledge that interaction between the airway epithelium and mesenchyme is critical for proper maintenance of both tissues, and that endothelial cells (EC) can regulate multiple functions of BC, the present study was designed to help understand the role of BC and EC cross-talk in regulating BC stem/progenitor function. Using an in vitro co-culture system that mimics the in vivo physical separation of these cell types, we assessed the impact of primary lung microvascular EC on differentiation of primary BC into a mucociliated epithelium. The data demonstrate that co-culture of BC and lung microvasculature EC results in increased ciliated cell differentiation of BC via activation of insulin (INS) and insulin-like growth factor 1 (IGF1) receptor (INSR and IGF1R) mediated signaling in BC. Consistent with this data, siRNA mediated knockdown of INSR and IGF1R in BC suppressed ciliated cell differentiation. Together these findings identify an important signaling pathway required for differentiation of BC into a ciliated cells and demonstrate the importance of BC-EC cross-talk in regulating normal airway epithelial structure. [ABSTRACT FROM AUTHOR]

Published

2017

40. «Implantation window» disturbance in patients with hyperplastic processes of endometrium

Author

O. I. Parnytska

Subjects

endometrium, endometrial hyperplasia, scanning electrone microscopy, ciliated cells, «implantation window», Pathology, RB1-214

Abstract

Introduction There is an increasing interest in the role of hyperplastic processes of endometrium in the “implantation window” disturbance and unsuccessful implantation rate. The endometrium represents a barrier to implantation except under appropriate and defined hormonal conditions. There is no doubt that endometrium has an important role for embryo implantation at early stages of development. Successful implantation requires a functionally normal embryo at the blastocyst stage and receptive endometrium, while the communication between them is also vital. Endometrium shows dynamic and cyclic morphological changes throughout the follicular phase and in the secretory phase. The progesterone-driven differentiative changes in the endometrial epithelium lead to the ‘opening’ of the “window of receptivity” for blastocyst implantation. Morphologically, progesterone-dependent apical cellular protrusions known as pinopods (uterodomes) become visible by scanning electron microscopy on 20th–21st days of human menstrual cycle and then are lost. Materials and methods A total of 180 endometrial specimens from women with simple hyperplasia (I gr.), endometrial polyps (II gr.) and asynchronous endometrium (III gr.) have been examined by scanning electron microscopy. Biopsies were obtained from fundus of the uterus and processed for light and scanning electron microscopy. Tissues for light microscopy were fixed in 1,25% glutardialdehyde, embedded in paraffin, sectioned and stained with hematoxylin and eosin. Results In I group with simple hyperplasia the ratio of glands and stroma is now increased. Most or all of the endometrial glands are more or less cystically dilated and lined by pseudostratified, highly proliferating epithelium with enlarged, elongated, nuclei in scanty, basophilic cytoplasm. Mitoses are frequent in the epithelium. II group shows endometrial polyps with proliferation of stromal cells incorporating a non-neoplastic glandular component. They were pedunculated with a central fibrovascular core which, when visible in the plane of the section, will be a characteristic diagnostic sign.The hyperplastic polyps contained areas of simple hyperplasia without atypia. In the III group morphology of the deficient secretory phase with coordinated true delay was evaluated and there were no significant changes in ciliated cells quality and quantity. We revealed only “implantation window” disturbance as delay in pinopodes formation or absence of uterodomes. Present study revealed isolated pathological changes of ciliated cells and its conjunction with abnormalities in pinopodes formation (“implantation window”) in women with simple hyperplasia (I group) and polyps (II group) in compare to endometrium of III group. Discussion We observed that significant increasing of ciliated cells quantity, cilliar hyperplasia and irregular distribution in women with simple hyperplasia of endometrium can cause breaking of embryo implantation (apposition and attachment) even in case of regular pinopodes formation. endometrium, endometrial hyperplasia, scanning electrone microscopy, ciliated cells, «implantation window»

Published

2013

41. Single-Cell RNA-Seq Analysis Reveals Lung Epithelial Cell Type-Specific Responses to HDM and Regulation by Tet1

Author

Tao Zhu, Anthony P. Brown, Lucy P. Cai, Gerald Quon, and Hong Ji

Subjects

ciliated cells, Knockout, allergic lung inflammation, Mice, Proto-Oncogene Proteins, Genetics, Animals, 2.1 Biological and endogenous factors, Aetiology, Lung, Genetics (clinical), alveolar type 2 (AT2) cells, Mice, Knockout, single-cell RNA-seq, Sequence Analysis, RNA, Pyroglyphidae, Epithelial Cells, Pneumonia, respiratory system, Epithelial Cell Adhesion Molecule, Asthma, Tet1, respiratory tract diseases, DNA-Binding Proteins, Health Effects of Indoor Air Pollution, Respiratory, RNA, Single-Cell Analysis, Sequence Analysis

