Your search keyword '"Ofer Regev"' showing total 17 results

1. Dendritic cell ICAM-1 strengthens synapses with CD8 T cells but is not required for their early differentiation

Author

Anita Sapoznikov, Stav Kozlovski, Nehora Levi, Sara W. Feigelson, Ofer Regev, Natalia Davidzohn, Shifra Ben-Dor, Rebecca Haffner-Krausz, Ester Feldmesser, Noa Wigoda, Ekaterina Petrovich-Kopitman, Moshe Biton, and Ronen Alon

Subjects

CP: Immunology, Biology (General), QH301-705.5

Abstract

Summary: Lymphocyte priming in lymph nodes (LNs) was postulated to depend on the formation of stable T cell receptor (TCR)-specific immune synapses (ISs) with antigen (Ag)-presenting dendritic cells (DCs). The high-affinity LFA-1 ligand ICAM-1 was implicated in different ISs studied in vitro. We dissect the in vivo roles of endogenous DC ICAM-1 in Ag-stimulated T cell proliferation and differentiation and find that under type 1 polarizing conditions in vaccinated or vaccinia virus-infected skin-draining LNs, Ag-presenting DCs engage in ICAM-1-dependent stable conjugates with a subset of Ag-specific CD8 blasts. Nevertheless, in the absence of these conjugates, CD8 lymphocyte proliferation and differentiation into functional cytotoxic T cells (CTLs) and skin homing effector lymphocytes takes place normally. Our results suggest that although CD8 T cell blasts engage in tight ICAM-1-dependent DC-T ISs, firm ISs are dispensable for TCR-triggered proliferation and differentiation into productive effector lymphocytes.

Published

2023

2. Health promotion programs in prison: attendance and role in promoting physical activity and subjective health status

Author

Riki Tesler, Ofer Regev, Ruth Birk, Sharon Barak, Yair Shapiro, Yossi Weiss, Avi Zigdon, Kathrin Ben Zvi, Yochanan Vaknin, Gizell Green, Idit Sohlberg, Moti Zwilling, and Liav Goldstein

Subjects

prison, health promotion, physical activity, health promotion programs, subjective health status, inmates, Public aspects of medicine, RA1-1270

Abstract

IntroductionMaintaining an inmate’s health can serve as a challenge due to unhealthy background, risky behavior, and long imprisonment. This study aimed to analyze the prevalence of participation in health promotion activities among Israeli inmates and its association with their physical activity levels and subjective health status.MethodsA cross-sectional study was designed to examine 522 inmates (429 males, 93 females). The data were collected by trained face-to-face interviewers and self-report questionnaires.ResultsMost of the participants (82.37%) did not meet the recommended physical activity level. Half of the participants reported that their physical activity levels decreased since they were in prison compared with 29.50% who reported that their physical activity levels increased. Physical activity and subjective health status were significantly higher among younger male inmates. Furthermore, participation in health-promoting activities was associated with higher levels of physical activity and subjective health status.DiscussionHealth promotion activities may play an important role in addressing the challenges of maintaining inmate health. Implications of the findings are further discussed.

Published

2023

3. ICAMs are dispensable for influenza clearance and anti-viral humoral and cellular immunity

Author

Stav Kozlovski, Ofer Regev, Anita Sapoznikov, Marina Kizner, Hagit Achdout, Ekaterina Petrovich-Kopitman, Jacob Elkahal, Yoseph Addadi, Fernanda Vargas E. Silva Castanheira, Sara W. Feigelson, Paul Kubes, Noam Erez, Natalio Garbi, and Ronen Alon

Subjects

leukocyte trafficking, integrins, endothelium, inflammation, memory, Immunologic diseases. Allergy, RC581-607

