Differential Monocyte Actuation in a Three‐Organ Functional Innate Immune System‐on‐a‐Chip

Sasserath, Trevor; Rumsey, John W.; McAleer, Christopher W.; Bridges, Lee; Long, Christopher J.; Elbrecht, Daniel; Schuler, Franz; Roth, Adrian; Bertinetti‐LaPatki, Christina; Shuler, Michael L.; Hickman, James J.

doi:10.1002/advs.202000323

Cited by 61 publications

(43 citation statements)

References 71 publications

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“…Although immune components such as macrophages have been included in a variety of single organ systems ( Huh et al, 2010 ; Jones et al, 2012 ; Hamza and Irimia, 2015 ), their integration in a recirculating multiorgan MPS device is not advancing as rapidly. A recent article by Sasserath et al (2020) presented the integration of a monocyte-derived cell line, THP-1, as a recirculating immune component in a multiorgan human model. The monocytes were added as part of the recirculating medium (blood surrogate) and allowed to flow through the three-organ system.…”

Section: Examples Of Mpsmentioning

confidence: 99%

Critical Considerations for the Design of Multi-Organ Microphysiological Systems (MPS)

Malik

Yang

Fathi

et al. 2021

Front. Cell Dev. Biol.

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Identification and approval of new drugs for use in patients requires extensive preclinical studies and clinical trials. Preclinical studies rely on in vitro experiments and animal models of human diseases. The transferability of drug toxicity and efficacy estimates to humans from animal models is being called into question. Subsequent clinical studies often reveal lower than expected efficacy and higher drug toxicity in humans than that seen in animal models. Microphysiological systems (MPS), sometimes called organ or human-on-chip models, present a potential alternative to animal-based models used for drug toxicity screening. This review discusses multi-organ MPS that can be used to model diseases and test the efficacy and safety of drug candidates. The translation of an in vivo environment to an in vitro system requires physiologically relevant organ scaling, vascular dimensions, and appropriate flow rates. Even small changes in those parameters can alter the outcome of experiments conducted with MPS. With many MPS devices being developed, we have outlined some established standards for designing MPS devices and described techniques to validate the devices. A physiologically realistic mimic of the human body can help determine the dose response and toxicity effects of a new drug candidate with higher predictive power.

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Section: Examples Of Mpsmentioning

confidence: 99%

Critical Considerations for the Design of Multi-Organ Microphysiological Systems (MPS)

Malik

Yang

Fathi

et al. 2021

Front. Cell Dev. Biol.

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“…Mononuclear phagocyte migration and its role in development and disease have been studied using OoC models (Biselli et al, 2017;Sasserath et al, 2020). Monocytes and macrophages embedded in OoCs respond to hypoxia and injury-associated signals, such as MCP-1 and IL-6, by migrating down chemokine gradients (Liu et al, 2018;Shanti et al, 2018).…”

Section: Organ-on-chip Systemsmentioning

confidence: 99%

“…These MPs express gene-expression programs similar to those observed to be crucial in development, such as programs involved in angiogenesis (VEGF, COX2, Wnt5a, FGF2), tissue remodeling (MMP9), glucose transport (e.g., solute carrier family 2 member 1), and glycolytic metabolism (enolase 2) (Chou et al, 2018;Shanti et al, 2018;Jang et al, 2019;Sriram et al, 2019). Other OoC models incorporating MPs have been developed for the spleen (Rigat-Brugarolas et al, 2014), skin (Sriram et al, 2019), bone marrow (Chou et al, 2018), liver (Jang et al, 2019), the feto-maternal interface (Richardson et al, 2020), and an inter-connected multi-organ platform (Sasserath et al, 2020). Sieber et al (2018) developed a BM-on-a-chip model consisting of two media perfused micro-channels filled with BM progenitor, stromal, and endothelial cells.…”

Section: Organ-on-chip Systemsmentioning

confidence: 99%

“…To achieve crosstalk of organs, long-term multi-OoC cultures have been developed to better mimic these multi-tissue interactions (Zhao et al, 2019). A multi-OoC model comprising cardiomyocytes, skeletal muscle, and the liver was successfully used to study the THP-1 macrophage response to drug and inflammatory stimuli (Sasserath et al, 2020). The multi-OoC model incorporated biological microelectromechanical systems (BioMEMS) to non-invasively measure cardiomyocyte electrical (microelectrode array) and muscle mechanical function (cantilever).…”

Section: Organ-on-chip Systemsmentioning

confidence: 99%

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Prenatal Development and Function of Human Mononuclear Phagocytes

Miah

Goh

Haniffa

2021

Front. Cell Dev. Biol.

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The human mononuclear phagocyte (MP) system, which includes dendritic cells, monocytes, and macrophages, is a critical regulator of innate and adaptive immune responses. During embryonic development, MPs derive sequentially in yolk sac progenitors, fetal liver, and bone marrow haematopoietic stem cells. MPs maintain tissue homeostasis and confer protective immunity in post-natal life. Recent evidence – primarily in animal models – highlight their critical role in coordinating the remodeling, maturation, and repair of target organs during embryonic and fetal development. However, the molecular regulation governing chemotaxis, homeostasis, and functional diversification of resident MP cells in their respective organ systems during development remains elusive. In this review, we summarize the current understanding of the development and functional contribution of tissue MPs during human organ development and morphogenesis and its relevance to regenerative medicine. We outline how single-cell multi-omic approaches and next-generation ex-vivo organ-on-chip models provide new experimental platforms to study the role of human MPs during development and disease.

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“…Sasserath et al [ 76 ] developed a three-OoC device consisting of the liver, cardiomyocytes and skeletal muscle, including the innate immune system, represented by circulating THP-1 monocytes. Its functionality was maintained for up to 28 days.…”

Section: Integration Of Immune Cells and Components For Organs-on-mentioning

confidence: 99%

Immune Organs and Immune Cells on a Chip: An Overview of Biomedical Applications

et al. 2020

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Understanding the immune system is of great importance for the development of drugs and the design of medical implants. Traditionally, two-dimensional static cultures have been used to investigate the immune system in vitro, while animal models have been used to study the immune system’s function and behavior in vivo. However, these conventional models do not fully emulate the complexity of the human immune system or the human in vivo microenvironment. Consequently, many promising preclinical findings have not been reproduced in human clinical trials. Organ-on-a-chip platforms can provide a solution to bridge this gap by offering human micro-(patho)physiological systems in which the immune system can be studied. This review provides an overview of the existing immune-organs-on-a-chip platforms, with a special emphasis on interorgan communication. In addition, future challenges to develop a comprehensive immune system-on-chip model are discussed.

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Differential Monocyte Actuation in a Three‐Organ Functional Innate Immune System‐on‐a‐Chip

Cited by 61 publications

References 71 publications

Critical Considerations for the Design of Multi-Organ Microphysiological Systems (MPS)

Critical Considerations for the Design of Multi-Organ Microphysiological Systems (MPS)

Prenatal Development and Function of Human Mononuclear Phagocytes

Immune Organs and Immune Cells on a Chip: An Overview of Biomedical Applications

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