Microfluidic tumor-on-a-chip model to evaluate the role of tumor environmental stress on NK cell exhaustion

Ayuso, Jesús Manso; Rehman, Shujah; Virumbrales-Muñoz, María; McMinn, Patrick H.; Geiger, Peter; Fitzgerald, Cate M.; Heaster, Tiffany M.; Skala, Melissa C.; Beebe, David J.

doi:10.1126/sciadv.abc2331

Cited by 97 publications

(79 citation statements)

References 53 publications

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“…More recently, the same group adapted the microfluidic set-up to investigate NK exhaustion due to tumour environmental stresses reproduced on-a-chip. 59 The device design allowed to control nutrient and pH gradients across 3D tumour models, as well as inducing cell proliferation and necrosis. Gene expression analysis showed greater exhaustion of the NK cells cultured in devices in comparison to those in well plates.…”

Section: Microfluidics For Solid Tumour Immunotherapiesmentioning

confidence: 99%

Microfluidic technologies for immunotherapy studies on solid tumours

et al. 2021

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Section: Microfluidics For Solid Tumour Immunotherapiesmentioning

confidence: 99%

Microfluidic technologies for immunotherapy studies on solid tumours

et al. 2021

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“…The migration of NK.92 NK cells in RGD-modified and MMP-degradable PEG gels was shown to be impaired in the presence of H1299 cancer lines that secreted anti-inflammatory TGF-β. 58 A more complex tumor on a chip model was developed that co-cultured NK.92 cells with MCF7 breast cancer cells in the presence of a endothelial cell-lined lumen; the cancer cells provided an immunosuppressive environment to the NK cells that diminished their cytotoxicity and resulted in their exhaustion, even after removal from the device 59 (Figure 4(a)).…”

Section: Microphysiological Systems For Characterizing Manufactured Cellsmentioning

confidence: 99%

Engineering microenvironments for manufacturing therapeutic cells

Kwee

Sung

2021

Exp Biol Med (Maywood)

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There are a growing number of globally approved products and clinical trials utilizing autologous and allogeneic therapeutic cells for applications in regenerative medicine and immunotherapies. However, there is a need to develop rapid and cost-effective methods for manufacturing therapeutically effective cells. Furthermore, the resulting manufactured cells may exhibit heterogeneities that result in mixed therapeutic outcomes. Engineering approaches that can provide distinct microenvironmental cues to these cells may be able to enhance the growth and characterization of these cell products. This mini-review describes strategies to potentially enhance the expansion of therapeutic cells with biomaterials and bioreactors, as well as to characterize the cell products with microphysiological systems. These systems can provide distinct cues to maintain the quality attributes of the cells and evaluate their function in physiologically relevant conditions.

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“…The cell cytoplasm was defined as the cell borders minus the nucleus. Values for NAD(P)H lifetime variables (𝜏𝜏 𝑚𝑚 , 𝜏𝜏 1 , 𝜏𝜏 2 , 𝛼𝛼 1 , 𝛼𝛼 2 ), FAD lifetime variables, NAD(P)H intensity, and FAD intensity were averaged for all pixels within the cytoplasm of each cell, as described previously 14,55,56 .…”

Section: Two-photon Optical Metabolic Imaging (Omi) Acquisition and Analysismentioning

confidence: 99%

“…Fluorescence intensity measurements are influenced by laser power, detector gain, light scattering, and the concentration of the fluorophore; however, fluorescence lifetimes are independent of these experimental factors 57,59 . Although the FLIRR is a useful measurement of cellular metabolism, it is not a substitute for the optical redox ratio and instead represents an additional variable to compare metabolic endpoints 55 . Hierarchical cluster analysis of OMI parameters was completed using group average cluster methods defined using Euclidean distant type (OriginPro 2020).…”

Section: Two-photon Optical Metabolic Imaging (Omi) Acquisition and Analysismentioning

confidence: 99%

Integrating Subclonal Response Heterogeneity to Define Cancer Organoid Therapeutic Sensitivity

Kratz

Rehman

Johnson

et al. 2021

Preprint

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Tumor heterogeneity is predicted to confer inferior clinical outcomes, however modeling heterogeneity in a manner that still represents the tumor of origin remains a formidable challenge. Sequencing technologies are limited in their ability to identify rare subclonal populations and predict response to the multitude of available treatments for patients. Patient-derived organotypic cultures have significantly improved the modeling of cancer biology by faithfully representing the molecular features of primary malignant tissues. Patient-derived cancer organoid (PCO) cultures contain numerous individual organoids with the potential to recapitulate heterogeneity, though PCOs are most commonly studied in bulk ignoring any diversity in the molecular profile or treatment response. Here we demonstrate the advantage of evaluating individual PCOs in conjunction with cellular level optical metabolic imaging to characterize the largely ignored heterogeneity within these cultures to predict clinical therapeutic response, identify subclonal populations, and determine patient specific mechanisms of resistance.

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Microfluidic tumor-on-a-chip model to evaluate the role of tumor environmental stress on NK cell exhaustion

Cited by 97 publications

References 53 publications

Microfluidic technologies for immunotherapy studies on solid tumours

Microfluidic technologies for immunotherapy studies on solid tumours

Engineering microenvironments for manufacturing therapeutic cells

Integrating Subclonal Response Heterogeneity to Define Cancer Organoid Therapeutic Sensitivity

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