Abstract

αLβ2 (LFA-1) mediated interactions with ICAM-1 and ICAM-2 predominate leukocyte-vascular interactions, but their functions in extravascular cell-cell communications is still debated. The roles of these two ligands in leukocyte trafficking, lymphocyte differentiation, and immunity to influenza infections were dissected in the present study. Surprisingly, double ICAM-1 and ICAM-2 knock out mice (herein ICAM-1/2-/- mice) infected with a lab adapted H1N1 influenza A virus fully recovered from infection, elicited potent humoral immunity, and generated normal long lasting anti-viral CD8+ T cell memory. Furthermore, lung capillary ICAMs were dispensable for both NK and neutrophil entry to virus infected lungs. Mediastinal lymph nodes (MedLNs) of ICAM-1/2-/- mice poorly recruited naïve T cells and B lymphocytes but elicited normal humoral immunity critical for viral clearance and effective CD8+ differentiation into IFN-γ producing T cells. Furthermore, whereas reduced numbers of virus specific effector CD8+ T cells accumulated inside infected ICAM-1/2-/- lungs, normal virus-specific TRM CD8+ cells were generated inside these lungs and fully protected ICAM-1/2-/- mice from secondary heterosubtypic infections. B lymphocyte entry to the MedLNs and differentiation into extrafollicular plasmablasts, producing high affinity anti-influenza IgG2a antibodies, were also ICAM-1 and ICAM-2 independent. A potent antiviral humoral response was associated with accumulation of hyper-stimulated cDC2s in ICAM null MedLNs and higher numbers of virus-specific T follicular helper (Tfh) cells generated following lung infection. Mice selectively depleted of cDC ICAM-1 expression supported, however, normal CTL and Tfh differentiation following influenza infection, ruling out essential co-stimulatory functions of DC ICAM-1 in CD8+ and CD4+ T cell differentiation. Collectively our findings suggest that lung ICAMs are dispensable for innate leukocyte trafficking to influenza infected lungs, for the generation of peri-epithelial TRM CD8+ cells, and long term anti-viral cellular immunity. In lung draining LNs, although ICAMs promote lymphocyte homing, these key integrin ligands are not required for influenza-specific humoral immunity or generation of IFN-γ effector CD8+ T cells. In conclusion, our findings suggest unexpected compensatory mechanisms that orchestrate protective anti-influenza immunity in the absence of vascular and extravascular ICAMs.

Published

2023

4. ICAM-1 on Breast Cancer Cells Suppresses Lung Metastasis but Is Dispensable for Tumor Growth and Killing by Cytotoxic T Cells

Author

Ofer Regev, Marina Kizner, Francesco Roncato, Maya Dadiani, Massimo Saini, Francesc Castro-Giner, Olga Yajuk, Stav Kozlovski, Nehora Levi, Yoseph Addadi, Ofra Golani, Shifra Ben-Dor, Zvi Granot, Nicola Aceto, and Ronen Alon

Subjects

adhesion, killing, metastasis, integrins, neutrophils, vasculature, Immunologic diseases. Allergy, RC581-607

Abstract

Breast tumors and their derived circulating cancer cells express the leukocyte β2 integrin ligand Intercellular adhesion molecule 1 (ICAM-1). We found that elevated ICAM-1 expression in breast cancer cells results in a favorable outcome and prolonged survival of breast cancer patients. We therefore assessed the direct in vivo contribution of ICAM-1 expressed by breast cancer cells to breast tumorigenesis and lung metastasis in syngeneic immunocompetent mice hosts using spontaneous and experimental models of the lung metastasis of the C57BL/6-derived E0771 cell line, a luminal B breast cancer subtype. Notably, the presence of ICAM-1 on E0771 did not alter tumor growth or the leukocyte composition in the tumor microenvironment. Interestingly, the elimination of Tregs led to the rapid killing of primary tumor cells independently of tumor ICAM-1 expression. The in vivo elimination of a primary E0771 tumor expressing the ovalbumin (OVA) model neoantigen by the OVA-specific OVA-tcr-I mice (OT-I) transgenic cytotoxic T lymphocytes (CTLs) also took place normally in the absence of ICAM-1 expression by E0771 breast cancer target cells. The whole lung imaging of these cells by light sheet microscopy (LSM) revealed that both Wild type (WT)- and ICAM-1-deficient E0771 cells were equally disseminated from resected tumors and accumulated inside the lung vasculature at similar magnitudes. ICAM-1-deficient breast cancer cells developed, however, much larger metastatic lesions than their control counterparts. Strikingly, the vast majority of these cells gave rise to intravascular tumor colonies both in spontaneous and experimental metastasis models. In the latter model, ICAM-1 expressing E0771- but not their ICAM-1-deficient counterparts were highly susceptible to elimination by neutrophils adoptively transferred from E0771 tumor-bearing donor mice. Ex vivo, neutrophils derived from tumor-bearing mice also killed cultured E0771 cells via ICAM-1-dependent interactions. Collectively, our results are a first indication that ICAM-1 expressed by metastatic breast cancer cells that expand inside the lung vasculature is involved in innate rather than in adaptive cancer cell killing. This is also a first indication that the breast tumor expression of ICAM-1 is not required for CTL-mediated killing but can function as a suppressor of intravascular breast cancer metastasis to lungs.

