Assessment of High Purity Mesenchymal Stromal Cells Derived Extracellular Vesicles Presenting NRP1 Show Functional Suppression of Activated Immune Cells

Gobin, Jonathan

04 January 2022

Background: The focus of this study was to investigate how producing human bone marrow (hBM) derived mesenchymal stromal cell (MSC) extracellular vehicles (EVs) in a high purity isolation system would affect their established characterization criteria and address the validity of these methods of EV production. Additionally, we set out to functionally characterize the hBM-MSC-EVs for their identified immunomodulatory ability while also assessing the presence of novel MSC-EV marker NRP1 identified by our group to further affirm its validity as a functional MSC-EV identity marker. Methods: Each hBM-MSC-EV donor was cultured in a hollow-fiber bioreactor system in non-stimulating serum/xeno-free conditions for 25 days to produce EVs persistently under quiescent conditions to characterize the hBM-MSC-EVs in their native form. EVs were isolated by traditional PEG-based precipitation for preliminary characterization to monitor bioreactor production wherein they were characterized using multimodal tangential flow filtration coupled with fast protein liquid chromatograph (FPLC) size exclusion/high-affinity purifications to obtain the final highly purified EV sample. Additionally, functional analysis of their immunomodulatory ability, EVs and MSCs were incubated with activated peripheral blood mononuclear cells (PBMCs) as an in-vitro model to evaluate their potency. Results: The hBM-MSC-EVs produced from the bioreactor system showed consistent characterization in accordance with the MISEV2018 establish criteria. We were also able to demonstrate their functional ability by observing statistically significantly immunomodulatory ability of activated PBMCs equivalent to native MSC ability. We were also able to validate the present of NRP1 on all hBM-MSC-EV samples produced confirming its validity as a MSC-EV marker. Conclusion: The significance of the results obtained from this study confirms the production of MSC-EV using a bioreactor and high purity isolation for obtaining consistent MSC-EVs for downstream investigation. Additionally, we were able to demonstrate the significance of MSC-EVs on MSC signaling for immunomodulation by showing equivalent functional potency when tested in-vitro. These results contribute to further understanding the biological attributes of MSC-EVs and contribute to the validation of currently established characterization guidelines.

Extracellular Vesicles (EVs)

NRP1

Mesenchymal Stromal Cells (MSCs)

Bioreactor

Tangential Flow Filtration (TFF)

Nanoparticle Trackning Analysis (NTA)

Immune Suppression

Characterization

Isolation

ISEV

ISCT

cGMP

Pre-clinical

Cell based therapy

Bovine and Porcine Adipogenesis, Myogenesis, and Tissue Engineering Strategies to Improve Flavor and Pigmentation of Cell-Based Meat

Krieger, Jessica

02 December 2020

No description available.

Biomedical Engineering

Biomedical Research

Food Science

Food science

meat science

bioengineering

biomedical engineering

biomedical sciences

in vitro meat

cell-based meat

cultured meat

cultivated meat

myogenesis

adipogenesis

bovine

porcine

myoglobin

How to Obtain a Mega-Intestine with Normal Morphology: In Silico Modelling of Postnatal Intestinal Growth in a Cd97-Transgenic Mouse

Hofmann, Felix, Thalheim, Torsten, Rother, Karen, Quaas, Marianne, Kerner, Christiane, Przybilla, Jens, Aust, Gabriela, Galle, Joerg

11 December 2023

Intestinal cylindrical growth peaks in mice a few weeks after birth, simultaneously with crypt fission activity. It nearly stops after weaning and cannot be reactivated later. Transgenic mice expressing Cd97/Adgre5 in the intestinal epithelium develop a mega-intestine with normal microscopic morphology in adult mice. Here, we demonstrate premature intestinal differentiation in Cd97/Adgre5 transgenic mice at both the cellular and molecular levels until postnatal day 14. Subsequently, the growth of the intestinal epithelium becomes activated and its maturation suppressed. These changes are paralleled by postnatal regulation of growth factors and by an increased expression of secretory cell markers, suggesting growth activation of non-epithelial tissue layers as the origin of enforced tissue growth. To understand postnatal intestinal growth mechanistically, we study epithelial fate decisions during this period with the use of a 3D individual cell-based computer model. In the model, the expansion of the intestinal stem cell (SC) population, a prerequisite for crypt fission, is largely independent of the tissue growth rate and is therefore not spontaneously adaptive. Accordingly, the model suggests that, besides the growth activation of non-epithelial tissue layers, the formation of a mega-intestine requires a released growth control in the epithelium, enabling accelerated SC expansion. The similar intestinal morphology in Cd97/Adgre5 transgenic and wild type mice indicates a synchronization of tissue growth and SC expansion, likely by a crypt density-controlled contact inhibition of growth of intestinal SC proliferation. The formation of a mega-intestine with normal microscopic morphology turns out to originate in changes of autonomous and conditional specification of the intestinal cell fate induced by the activation of Cd97/Adgre5.

info:eu-repo/classification/ddc/500

ddc:500

Development of a novel cell-based screening platform to identify inhibitors of viral interferon antagonists from clinically important viruses