Abstract

Tet1 protects against house dust mite (HDM)-induced lung inflammation in mice and alters the lung methylome and transcriptome. In order to explore the role of Tet1 in individual lung epithelial cell types in HDM-induced inflammation, we established a model of HDM-induced lung inflammation in Tet1 knockout and littermate wild-type mice, then studied EpCAM+ lung epithelial cells using single-cell RNA-seq analysis. We identified eight EpCAM+ lung epithelial cell types, among which AT2 cells were the most abundant. HDM challenge altered the relative abundance of epithelial cell types and resulted in cell type-specific transcriptomic changes. Bulk and cell type-specific analysis also showed that loss of Tet1 led to the altered expression of genes linked to augmented HDM-induced lung inflammation, including alarms, detoxification enzymes, oxidative stress response genes, and tissue repair genes. The transcriptomic regulation was accompanied by alterations in TF activities. Trajectory analysis supports that HDM may enhance the differentiation of AP and BAS cells into AT2 cells, independent of Tet1. Collectively, our data showed that lung epithelial cells had common and unique transcriptomic signatures of allergic lung inflammation. Tet1 deletion altered transcriptomic networks in various lung epithelial cells, which may promote allergen-induced lung inflammation.

Published

2022

42. Changes in Morphology and Presence of Pinopodes in Endometrial Cells during the Luteal Phase in Women with Infertility Problems: A Pilot Study

Author

Marina Aunapuu, Piret Kibur, Tõnu Järveots, and Andres Arend

Subjects

endometrium, ciliated cells, secretory cells, pinopodes, infertility, Medicine (General), R5-920

Abstract

Objective: To investigate morphological changes in the endometrial epithelial cells of patients with infertility problems. Materials and methods: Endometrial biopsies were obtained from 10 women who have undergone several unsuccessful in vitro fertilisation (IVF) procedures. Endometrial biopsies were performed between luteinizing hormone surge days LH+6 to +10 of the natural menstrual cycle. Each sample was divided into three parts, which were processed for histological, transmission (TEM), and scanning electron microscopy (SEM) investigations. Results: Histological investigations demonstrated significant alterations in the apical part of epithelial cells of one patient; in four patients, the gland maturity was low, not matching the cycle day, and thus a phase lag had developed. By TEM examination, we ascertained changes in secretory and ciliated cells in three patients (decreased amount or missing microvilli, irregular cilia in ciliated cells). SEM examination found pinopodes in five patients: three samples contained fully developed pinopodes—larger and completely smooth, with only some wrinkles; one sample contained regressing small pinopodes, with wrinkled surfaces; and one sample had both developed and regressing pinopodes. Conclusions: To conclude, our study shows that the endometrium of patients with poor IVF outcome has either significant changes in the morphology or the endometrial maturation is inhibited and a phase lag often develops. Our study shows that endometrial pinopodes are found throughout the mid-luteal phase up to day LH+10.

Published

2018

43. Cytofunctional changes in nasal ciliated cells in patients treated with hyaluronate after nasal surgery.

Author

Cassano, Michele, Russo, Giuseppe Maria, Granieri, Carla, and Cassano, Pasquale

Subjects

NASAL surgery, THERAPEUTIC use of hyaluronic acid, NASAL mucosa, MUCOCILIARY system, RANDOMIZED controlled trials, WOUNDS & injuries

Abstract

Background: Hyaluronic acid (HA) plays a significant role in tissue repair of mucosal surfaces and, consequently, in surgical injury remodelling of nasal mucosa. Objective: To assess the effect of high-molecular-weight HA administered by aerosol on the morphofunctional recovery of ciliated cells damaged by surgical trauma. Methods: A single-blind, prospective, randomized trial was carried out with 94 patients who were randomly assigned, after endoscopic turbinoplasty, either to treatment with nasal saline solution irrigation (control group, n = 47) or to treatment with nasal douches based on high concentration (9 mg) and high-molecular-weight sodium hyaluronate (active treatment group, n = 47). All the patients were evaluated by using nasal fiberendoscopy, mucociliary transport time, nasal cytologic test, and a visual analog scale in terms of symptoms before and at 2 and 4 weeks after surgery. Results: Visual analog scale values were significantly lower in the active treatment (AT) group at week 2 regarding each individual symptom. Mucociliary transport time was significantly reduced in patients in the AT group but only 1 month after surgery. Both the percentage of cellular impairments and the number of cells with hyperchromatic supranuclear stria showed significant improvements in the AT group in all postsurgery evaluations (p < 0.05). Conclusion: Intranasal use of sodium hyaluronate in patients who underwent functional nasal surgery improved both mucociliary clearance and nasal mucosa regeneration due to a faster recovery of the impaired ciliated cells. [ABSTRACT FROM AUTHOR]