Published

2022

5. Assessment of Nutritional Status and Health Perception among Male Inmates in Israeli Prisons

Author

Shani Ben Aharon, Ofer Regev, Riki Tesler, Sharon Barak, Yair Shapira, Yossi Weiss, Noa Shtainmetz, Yochanan Vaknin, Liav Goldstein, Kathrine Ben-Zvi, and Ruth Birk

Subjects

inmates, nutrition, subjective health status, well-being, overweight, obesity, Nutrition. Foods and food supply, TX341-641

Abstract

The nutritional and health perceptions of inmates are crucial to their overall well-being. However, limited research has been conducted on this topic. This study aimed to assess the nutritional and health perception state of male inmates in eleven prisons in Israel. A cross-sectional study was conducted between February and September 2019 with 176 voluntary participants. Structured questionnaires were used to collect data on socio-demographic characteristics, healthy habits, subjective health status, and prison situation variables. The study found that the prevalence of overweight (40%) and obesity (18.1%) among 18–34-year-old inmates was significantly higher than in the reference Israeli population. Short detention periods (up to one year) predicted less weight gain, while older age predicted poorer health status. Better emotional status significantly predicted better subjective health status among male inmates. There is a need for nutrition interventions to improve the health of inmates. The significant weight gain during incarceration and the associated lower health index and stress highlights the importance of increasing knowledge and promoting a healthier lifestyle in incarceration as early as possible and continuing over time.

Published

2023

6. Microtubule destabilization is a critical checkpoint of chemotaxis and transendothelial migration in melanoma cells but not in T cells

Author

Francesco Roncato, Ofer Regev, Sandeep Kumar Yadav, and Ronen Alon

Subjects

cytoskeleton, motility, cancer, metastasis, taxol, Cytology, QH573-671

Abstract

Microtubules (MTs) control cell shape and intracellular cargo transport. The role of MT turnover in the migration of slow-moving cells through endothelial barriers remains unclear. To irreversibly interfere with MT disassembly, we have used the MT-stabilizing agent zampanolide (ZMP) in Β16F10 melanoma as amodel of slow-moving cells. ZMP-treated B16 cells failed to follow chemotactic gradients across rigid confinements and could not generate stable sub-endothelial pseudopodia under endothelial monolayers. In vivo, ZMP-treated Β16 cells failed to extravasate though lung capillaries. In contrast to melanoma cells, the chemotaxis and transendothelial migration of ZMP-treated Tcells were largely conserved. This is afirst demonstration that MT disassembly is akey checkpoint in the directional migration of cancer cells but not of lymphocytes.

