2021
DOI: 10.1101/2021.08.08.455559
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Autologous human immunocompetent white adipose tissue-on-chip

Abstract: Obesity and associated diseases, such as diabetes, have reached epidemic proportions globally. In the era of 'diabesity' and due to its central role for metabolic and endocrine processes, adipose tissue (specifically white adipose tissue; WAT) has become a target of high interest for therapeutic strategies. To gain insights in cellular and molecular mechanisms of adipose (patho-)physiology, researchers traditionally relied on animal models since in vitro studies on human WAT are challenging due to the large si… Show more

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Cited by 2 publications
(7 citation statements)
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“…The group later published an improved version of this bottom-up approach in a system that integrates autologous mature adipocytes, ECs, and AT macrophages (figures 9(C) and (D)) [334]. This system recapitulates WAT functions such as energy storage and release as well as endocrine and immunomodulatory activities.…”
Section: Microfluidics and At On-a-chipmentioning
confidence: 99%
“…The group later published an improved version of this bottom-up approach in a system that integrates autologous mature adipocytes, ECs, and AT macrophages (figures 9(C) and (D)) [334]. This system recapitulates WAT functions such as energy storage and release as well as endocrine and immunomodulatory activities.…”
Section: Microfluidics and At On-a-chipmentioning
confidence: 99%
“…The tumor-on-chip consists of two stacked microfluidic channels separated by an isoporous, semipermeable polyethylene terephthalate (PET) membrane (5 µm poresize: r P \=\5\µm; ρ P \=\6\×\10 5 pores per cm 2 ; TRAKETCH® PET 5.0 p S210\×\300, SABEU GmbH & Co. KG, Northeim, Germany), which was functionalized by a plasma-enhanced, chemical vapor deposition (PECVD) process as previously described 40 . The tumor chambers (1 mm in diameter, 0.3 mm in height, six chambers per chip) branch off a main injection channel (0.2 mm in height) at a 45° angle and a highresistance channel towards the outlet port, which forces the aggregates/organoids to sequentially enter the tumor chambers during the injection process, utilizing an injection mechanism previously successfully established in other organ-on-chip model 11 . This concept and design enable the integration of any aggregate/organoid below 0.2 mm in size.…”
Section: Tumor Chip Concept Design and Fabricationmentioning
confidence: 99%
“…This ensures the placement of the cells into the tumor chambers during the injection instead of flowing out towards the outlet. The media channel is situated right above the tumor chambers and is separated by a porous PET membrane that serves multiple functions: during the cell injection step, it enables the entrapment of the tumor aggregates/PDOs and provides a growth surface for the endothelial barrier formation, whereas during the culture period, its 5 µm pore size allows T cell trafficking and passive diffusion of diluted species 11 .…”
Section: Tumor Chip Concept Design and Fabricationmentioning
confidence: 99%
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