Published

2016

44. Elimination of IL-13 Reverses Established Goblet Cell Metaplasia into Ciliated Epithelia in Airway Epithelial Cell Culture

Author

Mitsuko Kondo, Jun Tamaoki, Kiyoshi Takeyama, Kazuo Isono, Kiyomi Kawatani, Takehiro Izumo, and Atsushi Nagai

Subjects

anti-IL-13 antibody, ciliated cells, goblet cells, IL-13, transition, Immunologic diseases. Allergy, RC581-607

Abstract

Background: Interleukin (IL)-13 induces goblet cell metaplasia and plays an important role in mucus hypersecretion in asthma. We previously reported that IL-13 induced goblet cell differentiation along with less ciliated cell differentiation in guinea pig tracheal epithelial cells in vitro. In this study, we asked whether elimination of IL-13 could reverse the established goblet cell metaplasia into ciliated epithelia. Methods: Primary epithelial cells from guinea pig tracheas were cultured at an air-liquid interface with the medium containing human recombinant IL-13 for 14 days, and continuously cultured with IL-13-eliminated medium, or cultured under the condition of neutralization of IL-13 with anti IL-13 antibody. Results: 2 days after elimination of IL-13, the periodic acid-Schiff-positive area as well as MUC5AC protein level rapidly decreased. After 4 days, the number of goblet cells dramatically decreased, while that of ciliated cells inversely increased. The total number of epithelial cells did not change, and 5-bromo-2’-deoxyuridine uptake decreased after IL-13 elimination. Transitional cells with cilia and secretory granules increased after IL-13 elimination. Similarly, the neutralization of IL-13 with anti-IL-13 antibody for 5 days reversed the goblet cell metaplasia into ciliated epithelia, and transitional cells also increased. Conclusions: Elimination of IL-13 reverses goblet cell metaplasia into ciliated epithelia in vitro, and transition of goblet cells to other phenotypes, especially ciliated cells, may be involved in this phenomenon. IL-13 inhibition may be a therapeutic strategy of established goblet cell metaplasia in asthma.

Published

2006

45. Normobaric hypoxia induces mild damage to epithelium of terminal bronchioles in rabbits (ultrastructural study)

Author

J. Uhlik, V. Konradova, L. Vajner, and J. Adaskova

Subjects

airways, clara cells, ciliated cells, electron microscopy, Veterinary medicine, SF600-1100

Abstract

We studied the ultrastructure of the epithelium of terminal bronchioles in rabbits exposed for 96 hours to hypoxia (10% O2) in isobaric hypoxic chamber. Rabbits of the first control group (treated controls) were exposed for the same time in the same hypoxic chamber with atmosphere regulated at 21% O2. In both groups, the temperature in the chamber was 23°C and humidity 100% during the whole experiment. The second control group (untreated controls) was kept under standard conditions. The target cells for the effect of high temperature, humidity and normobaric hypoxia were the secretory elements. Both in hypoxic animals and treated controls, isolated Clara cells revealed signs of pathological alteration. More degenerative changes of Clara cells and marks of their compensatory proliferation were ascertained after exposure to hypoxia. Electron dense secretory granules were observed in most Clara cells. This finding reflected the initial stage of their secretory product formation. The secretory granules were usually stored in cytoplasm; morphological signs of their evacuation were found only exceptionally. The ciliated cells were less damaged than the secretory ones. On their apical surfaces, formation of cytoplasmic protrusions, which sometimes led to degeneration of free cilia, was ascertained. The damage of the epithelium and mild secretory stimulation of its secretory elements could play a role in the lung injury caused by the subacute normobaric hypoxia.