Published

2021

7. p53 in Bronchial Club Cells Facilitates Chronic Lung Inflammation by Promoting Senescence

Author

Adi Sagiv, Amir Bar-Shai, Naama Levi, Miki Hatzav, Lior Zada, Yossi Ovadya, Lior Roitman, Gal Manella, Ofer Regev, Julia Majewska, Ezra Vadai, Raya Eilam, Sara W. Feigelson, Michael Tsoory, Michel Tauc, Ronen Alon, and Valery Krizhanovsky

Subjects

Biology (General), QH301-705.5

Abstract

Summary: The tumor suppressor p53 limits tumorigenesis by inducing apoptosis, cell cycle arrest, and senescence. Although p53 is known to limit inflammation during tumor development, its role in regulating chronic lung inflammation is less well understood. To elucidate the function of airway epithelial p53 in such inflammation, we subjected genetically modified mice, whose bronchial epithelial club cells lack p53, to repetitive inhalations of lipopolysaccharide (LPS), an exposure that leads to severe chronic bronchitis and airway senescence in wild-type mice. Surprisingly, the club cell p53 knockout mice exhibited reduced airway senescence and bronchitis in response to chronic LPS exposure and were significantly protected from global lung destruction. Furthermore, pharmacological elimination of senescent cells also protected wild-type mice from chronic LPS-induced bronchitis. Our results implicate p53 in induction of club-cell senescence and correlate epithelial cell senescence of chronic airway inflammation and lung destruction. : Sagiv et al. find that senescence and p53 in bronchial epithelial cells promote chronic lung inflammation and COPD-like disease. Genetic or pharmacological reduction in senescent cell number blunts chronic inflammation and limits disease progression. Keywords: cellular senescence, p53, bronchitis, inflammation, club cells

Published

2018

8. ICAMs Are Not Obligatory for Functional Immune Synapses between Naive CD4 T Cells and Lymph Node DCs

Author

Sara W. Feigelson, Adam Solomon, Adi Biram, Miki Hatzav, Moria Lichtenstein, Ofer Regev, Stav Kozlovski, Diana Varol, Caterina Curato, Dena Leshkowitz, Steffen Jung, Ziv Shulman, and Ronen Alon

Subjects

T cell activation, adaptive immunity, vaccination, antigens, differentiation, inflammation, Biology (General), QH301-705.5

Abstract

Protective immune responses depend on the formation of immune synapses between T cells and antigen-presenting cells (APCs). The two main LFA-1 ligands, ICAM-1 and ICAM-2, are co-expressed on many cell types, including APCs and blood vessels. Although these molecules were suggested to be key players in immune synapses studied in vitro, their contribution to helper T cell priming in vivo is unclear. Here, we used transgenic mice and intravital imaging to examine the role of dendritic cell (DC) ICAM-1 and ICAM-2 in naive CD4 T cell priming and differentiation in skin-draining lymph nodes. Surprisingly, ICAM deficiency on endogenous CD40-stimulated lymph node DCs did not impair their ability to arrest and prime CD4 lymphocyte activation and differentiation into Th1 and Tfh effectors. Thus, functional T cell receptor (TCR)-specific helper T cell synapses with antigen-presenting DCs and subsequent proliferation and early differentiation into T effectors do not require LFA-1-mediated T cell adhesiveness to DC ICAMs.

Published

2018

9. Microtubule destabilization is a critical checkpoint of chemotaxis and transendothelial migration in melanoma cells but not in T cells

Author

Ronen Alon, Ofer Regev, Francesco Roncato, and Sandeep Kumar Yadav

Subjects

Male, 0301 basic medicine, Short Communication, T-Lymphocytes, Motility, macromolecular substances, Microtubules, Metastasis, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Cell Movement, Microtubule, Cell Line, Tumor, medicine, cancer, metastasis, Animals, Pseudopodia, Cytoskeleton, Melanoma, taxol, QH573-671, Chemistry, Brief Report, Chemotaxis, Transendothelial and Transepithelial Migration, Cancer, Cell Biology, medicine.disease, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, motility, 030220 oncology & carcinogenesis, Macrolides, Cytology, Intracellular

Abstract

Microtubules (MTs) control cell shape and intracellular cargo transport. The role of MT turnover in the migration of slow-moving cells through endothelial barriers remains unclear. To irreversibly interfere with MT disassembly, we have used the MT-stabilizing agent zampanolide (ZMP) in Β16F10 melanoma as amodel of slow-moving cells. ZMP-treated B16 cells failed to follow chemotactic gradients across rigid confinements and could not generate stable sub-endothelial pseudopodia under endothelial monolayers. In vivo, ZMP-treated Β16 cells failed to extravasate though lung capillaries. In contrast to melanoma cells, the chemotaxis and transendothelial migration of ZMP-treated Tcells were largely conserved. This is afirst demonstration that MT disassembly is akey checkpoint in the directional migration of cancer cells but not of lymphocytes.

