microphysiological systems
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2022 ◽  
Vol 0 (0) ◽  
Author(s):  
Alla B. Salmina ◽  
Natalia A. Malinovskaya ◽  
Andrey V. Morgun ◽  
Elena D. Khilazheva ◽  
Yulia A. Uspenskaya ◽  
...  

Abstract The current prevalence of neurodevelopmental, neurodegenerative diseases, stroke and brain injury stimulates studies aimed to identify new molecular targets, to select the drug candidates, to complete the whole set of preclinical and clinical trials, and to implement new drugs into routine neurological practice. Establishment of protocols based on microfluidics, blood–brain barrier- or neurovascular unit-on-chip, and microphysiological systems allowed improving the barrier characteristics and analyzing the regulation of local microcirculation, angiogenesis, and neurogenesis. Reconstruction of key mechanisms of brain development and even some aspects of experience-driven brain plasticity would be helpful in the establishment of brain in vitro models with the highest degree of reliability. Activity, metabolic status and expression pattern of cells within the models can be effectively assessed with the protocols of system biology, cell imaging, and functional cell analysis. The next generation of in vitro models should demonstrate high scalability, 3D or 4D complexity, possibility to be combined with other tissues or cell types within the microphysiological systems, compatibility with bio-inks or extracellular matrix-like materials, achievement of adequate vascularization, patient-specific characteristics, and opportunity to provide high-content screening. In this review, we will focus on currently available and prospective brain tissue in vitro models suitable for experimental and preclinical studies with the special focus on models enabling 4D reconstruction of brain tissue for the assessment of brain development, brain plasticity, and drug kinetics.


2021 ◽  
Author(s):  
Clement Quintard ◽  
Emily Tubbs ◽  
Jean-Luc Achard ◽  
Fabrice Navarro ◽  
Xavier Gidrol ◽  
...  

Advances in microphysiological systems have prompted the need for robust and reliable cell culture devices. While microfluidic technology has made significant progress, devices often lack user-friendliness and are not designed to be industrialized on a large scale. Pancreatic islets are often being studied using microfluidic platforms in which the monitoring of fluxes is generally very limited, especially because the integration of valves to direct the flow is difficult to achieve. Considering these constraints, we present a thermoplastic manufactured microfluidic chip with an automated control of fluxes for the stimulation and secretion collection of pancreatic islet. The islet was directed toward precise locations through passive hydrodynamic trapping and both dynamic glucose stimulation and insulin harvesting were done automatically via a network of large deformation valves, directing the reagents and the pancreatic islet toward different pathways. This device we developed enables monitoring of insulin secretion from a single islet and can be adapted for the study of a wide variety of biological tissues and secretomes.


Small ◽  
2021 ◽  
pp. 2103157
Author(s):  
Lin Qi ◽  
Peter‐James H. Zushin ◽  
Ching‐Fang Chang ◽  
Yue Tung Lee ◽  
Diana L. Alba ◽  
...  

Science ◽  
2021 ◽  
Vol 373 (6561) ◽  
pp. 1304-1306
Author(s):  
Adrian Roth ◽  

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