Published

2005

46. The NOTCH3 Downstream Target HEYL Is Required for Efficient Human Airway Basal Cell Differentiation

Author

Andrew R. Moore, Willard M. Freeman, Jonathan D. Wren, Manish Bodas, Sarah R. Ocañas, Matthew S. Walters, Bharathiraja Subramaniyan, Jordan P. Metcalf, and Constantin Georgescu

Subjects

Adult, Male, ciliated cells, NOTCH3 signaling, goblet cells, QH301-705.5, proliferation, Regulator, Notch signaling pathway, Biology, Article, Pulmonary Disease, Chronic Obstructive, Basic Helix-Loop-Helix Transcription Factors, Humans, COPD, Progenitor cell, RNA, Small Interfering, Biology (General), Lung, Receptor, Notch3, Aged, Cell Proliferation, Gene knockdown, Cell growth, Air, Cell Differentiation, Epithelial Cells, airway epithelium, General Medicine, HEYL, differentiation, Middle Aged, Phenotype, Tissue Donors, Cell biology, Repressor Proteins, Club cell, Gene Expression Regulation, basal stem/progenitor cells, Respiratory epithelium, Female, club cells, Signal Transduction

Abstract

Basal cells (BCs) are stem/progenitor cells of the mucociliary airway epithelium, and their differentiation is orchestrated by the NOTCH signaling pathway. NOTCH3 receptor signaling regulates BC to club cell differentiation, however, the downstream responses that regulate this process are unknown. Overexpression of the active NOTCH3 intracellular domain (NICD3) in primary human bronchial epithelial cells (HBECs) on in vitro air–liquid interface culture promoted club cell differentiation. Bulk RNA-seq analysis identified 692 NICD3-responsive genes, including the classical NOTCH target HEYL, which increased in response to NICD3 and positively correlated with SCGB1A1 (club cell marker) expression. siRNA knockdown of HEYL decreased tight junction formation and cell proliferation. Further, HEYL knockdown reduced club, goblet and ciliated cell differentiation. In addition, we observed decreased expression of HEYL in HBECs from donors with chronic obstructive pulmonary disease (COPD) vs. normal donors which correlates with the impaired differentiation capacity of COPD cells. Finally, overexpression of HEYL in COPD HBECs promoted differentiation into club, goblet and ciliated cells, suggesting the impaired capacity of COPD cells to generate a normal airway epithelium is a reversible phenotype that can be regulated by HEYL. Overall, our data identify the NOTCH3 downstream target HEYL as a key regulator of airway epithelial differentiation.

Published

2021

47. Exposure to hypoxia injures tracheal epithelium (ultrastructural study)

Author

V. Konrádová, J. Uhlík, L. Vajner, J. Herget, and J. Adášková

Subjects

airway epithelium, goblet cells, ciliated cells, ultrastructure, rabbit, Veterinary medicine, SF600-1100

Abstract

The ultrastructure of the tracheal epithelium in rabbits exposed for 96 hours to normobaric hypoxia was studied. In rabbits placed for 96 hours in environment with increased temperature and humidity, the first phase of common response of goblet cells to injury, represented mostly by degeneration of the exhausted cells, was revealed. The decrease in O2concentration highly accelerated the reaction of the goblet cells. Due to the influence of high temperature, humidity and normobaric hypoxia, the second phase of the goblet cells' reaction, massive differentiation of new secretory elements accompanied with intraepithelial mucous glands' development, was recorded. In the ciliated cells, only mild signs of pathological alteration of deeper portions of their cytoplasm were noticed. In the area of the ciliary border, significant decrease in the number of kinocilia/μm2, increase in percentage of altered cilia and morphological signs of impairment of the vital self-cleaning ability were recorded.

Published

2002

48. Morphological features of endometrial pinopodia formation during the luteal phase in women with previous unsuccessful implantation

Abstract

Pinopodia of the receptive endometrium is one of the prerequisites for successful embryo implantation.Study objective: to analyze the morphological changes of the endometrium in infertile women, in particular to investigate the apical surface of epithelial cells and pinopodia formation. Materials and methods. 12 patients with a history of previous implantation failure were examined. Patients underwent hysteroscopy with biopsy under intravenous anesthesia on 20–24th day of the menstrual cycle. Morphological structure of pinopodia on the surface of the endometrial epithelium was evaluated by scanning electron microscopy.Results. Apical surface of epitheliocytes was damaged in 16.7% studied biopsies. Morphological picture and maturity of the endometrial glands did not correspond to the actual day of the menstrual cycle in 41.7% biopsies. Degree of glands maturity in these patients was low, so there was a delay in the menstrual cycle. Ultrastructural examination showed clear changes in the structure of secretory and ciliary cells in 33.3%. On the apical surface of the secretory cells there was no or small number of microvilli; cilia of eyelashes were shortened or sometimes fused together. Pinopodia as a one of the most important components of implantation was detected in only 50% of patients. Only in 33.3% of participants visualized fully developed, mature pinopodia. Conclusions. Analysis of own data showed that in the endometrium of women with previous unsuccessful implantation there are certain morphological changes, which are physiologically manifested by a delay in the luteinizing phase of the menstrual cycle and, possibly, as a result mismatch of endometrial structure and embryo maturity. Time of pinopodia onset in participants varied from 20 to 24 days of the menstrual cycle. It is necessary to improve the design and conduct further research to study the association between the expression of receptivity markers and ultrastructural structure.