Published

2021

10. Mesenchymal soluble factors confer imatinib drug resistance in chronic myelogenous leukemia cells

Author

Meshel Nicola, Noa Kidan, Martin Ruthardt, Ofer Regev, Jamal Mahajna, and Hazem Khamisie

Subjects

Crizotinib, business.industry, Mesenchymal stem cell, medicine, Cancer research, Imatinib, General Medicine, Drug resistance, medicine.disease, business, Letter to the Editor, medicine.drug, Chronic myelogenous leukemia

Published

2020

11. Reduced Lamin A/C Does Not Facilitate Cancer Cell Transendothelial Migration but Compromises Lung Metastasis

Author

Ofer Regev, Ronen Alon, Yossi Ovadya, Francesco Roncato, Gabi Gerlitz, Sandeep Kumar Yadav, Yoseph Addadi, Ester Feldmesser, Sérgio F. de Almeida, Marina Kizner, Nehora Levi, João C. Sabino, Diana Drago-Garcia, Sara W. Feigelson, Lukasz Kaczmarczyk, and Samuel Ovadia

Subjects

0301 basic medicine, EXPRESSION, Cancer Research, animal structures, Cell, Article, Metastasis, PATHWAY, 03 medical and health sciences, MOVEMENT, 0302 clinical medicine, Downregulation and upregulation, cancer metastasis, medicine, RNA-SEQ, chemotaxis, NUCLEAR-ENVELOPE, RC254-282, REPAIR, Gene knockdown, Science & Technology, epigenetics, Chemistry, nucleus, diapedesis, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, imaging, STIFFNESS, medicine.disease, Extravasation, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Oncology, DNA-DAMAGE, SENESCENCE, 030220 oncology & carcinogenesis, Cancer cell, embryonic structures, Nuclear lamina, GROWTH, Life Sciences & Biomedicine, Lamin, extravasation

Abstract

Simple Summary The nucleus is the largest and stiffest organelle of tumor cells. Cancer metastasis depends on the ability of cancer cells circulating in the blood to exit blood vessels and survive in target organs. The roles of the shell (lamina) of the nucleus in cancer cell migration and survival in distinct organs of metastasis are still unclear. A-type lamins are key lamina components that increase nuclear stiffness and reduce squeezing capacity through highly rigid barriers. We addressed how reduced expression of A-lamins (lamin A/C) affects cancer cell survival and crossing of endothelial barriers and lung capillaries and found that reduced lamin A/C expression impairs cancer growth in spheroids and restricts cancer metastasis to lungs without improving cancer cell squeezing and extravasation from lung vessels, the key platform for cancer entry into lungs. Abstract The mechanisms by which the nuclear lamina of tumor cells influences tumor growth and migration are highly disputed. Lamin A and its variant lamin C are key lamina proteins that control nucleus stiffness and chromatin conformation. Downregulation of lamin A/C in two prototypic metastatic lines, B16F10 melanoma and E0771 breast carcinoma, facilitated cell squeezing through rigid pores, and reduced heterochromatin content. Surprisingly, both lamin A/C knockdown cells grew poorly in 3D spheroids within soft agar, and lamin A/C deficient cells derived from spheroids transcribed lower levels of the growth regulator Yap1. Unexpectedly, the transendothelial migration of both cancer cells in vitro and in vivo, through lung capillaries, was not elevated by lamin A/C knockdown and their metastasis in lungs was even dramatically reduced. Our results are the first indication that reduced lamin A/C content in distinct types of highly metastatic cancer cells does not elevate their transendothelial migration (TEM) capacity and diapedesis through lung vessels but can compromise lung metastasis at a post extravasation level.