Vasou, Andri

January 2016

All viruses encode for at least one viral interferon (IFN) antagonist, which is used to subvert the cellular IFN response, a powerful antiviral innate immune response. Numerous in vitro and in vivo studies have demonstrated that IFN antagonism is crucial for virus survival, suggesting that viral IFN antagonists could represent promising therapeutic targets. This study focuses on Respiratory Syncytial Virus (RSV), an important human pathogen for which there is no vaccine or virus-specific antiviral drug. RSV encodes two IFN antagonists NS1 and NS2, which play a critical role in RSV replication and pathogenicity. We developed a high-throughput screening (HTS) assay to target NS2 via our A549.pr(ISRE)GFP-RSV/NS2 cell-line, which contains a GFP gene under the control of an IFN-stimulated response element (ISRE) to monitor IFN- signalling pathway. NS2 inhibits the IFN-signalling pathway and hence GFP expression in the A549.pr(ISRE)GFP-RSV/NS2 cell-line by mediating STAT2 degradation. Using a HTS approach, we screened 16,000 compounds to identify small molecules that inhibit NS2 function and therefore relinquish the NS2 imposed block to IFN-signalling, leading to restoration of GFP expression. A total of twenty-eight hits were identified; elimination of false positives left eight hits, four of which (AV-14, -16, -18, -19) are the most promising. These four hit compounds have EC₅₀ values in the single μM range and three of them (AV-14, -16, -18) represent a chemically related series with an indole structure. We demonstrated that the hit compounds specifically inhibit the STAT2 degradation function of NS2, not the function of NS1 or unrelated viral IFN antagonists. At the current time, compounds do not restrict RSV replication in vitro, hence hit optimization is required to improve their potency. Nonetheless, these compounds could be used as chemical tools to determine the unknown mechanism by which NS2 mediates STAT2 degradation and tackle fundamental questions about RSV biology.

616.07

Label-free surface-enhanced Raman spectroscopy-linked immunosensor assay (SLISA) for environmental surveillance

bhardwaj, vinay

02 October 2015

The contamination of the environment, accidental or intentional, in particular with chemical toxins such as industrial chemicals and chemical warfare agents has increased public fear. There is a critical requirement for the continuous detection of toxins present at very low levels in the environment. Indeed, some ultra-sensitive analytical techniques already exist, for example chromatography and mass spectroscopy, which are approved by the US Environmental Protection Agency for the detection of toxins. However, these techniques are limited to the detection of known toxins. Cellular expression of genomic and proteomic biomarkers in response to toxins allows monitoring of known as well as unknown toxins using Polymerase Chain Reaction and Enzyme Linked Immunosensor Assays. However, these molecular assays allow only the endpoint (extracellular) detection and use labels such as fluorometric, colorimetric and radioactive, which increase chances of uncertainty in detection. Additionally, they are time, labor and cost intensive. These technical limitations are unfavorable towards the development of a biosensor technology for continuous detection of toxins. Federal agencies including the Departments of Homeland Security, Agriculture, Defense and others have urged the development of a detect-to-protect class of advanced biosensors, which enable environmental surveillance of toxins in resource-limited settings. In this study a Surface-Enhanced Raman Spectroscopy (SERS) immunosensor, aka a SERS-linked immunosensor assay (SLISA), has been developed. Colloidal silver nanoparticles (Ag NPs) were used to design a flexible SERS immunosensor. The SLISA proof-of-concept biosensor was validated by the measurement of a dose dependent expression of RAD54 and HSP70 proteins in response to H2O2 and UV. A prototype microchip, best suited for SERS acquisition, was fabricated using an on-chip SLISA to detect RAD54 expression in response to H2O2. A dose-response relationship between H2O2 and RAD54 is established and correlated with EPA databases, which are established for human health risk assessment in the events of chemical exposure. SLISA outperformed ELISA by allowing RISE (rapid, inexpensive, simple and effective) detection of proteins within 2 hours and 3 steps. It did not require any label and provided qualitative information on antigen-antibody binding. SLISA can easily be translated to a portable assay using a handheld Raman spectrometer and it can be used in resource-limited settings. Additionally, this is the first report to deliver Ag NPs using TATHA2, a fusogenic peptide with cell permeability and endosomal rupture release properties, for rapid and high levels of Ag NPs uptake into yeast without significant toxicity, prerequisites for the development of the first intracellular SERS immunosensor.

surface-enhanced Raman spectroscopy

Immunosensor

chemical toxins

cell-based biosensor

yeast

protein biomarkers

silver nanoparticles

SLISA

ELISA

Biochemical and Biomolecular Engineering

Bioimaging and Biomedical Optics

Biological Engineering

Biomaterials

Biomedical Devices and Instrumentation

Biotechnology

Environmental Engineering

Environmental Health

Nanomedicine

Nanoscience and Nanotechnology

Toxicology

Established and Emerging Treatments of Skin GvHD

Link-Rachner, Cornelia S., Sockel, Katja, Schuetz, Catharina

30 May 2024

Graft-versus-host disease (GvHD) of the skin is a severe allo-immune reaction and complication following allogeneic stem cell transplantation. Over the past years, intensive pre-clinical research has led to an improved understanding of the pathophysiology of acute and to a lesser extend chronic GvHD. This has translated into the approval of several new agents for the treatment of both forms of GvHD. This review summarizes the most recent advances in underlying pathomechanisms, clinical trials and newly approved agents for GvHD, with a special focus on skin involvement.