Published

2021

49. Морфологические особенности формирования пиноподий эндометрия во время лютеиновой фазы у женщин с предыдущей неудачной имплантацией

Subjects

реснитчатые клетки, ciliated cells, secretory cells, секретирующие клетки, секретуючі клітини, pinopodia, війчасті клітини, інфертильність, инфертильность, эндометрий, пиноподии, ендометрій, endometrium, infertility, піноподії

Abstract

Pinopodia of the receptive endometrium is one of the prerequisites for successful embryo implantation.Study objective: to analyze the morphological changes of the endometrium in infertile women, in particular to investigate the apical surface of epithelial cells and pinopodia formation. Materials and methods. 12 patients with a history of previous implantation failure were examined. Patients underwent hysteroscopy with biopsy under intravenous anesthesia on 20–24th day of the menstrual cycle. Morphological structure of pinopodia on the surface of the endometrial epithelium was evaluated by scanning electron microscopy.Results. Apical surface of epitheliocytes was damaged in 16.7% studied biopsies. Morphological picture and maturity of the endometrial glands did not correspond to the actual day of the menstrual cycle in 41.7% biopsies. Degree of glands maturity in these patients was low, so there was a delay in the menstrual cycle. Ultrastructural examination showed clear changes in the structure of secretory and ciliary cells in 33.3%. On the apical surface of the secretory cells there was no or small number of microvilli; cilia of eyelashes were shortened or sometimes fused together. Pinopodia as a one of the most important components of implantation was detected in only 50% of patients. Only in 33.3% of participants visualized fully developed, mature pinopodia. Conclusions. Analysis of own data showed that in the endometrium of women with previous unsuccessful implantation there are certain morphological changes, which are physiologically manifested by a delay in the luteinizing phase of the menstrual cycle and, possibly, as a result mismatch of endometrial structure and embryo maturity. Time of pinopodia onset in participants varied from 20 to 24 days of the menstrual cycle. It is necessary to improve the design and conduct further research to study the association between the expression of receptivity markers and ultrastructural structure., Одной из предпосылок для успешной имплантации эмбриона является наличие пиноподий рецептивного эндометрия. Цель исследования: проанализировать морфологические изменения эндометрия у инфертильных женщин, в частности исследовать апикальную поверхность эпителиальных клеток и формирование пиноподий.Материалы и методы. Были обследованы 12 пациенток с предыдущей неудачной имплантацией в анамнезе. Пациенткам проводили гистероскопию с биопсией под внутривенным наркозом на 20–24 день менструального цикла. Оценивалось морфологическое строение пиноподий на поверхности эпителия эндометрия с помощью сканирующей электронной микроскопии.Результаты. Среди исследуемых биоптатов у 16,7% апикальная поверхность эпителиоцитов была повреждена. Кроме того, у 41,7% морфологическая картина и зрелость желез эндометрия не соответствовала фактическому дню менструального цикла. Степень зрелости желез у этих пациенток была низкой, соответственно клинически наблюдалась задержка менструального цикла. При ультраструктурном исследовании прослеживались четкие изменения в строении секретирующих и ресничных клеток в 33,3% препаратов. На апикальной поверхности секретирующих клеток наблюдалось отсутствие или малое количество микроворсинок; реснички ресничных клеток были укорочены или местами срослись между собой. Наличие пиноподий – одной из важнейших составляющих имплантации, было обнаружено лишь у 50% пациенток. Однако при анализе строения пиноподий у остальных пациенток только у 33,3% испытуемых были визуализированы полностью развитые, зрелые пиноподии.Выводы. Анализ собственных данных показал, что в эндометрии женщин с предыдущей неудачной имплантацией имеют место определенные морфологические изменения, которые физиологически проявляются задержкой лютеинизирующей фазы менструального цикла и, возможно, как результат – несоответствием строения эндометрия и зрелости эмбриона. Морфологически срок появления пиноподий варьировал у участниц исследования от 20 до 24 дня менструального цикла. Однако для изучения взаимосвязи экспрессии маркеров рецептивности и ультраструктурных строений в одном исследовании необходимо совершенствование дизайна и проведение дальнейших исследований., Однією з передумов для успішної імплантації ембріона є наявність піноподій рецептивного ендометрія.Мета дослідження: проаналізувати морфологічні зміни ендометрія в інфертильних жінок, зокрема дослідити апікальну поверхню епітеліальних клітин і формування піноподій. Матеріали та методи. Було обстежено 12 пацієнток із попередньою невдалою імплантацією в анамнезі. Пацієнткам проводили гістероскопію з біопсією під внутрішньовенним наркозом на 20–24 день менструального циклу. Оцінювали морфологічну будову піноподій на поверхні епітелію ендометрія за допомогою скануючої електронної мікроскопії. Результати. Серед досліджуваних біоптатів у 16,7% апікальна поверхня епітеліоцитів була пошкоджена. Крім того, у 41,7% морфологічна картина і зрілість залоз ендометрія не відповідала фактичному дню менструального циклу. Ступінь зрілості залоз у цих пацієнток був низьким, відповідно клінічно спостерігалася затримка менструального циклу. При ультраструктурному дослідженні простежувалися чіткі зміни в будові секретуючих і війчастих клітин у 33,3% препаратів. На апікальній поверхні секретуючих клітин спостерігалася відсутність або мала кількість мікроворсинок; вії війкових клітин були вкорочені або подекуди зрощені між собою. Наявність піноподій – однієї з найважливіших складових імплантації, була виявлена лише у 50% пацієнток. Однак під час аналізу структури піноподій в інших пацієнток тільки у 33,3% учасниць були візуалізовані повністю розвинені, зрілі піноподії.Висновки. Аналіз власних даних показав, що в ендометрії жінок із попередньою невдалою імплантацією мають місце певні морфологічні зміни, які фізіологічно проявляються затримкою лютеїнізуючої фази менструального циклу і, можливо, як результат – невідповідністю структури ендометрія і зрілості ембріона. Морфологічно час появи піноподій варіював в учасниць дослідження від 20 до 24 дня менструального циклу. Однак для вивчення взаємозв'язку експресії маркерів рецептивності й ультраструктурної будови в одному дослідженні необхідно вдосконалення дизайну і проведення подальших досліджень.