Published

2021

12. ICAMs Are Not Obligatory for Functional Immune Synapses between Naive CD4 T Cells and Lymph Node DCs

Author

Adam Solomon, Miki Hatzav, Ronen Alon, Moria Lichtenstein, Dena Leshkowitz, Ofer Regev, Adi Biram, Sara W. Feigelson, Diana Varol, Steffen Jung, Ziv Shulman, Stav Kozlovski, and Caterina Curato

Subjects

CD4-Positive T-Lymphocytes, 0301 basic medicine, Priming (immunology), Inflammation, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, antigens, medicine, Humans, lcsh:QH301-705.5, Lymph node, T cell activation, T-cell receptor, Dendritic Cells, adaptive immunity, differentiation, Dendritic cell, Intercellular Adhesion Molecule-1, vaccination, Acquired immune system, Cell biology, 030104 developmental biology, medicine.anatomical_structure, lcsh:Biology (General), inflammation, Lymph Nodes, medicine.symptom, 030215 immunology

Abstract

Summary Protective immune responses depend on the formation of immune synapses between T cells and antigen-presenting cells (APCs). The two main LFA-1 ligands, ICAM-1 and ICAM-2, are co-expressed on many cell types, including APCs and blood vessels. Although these molecules were suggested to be key players in immune synapses studied in vitro , their contribution to helper T cell priming in vivo is unclear. Here, we used transgenic mice and intravital imaging to examine the role of dendritic cell (DC) ICAM-1 and ICAM-2 in naive CD4 T cell priming and differentiation in skin-draining lymph nodes. Surprisingly, ICAM deficiency on endogenous CD40-stimulated lymph node DCs did not impair their ability to arrest and prime CD4 lymphocyte activation and differentiation into Th1 and Tfh effectors. Thus, functional T cell receptor (TCR)-specific helper T cell synapses with antigen-presenting DCs and subsequent proliferation and early differentiation into T effectors do not require LFA-1-mediated T cell adhesiveness to DC ICAMs.

Published

2018

13. Abstract 2726: Nuclear checkpoints for melanoma and breast cancer lung metastasis

Author

Ronen Alon, Gabi Gerlitz, Francesco Roncato, Sara W. Feigelson, Ofer Regev, and Nehora Levi

Subjects

Cancer Research, Chemistry, Cell, Intravasation, Cancer, medicine.disease, Extravasation, Metastasis, medicine.anatomical_structure, Oncology, Cancer cell, medicine, Cancer research, Nuclear lamina, Lamin

Abstract

Introduction Metastasis involves cancer cell intravasation and extravasation from blood vessels at target organs. The mechanisms by which the nuclei of metastatic tumor cells squeeze through different vascular and epithelial barriers are poorly understood. The nuclear lamina attaches chromatin domains to the nuclear periphery and controls the mechanical properties of the nucleus and its crosstalk with the cell cytoskeleton. A-type lamins, lamin A and its splice variant lamin C, are key nuclear lamina proteins that control nucleus stiffness and regulate chromatin conformation. Reduced lamin A was reported in some aggressive cancers. Results and Discussion Using a new in vitro transendothelial migration (TEM) assay we found that melanoma and breast cancer cells slowly squeeze their nuclei and complete TEM through endothelial junctions irrespective of their relative lamin A/C levels, suggesting that lamin A/C dependent nuclear stiffening is not a rate-limiting step for cancer cell squeezing through endothelial cells in vitro. In contrast, reduced lamin A/C enhanced cancer cell squeezing through rigid pores. Tumor emigration analysis across blood vessels in vivo was performed by new 3D imaging of fluorescently labeled cancer cells with high and low lamin A/C levels. This imaging was based on light sheet microscopy of lipid-cleared lungs of recipient mice in situ labeled with anti-vascular CD31 mAb. Using this technology, we found that reduced lamin A/C expression did not enhance the emigration of circulating murine melanoma and breast cancer cells across lung capillaries in vivo. Lower lamin A/C levels reduced the constitutive, transcriptionally repressed, heterochromatin in both melanoma and breast cancer cells. Decreased lamin A/C expression did not enhance however, nuclear rupture in the tumor cells that entered the lung parenchyma. The outcomes of the epigenetic and mechanical changes resulting of lamin A/C suppression on tumor growth and metastasis are under current investigation. Conclusions Our results suggest that subsets of tumor cells may benefit from reducing their nuclear content of lamin A/C mainly at the level of rigid barrier crossing (e.g. dense interstitial spaces), but not at the level of extravasation or post extravasation survival at target organs. How alterations in lamin A/C content contribute to tumor heterogeneity and metastatic potential of singular cancer cells remains an open question. Citation Format: Francesco Roncato, Ofer Regev, Nehora Levi, Sara W. Feigelson, Gabi Gerlitz, Ronen Alon. Nuclear checkpoints for melanoma and breast cancer lung metastasis [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 2726.

