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Biomimetics of the pulmonary environment in vitro: A microfluidics perspective

The entire luminal surface of the lungs is populated with a complex yet confluent, uninterrupted airway epithelium in conjunction with an extracellular liquid lining layer that creates the air-liquid interface (ALI), a critical feature of healthy lungs. Motivated by lung disease modelling, cytotoxic...

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Autores principales: Tenenbaum-Katan, Janna, Artzy-Schnirman, Arbel, Fishler, Rami, Korin, Netanel, Sznitman, Josué
Formato: Online Artículo Texto
Lenguaje:English
Publicado: AIP Publishing LLC 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5973897/
https://www.ncbi.nlm.nih.gov/pubmed/29887933
http://dx.doi.org/10.1063/1.5023034
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author Tenenbaum-Katan, Janna
Artzy-Schnirman, Arbel
Fishler, Rami
Korin, Netanel
Sznitman, Josué
author_facet Tenenbaum-Katan, Janna
Artzy-Schnirman, Arbel
Fishler, Rami
Korin, Netanel
Sznitman, Josué
author_sort Tenenbaum-Katan, Janna
collection PubMed
description The entire luminal surface of the lungs is populated with a complex yet confluent, uninterrupted airway epithelium in conjunction with an extracellular liquid lining layer that creates the air-liquid interface (ALI), a critical feature of healthy lungs. Motivated by lung disease modelling, cytotoxicity studies, and drug delivery assessments amongst other, in vitro setups have been traditionally conducted using macroscopic cultures of isolated airway cells under submerged conditions or instead using transwell inserts with permeable membranes to model the ALI architecture. Yet, such strategies continue to fall short of delivering a sufficiently realistic physiological in vitro airway environment that cohesively integrates at true-scale three essential pillars: morphological constraints (i.e., airway anatomy), physiological conditions (e.g., respiratory airflows), and biological functionality (e.g., cellular makeup). With the advent of microfluidic lung-on-chips, there have been tremendous efforts towards designing biomimetic airway models of the epithelial barrier, including the ALI, and leveraging such in vitro scaffolds as a gateway for pulmonary disease modelling and drug screening assays. Here, we review in vitro platforms mimicking the pulmonary environment and identify ongoing challenges in reconstituting accurate biological airway barriers that still widely prevent microfluidic systems from delivering mainstream assays for the end-user, as compared to macroscale in vitro cell cultures. We further discuss existing hurdles in scaling up current lung-on-chip designs, from single airway models to more physiologically realistic airway environments that are anticipated to deliver increasingly meaningful whole-organ functions, with an outlook on translational and precision medicine.
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spelling pubmed-59738972018-06-10 Biomimetics of the pulmonary environment in vitro: A microfluidics perspective Tenenbaum-Katan, Janna Artzy-Schnirman, Arbel Fishler, Rami Korin, Netanel Sznitman, Josué Biomicrofluidics SPECIAL TOPIC: BIO-TRANSPORT PROCESSES AND DRUG DELIVERY IN PHYSIOLOGICAL MICRO-DEVICES The entire luminal surface of the lungs is populated with a complex yet confluent, uninterrupted airway epithelium in conjunction with an extracellular liquid lining layer that creates the air-liquid interface (ALI), a critical feature of healthy lungs. Motivated by lung disease modelling, cytotoxicity studies, and drug delivery assessments amongst other, in vitro setups have been traditionally conducted using macroscopic cultures of isolated airway cells under submerged conditions or instead using transwell inserts with permeable membranes to model the ALI architecture. Yet, such strategies continue to fall short of delivering a sufficiently realistic physiological in vitro airway environment that cohesively integrates at true-scale three essential pillars: morphological constraints (i.e., airway anatomy), physiological conditions (e.g., respiratory airflows), and biological functionality (e.g., cellular makeup). With the advent of microfluidic lung-on-chips, there have been tremendous efforts towards designing biomimetic airway models of the epithelial barrier, including the ALI, and leveraging such in vitro scaffolds as a gateway for pulmonary disease modelling and drug screening assays. Here, we review in vitro platforms mimicking the pulmonary environment and identify ongoing challenges in reconstituting accurate biological airway barriers that still widely prevent microfluidic systems from delivering mainstream assays for the end-user, as compared to macroscale in vitro cell cultures. We further discuss existing hurdles in scaling up current lung-on-chip designs, from single airway models to more physiologically realistic airway environments that are anticipated to deliver increasingly meaningful whole-organ functions, with an outlook on translational and precision medicine. AIP Publishing LLC 2018-05-29 /pmc/articles/PMC5973897/ /pubmed/29887933 http://dx.doi.org/10.1063/1.5023034 Text en © 2018 Author(s). 1932-1058/2018/12(4)/042209/18 All article content, except where otherwise noted, is licensed under a Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle SPECIAL TOPIC: BIO-TRANSPORT PROCESSES AND DRUG DELIVERY IN PHYSIOLOGICAL MICRO-DEVICES
Tenenbaum-Katan, Janna
Artzy-Schnirman, Arbel
Fishler, Rami
Korin, Netanel
Sznitman, Josué
Biomimetics of the pulmonary environment in vitro: A microfluidics perspective
title Biomimetics of the pulmonary environment in vitro: A microfluidics perspective
title_full Biomimetics of the pulmonary environment in vitro: A microfluidics perspective
title_fullStr Biomimetics of the pulmonary environment in vitro: A microfluidics perspective
title_full_unstemmed Biomimetics of the pulmonary environment in vitro: A microfluidics perspective
title_short Biomimetics of the pulmonary environment in vitro: A microfluidics perspective
title_sort biomimetics of the pulmonary environment in vitro: a microfluidics perspective
topic SPECIAL TOPIC: BIO-TRANSPORT PROCESSES AND DRUG DELIVERY IN PHYSIOLOGICAL MICRO-DEVICES
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5973897/
https://www.ncbi.nlm.nih.gov/pubmed/29887933
http://dx.doi.org/10.1063/1.5023034
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