Published

2021

50. Goblet Cell Hyperplasia Increases SARS-CoV-2 Infection in COPD

Author

Katie Bailey, K. Jerome, Masfique Mehedi, J. K. Osan, Heinz Feldmann, S. N. Talukdar, B. Ann DeMontigny, and Friederike Feldmann

Subjects

goblet cell hyperplasia, Adult, ciliated cells, squamous metaplasia, goblet cells, viruses, Cell, air-liquid interface, TMPRSS2, Article, Pulmonary Disease, Chronic Obstructive, medicine, COPD, Humans, Receptor, skin and connective tissue diseases, Syncytium, Goblet cell, Lung, Hyperplasia, business.industry, SARS-CoV-2, fungi, COVID-19, respiratory system, medicine.disease, respiratory tract diseases, medicine.anatomical_structure, Immunology, Respiratory epithelium, cell sloughing, business, syncytium

Abstract

Summary. SARS-CoV-2 has become a major problem across the globe, with approximately 50 million cases and more than 1 million deaths and currently no approved treatment or vaccine. Chronic obstructive pulmonary disease (COPD) is one of the underlying conditions in adults of any age that place them at risk for developing severe illness associated with COVID-19. We established an airway epithelium model to study SARS-CoV-2 infection in healthy and COPD lung cells. We found that both the entry receptor ACE2 and the co-factor transmembrane protease TMPRSS2 are expressed at higher levels on nonciliated goblet cell, a novel target for SARS-CoV-2 infection. We observed that SARS-CoV-2 infected goblet cells and induced syncytium formation and cell sloughing. We also found that SARS-CoV-2 replication was increased in the COPD airway epithelium likely due to COPD associated goblet cell hyperplasia. Our results reveal goblet cells play a critical role in SARS-CoV-2 infection in the lung., Graphical Abstract, In Brief: Osan et al. showed that SARS-CoV-2 preferentially infects and replicates in nonciliated goblet cells inducing syncytium formation and cell sloughing. Our results suggest that goblet cells play a critical role in SARS-CoV-2-induced pathophysiology in the lung.

Published

2020