Published

2020

14. p53 in Bronchial Club Cells Facilitates Chronic Lung Inflammation by Promoting Senescence

Author

Julia Majewska, Amir Bar-Shai, Michael Tsoory, Raya Eilam, Adi Sagiv, Gal Manella, Naama Levi, Michel Tauc, Valery Krizhanovsky, Lior Zada, Sara W. Feigelson, Ezra Vadai, Ofer Regev, Miki Hatzav, Yossi Ovadya, Lior Roitman, Ronen Alon, Weizmann Institute of Science [Rehovot, Israël], Laboratoire CNRS 3093, Université de Nice-Sophia Antipolis, Centre National de la Recherche Scientifique (CNRS), Department of Immunology, and Department of Molecular Cell Biology [Rehovot]

Subjects

0301 basic medicine, Senescence, Chronic bronchitis, [SDV]Life Sciences [q-bio], Inflammation, Bronchi, medicine.disease_cause, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Mice, 0302 clinical medicine, medicine, Animals, lcsh:QH301-705.5, Cellular Senescence, ComputingMilieux_MISCELLANEOUS, Lung, business.industry, Pneumonia, respiratory system, medicine.disease, respiratory tract diseases, 3. Good health, Mice, Inbred C57BL, 030104 developmental biology, Club cell, medicine.anatomical_structure, lcsh:Biology (General), 030220 oncology & carcinogenesis, Knockout mouse, Chronic Disease, Cancer research, Disease Progression, Bronchitis, Female, medicine.symptom, Tumor Suppressor Protein p53, Carcinogenesis, business

Abstract

Summary: The tumor suppressor p53 limits tumorigenesis by inducing apoptosis, cell cycle arrest, and senescence. Although p53 is known to limit inflammation during tumor development, its role in regulating chronic lung inflammation is less well understood. To elucidate the function of airway epithelial p53 in such inflammation, we subjected genetically modified mice, whose bronchial epithelial club cells lack p53, to repetitive inhalations of lipopolysaccharide (LPS), an exposure that leads to severe chronic bronchitis and airway senescence in wild-type mice. Surprisingly, the club cell p53 knockout mice exhibited reduced airway senescence and bronchitis in response to chronic LPS exposure and were significantly protected from global lung destruction. Furthermore, pharmacological elimination of senescent cells also protected wild-type mice from chronic LPS-induced bronchitis. Our results implicate p53 in induction of club-cell senescence and correlate epithelial cell senescence of chronic airway inflammation and lung destruction. : Sagiv et al. find that senescence and p53 in bronchial epithelial cells promote chronic lung inflammation and COPD-like disease. Genetic or pharmacological reduction in senescent cell number blunts chronic inflammation and limits disease progression. Keywords: cellular senescence, p53, bronchitis, inflammation, club cells

Published

2018

15. High avidity TCR-peptide interactions between CD4 lymphocytes and lymph node dendritic cells promote normal lymphocyte arrest, activation, proliferation, and differentiation independently of dendritic cell ICAM-1 and 2

