Literature DB >> 35284602

Investigation of Microvesicle Uptake by Mouse Lung-marginated Monocytes in vitro.

Ying Ying Tan1, Kieran P O'Dea1, Brijesh V Patel1, Masao Takata1.   

Abstract

Extracellular microvesicles (MVs) are released into the circulation in large numbers during acute systemic inflammation, yet little is known of their intravascular cell/tissue-specific interactions under these conditions. We recently described a dramatic increase in the uptake of intravenously injected MVs by monocytes marginated within the pulmonary vasculature, in a mouse model of low-dose lipopolysaccharide-induced systemic inflammation. To investigate the mechanisms of enhanced MV uptake by monocytes, we developed an in vitro model using in vivo derived monocytes. Although mouse blood is a convenient source, monocyte numbers are too low for in vitro experimentation. In contrast, differentiated bone marrow monocytes are abundant, but they are rapidly mobilized during systemic inflammation, and thus no longer available. Instead, we developed a protocol using marginated monocytes from the pulmonary vasculature as an anatomically relevant and abundant source. Mice are sacrificed by terminal anesthesia, the lungs inflated and perfused via the pulmonary artery. Perfusate cell populations are evaluated by flow cytometry, combined with in vitro generated fluorescently labelled MVs, and incubated in suspension for up to one hour. Washed cells are analyzed by flow cytometry to quantify MV uptake and confocal microscopy to localize MVs within cells (O'Dea et al., 2020). Using this perfusion-based method, substantial numbers of marginated pulmonary vascular monocytes are recovered, allowing multiple in vitro tests to be performed from a single mouse donor. As MV uptake profiles were comparable to those observed in vivo, this method is suitable for physiologically relevant high throughput mechanistic studies on mouse monocytes under in vitro conditions. Graphic abstract: Figure 1. Schematic of lung perfusate cell harvest and co-incubation with in vitro generated MVs. Created with BioRender.com.
Copyright © 2022 The Authors; exclusive licensee Bio-protocol LLC.

Entities:  

Keywords:  Extracellular vesicles; Lungs; Microvesicles; Monocytes; Sepsis

Year:  2022        PMID: 35284602      PMCID: PMC8855083          DOI: 10.21769/BioProtoc.4307

Source DB:  PubMed          Journal:  Bio Protoc        ISSN: 2331-8325


  15 in total

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Journal:  Eur Surg Res       Date:  2002 Jan-Apr       Impact factor: 1.745

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Authors:  María Yáñez-Mó; Pia R-M Siljander; Zoraida Andreu; Apolonija Bedina Zavec; Francesc E Borràs; Edit I Buzas; Krisztina Buzas; Enriqueta Casal; Francesco Cappello; Joana Carvalho; Eva Colás; Anabela Cordeiro-da Silva; Stefano Fais; Juan M Falcon-Perez; Irene M Ghobrial; Bernd Giebel; Mario Gimona; Michael Graner; Ihsan Gursel; Mayda Gursel; Niels H H Heegaard; An Hendrix; Peter Kierulf; Katsutoshi Kokubun; Maja Kosanovic; Veronika Kralj-Iglic; Eva-Maria Krämer-Albers; Saara Laitinen; Cecilia Lässer; Thomas Lener; Erzsébet Ligeti; Aija Linē; Georg Lipps; Alicia Llorente; Jan Lötvall; Mateja Manček-Keber; Antonio Marcilla; Maria Mittelbrunn; Irina Nazarenko; Esther N M Nolte-'t Hoen; Tuula A Nyman; Lorraine O'Driscoll; Mireia Olivan; Carla Oliveira; Éva Pállinger; Hernando A Del Portillo; Jaume Reventós; Marina Rigau; Eva Rohde; Marei Sammar; Francisco Sánchez-Madrid; N Santarém; Katharina Schallmoser; Marie Stampe Ostenfeld; Willem Stoorvogel; Roman Stukelj; Susanne G Van der Grein; M Helena Vasconcelos; Marca H M Wauben; Olivier De Wever
Journal:  J Extracell Vesicles       Date:  2015-05-14

3.  Cellular origin and procoagulant properties of microparticles in meningococcal sepsis.

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Journal:  Sci Immunol       Date:  2017-04-28

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Authors:  D E Doherty; G S Worthen
Journal:  Chest       Date:  1994-03       Impact factor: 9.410

6.  CX3CR1-dependent endothelial margination modulates Ly6Chigh monocyte systemic deployment upon inflammation in mice.

Authors:  Pauline Hamon; Pierre-Louis Loyher; Camille Baudesson de Chanville; Fabrice Licata; Christophe Combadière; Alexandre Boissonnas
Journal:  Blood       Date:  2016-12-23       Impact factor: 22.113

7.  Liver Kupffer cells rapidly remove red blood cell-derived vesicles from the circulation by scavenger receptors.

Authors:  Frans L A Willekens; Jan M Werre; J Kar Kruijt; Bregt Roerdinkholder-Stoelwinder; Yvonne A M Groenen-Döpp; Annegeet G van den Bos; Giel J C G M Bosman; Theo J C van Berkel
Journal:  Blood       Date:  2004-11-18       Impact factor: 22.113

8.  Circulating Microvesicles Are Elevated Acutely following Major Burns Injury and Associated with Clinical Severity.

Authors:  Kieran P O'Dea; John R Porter; Nikhil Tirlapur; Umar Katbeh; Suveer Singh; Jonathan M Handy; Masao Takata
Journal:  PLoS One       Date:  2016-12-09       Impact factor: 3.240

9.  Monocytes mediate homing of circulating microvesicles to the pulmonary vasculature during low-grade systemic inflammation.

Authors:  Kieran P O'Dea; Ying Ying Tan; Sneh Shah; Brijesh V Patel; Kate C Tatham; Mike R Wilson; Sanooj Soni; Masao Takata
Journal:  J Extracell Vesicles       Date:  2020-01-05

10.  Mobilization and margination of bone marrow Gr-1high monocytes during subclinical endotoxemia predisposes the lungs toward acute injury.

Authors:  Kieran P O'Dea; Michael R Wilson; Justina O Dokpesi; Kenji Wakabayashi; Louise Tatton; Nico van Rooijen; Masao Takata
Journal:  J Immunol       Date:  2009-01-15       Impact factor: 5.422

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