info:eu-repo/classification/ddc/610

ddc:610

Modellierung, Planung und Gestaltung der Logistikstrukturen kompetenzzellenbasierter Netze

Ackermann, Jörg

09 October 2007

Kompetenzzellenbasierte (regionale) Netze stellen besondere Anforderungen an die Modellierung, Planung und Gestaltung der Logistikstrukturen. Für die Logistikstrukturmodellierung werden ein generischer Beschreibungsrahmen für produktionslogistische soziotechnische Systeme, Definitionen u.a. zum zentralen Begriff Logistikstruktur sowie ein 3-Ebenen-Modell und Strukturtypen für eine vertiefende Materialflussanalyse und -synthese bereitgestellt. Für die Logistikstrukturplanung wird darauf aufbauend mit der Methode der Integrativen Prozess- und Systemstrukturierung (IPSS) eine Methode zur Behandlung von Strukturierungsproblemen konzipiert, die sowohl speziell für kompetenzzellenbasierte Netze als auch allgemein für Produktions- und Logistiksysteme angewandt werden kann. Für die Logistikstrukturgestaltung werden unter Modell- und Methodenverwendung Szenarien sowie Gestaltungs- und Vorzugslösungen für den Materialfluss abgeleitet. / Competence-cell based (regional) networks put special requirements on the modelling, planning and design of logistics structures. For the modelling of logistics structures, a generic description framework for production logistic sociotechnical systems, definitions for, amongst others, the central term logistics structure as well as a 3-layer-model and structure types for a more detailed material flow analysis and synthesis are provided. For the planning of logistics structures, the Method of Integrative Process and System Structuring (IPSS) is developed as a method for handling structuring problems. It can be applied especially to Competence-cell based networks as well as generally to production and logistics systems. For the design of logistics structures, scenarios as well as design and preference solutions for the material flow are derived.

3-Ebenen-Modell

3-Layer-Model

Competence-cell Based Network

Design

IPSS

Kompetenzzellenbasiertes Netz

Logistics

Logistics Network

Logistics Structure

Logistics System

Logistiknetz

Logistikstruktur

Material Flow

Modelling

Planning

Production

Production Network

Production System

Produktionsnetz

Structure Type

Structuring

Strukturtyp

ddc:620

Gestaltung

Logistik

Logistiksystem

Materialfluss

Modellierung

Planung

Produktion

Produktionssystem

Strukturierung

Modellierung, Planung und Gestaltung der Logistikstrukturen kompetenzzellenbasierter Netze

Ackermann, Jörg

05 September 2007

Kompetenzzellenbasierte (regionale) Netze stellen besondere Anforderungen an die Modellierung, Planung und Gestaltung der Logistikstrukturen. Für die Logistikstrukturmodellierung werden ein generischer Beschreibungsrahmen für produktionslogistische soziotechnische Systeme, Definitionen u.a. zum zentralen Begriff Logistikstruktur sowie ein 3-Ebenen-Modell und Strukturtypen für eine vertiefende Materialflussanalyse und -synthese bereitgestellt. Für die Logistikstrukturplanung wird darauf aufbauend mit der Methode der Integrativen Prozess- und Systemstrukturierung (IPSS) eine Methode zur Behandlung von Strukturierungsproblemen konzipiert, die sowohl speziell für kompetenzzellenbasierte Netze als auch allgemein für Produktions- und Logistiksysteme angewandt werden kann. Für die Logistikstrukturgestaltung werden unter Modell- und Methodenverwendung Szenarien sowie Gestaltungs- und Vorzugslösungen für den Materialfluss abgeleitet. / Competence-cell based (regional) networks put special requirements on the modelling, planning and design of logistics structures. For the modelling of logistics structures, a generic description framework for production logistic sociotechnical systems, definitions for, amongst others, the central term logistics structure as well as a 3-layer-model and structure types for a more detailed material flow analysis and synthesis are provided. For the planning of logistics structures, the Method of Integrative Process and System Structuring (IPSS) is developed as a method for handling structuring problems. It can be applied especially to Competence-cell based networks as well as generally to production and logistics systems. For the design of logistics structures, scenarios as well as design and preference solutions for the material flow are derived.

info:eu-repo/classification/ddc/620

ddc:620

Gestaltung

Logistik

Logistiksystem

Materialfluss

Modellierung

Planung

Produktion

Produktionssystem

Strukturierung

3-Ebenen-Modell

3-Layer-Model

Competence-cell Based Network

Design

IPSS

Kompetenzzellenbasiertes Netz

Logistics

Logistics Network

Logistics Structure

Logistics System

Logistiknetz

Logistikstruktur

Material Flow

Modelling

Planning

Production

Production Network

Production System

Produktionsnetz

Structure Type

Structuring

Strukturtyp