Author

Sara W Feigelson, Adam Solomon, Adi Biram, Miki Hatzav, Maria Lichtenstein, Ofer Regev, Caterina Curato, Diana Rashkovan, Dena Lefkowitz, Steffen Jung, Ziv Shulman, and Ronen Alon

Subjects

Immunology, Immunology and Allergy

Abstract

The two main LFA-1 ligands ICAM-1 and ICAM-2 are constitutively co-expressed on antigen presenting cells (APCs) and on the lymph node stroma. We find abrogated antigen specific CD4 T cell priming in ICAM-1 and ICAM-2 deficient spleens. Nevertheless, the in vivo contribution of these ligands to lymphocyte activation proliferation and differentiation in lymph nodes has been difficult to dissect in total knockout mice due to their multiple roles in lymphocyte entry and priming in these organs. We therefore constructed lethally irradiated chimeric mice reconstituted with ICAM-1 and 2 double knock out (DKO) APCs in which lymphocyte entry into peripheral lymph nodes was reconstituted. Strikingly, these mice elicited normal antigen specific OT-II T cell activation, proliferation and differentiation into Th1 and Tfh effectors. OT-II T cells could also normally arrest on DCs deficient in ICAM-1 and 2. A compensatory role of VCAM-1 in ICAM deficient DCs was ruled out. Nevertheless, polyclonal T cell proliferation in response to endogenous self-antigens required the presence of ICAM-1 and ICAM-2 on endogenous lymph node DCs. Our results are the first indication that high avidity TCR peptide-MHC-II recognition can bypass integrin-mediated lymphocyte adhesions to DCs under specific settings.

Published

2017

16. p21 facilitates chronic lung inflammation via epithelial and endothelial cells

Author

Naama Levi, Nurit Papismadov, Julia Majewska, Lior Roitman, Noa Wigoda, Raya Eilam, Michael Tsoory, Ron Rotkopf, Yossi Ovadya, Hagay Akiva, Ofer Regev, and Valery Krizhanovsky

Subjects

Aging, Cell Biology

17. Nuclear lamin A/C promotes cancer cell survival and lung metastasis without restricting transendothelial migration

Author

Francesco Roncato, Marina Kizner, Sandeep Kumar Yadav, Diana Drago-Garcia, Ofer Regev, Ronen Alon, Ester Feldmesser, Sérgio F. de Almeida, Yossi Ovadya, Gabi Gerlitz, Nehora Levi, Sara W. Feigelson, Lukasz Kaczmarczyk, Samuel Ovadia, Yoseph Addadi, and João C. Sabino

Subjects

0303 health sciences, Gene knockdown, animal structures, Chemistry, Melanoma, Cell, medicine.disease, In vitro, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Downregulation and upregulation, 030220 oncology & carcinogenesis, embryonic structures, Cancer cell, medicine, Cancer research, Nuclear lamina, Lamin, 030304 developmental biology

Abstract

The mechanisms by which the nuclear lamina of tumor cells controls their migration and survival are poorly understood. Lamin A and its variant lamin C are key nuclear lamina proteins that control nucleus stiffness and chromatin conformation. Downregulation of lamin A/C levels in two metastatic lines, B16F10 melanoma and E0771 breast carcinoma, facilitated cell squeezing through rigid pores, elevated nuclear deformability and reduced heterochromatin. Unexpectedly, the transendothelial migration of both cancer cells in vitro and in vivo, through lung capillaries, was not elevated by lamin A/C knockdown. Both cancer cells with lamin A/C knockdown grew normally in primary tumors and in vitro on rigid surfaces. Strikingly, however, both lamin A/C deficient melanoma and breast cancer cells grew poorly in 3D spheroids expanded in soft agar cultures. Experimental lung metastasis of both lamin A/C knockdown cells was also markedly reduced. Taken together, our results suggest that high content of lamin A/C in multiple cancer cells promotes cancer cell survival and ability to generate lung metastasis without compromising cancer cell emigration from lung vessels.