Assessment of Cell Viability in Three-Dimensional Scaffolds Using Cellular Auto-Fluorescence

Dittmar, R Roman; Potier, Esther; Zandvoort, M Marc van; Ito, Keita

doi:10.1089/ten.tec.2011.0334

Cited by 53 publications

(42 citation statements)

References 39 publications

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“…4A-B ). Of note, at day 10, non-infected (mock) islet cells emit low levels of fluorescent, indicative of auto-fluorescence produced by apoptotic cells [37]. Consistent with this premise, islet architecture was strongly compromised at day 10 with signs of necrosis as compared to islets 4 days post infection (Fig.…”

Section: Resultssupporting

confidence: 55%

A Simple High Efficiency Intra-Islet Transduction Protocol Using Lentiviral Vectors

Jiménez-Moreno¹,

Herrera-Gómez²,

López-Noriega³

et al. 2015

CGT

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Successful normalization of blood glucose in patients transplanted with pancreatic islets isolated from cadaveric donors established the proof-of-concept that Type 1 Diabetes Mellitus is a curable disease. Nonetheless, major caveats to the widespread use of this cell therapy approach have been the shortage of islets combined with the low viability and functional rates subsequent to transplantation. Gene therapy targeted to enhance survival and performance prior to transplantation could offer a feasible approach to circumvent these issues and sustain a durable functional β-cell mass in vivo. However, efficient and safe delivery of nucleic acids to intact islet remains a challenging task. Here we describe a simple and easy-to-use lentiviral transduction protocol that allows the transduction of approximately 80% of mouse and human islet cells while preserving islet architecture, metabolic function and glucose-dependent stimulation of insulin secretion. Our protocol will facilitate to fully determine the potential of gene expression modulation of therapeutically promising targets in entire pancreatic islets for xenotransplantation purposes.

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Section: Resultssupporting

confidence: 55%

A Simple High Efficiency Intra-Islet Transduction Protocol Using Lentiviral Vectors

Jiménez-Moreno¹,

Herrera-Gómez²,

López-Noriega³

et al. 2015

CGT

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“…Therefore, the development of reliable, label-free technologies that allow real-time, non-invasive assessment on the tissue, cellular, and molecular levels is required to provide a more complete and accurate description of construct viability both in vitro and in situ . Nonlinear optical molecular imaging with quantitative analysis provides a rapid, non-destructive, non-invasive, objective, label-free, and spatially-resolved assessment of tissue-engineered construct viability [25–29]. The constructs employed here, EVPOMEs, contained multiple endogenous sources of molecular optical contrast (including keratin, NAD(P)H, FAD, and collagen) that provided cellular and extracellular information on tissue morphology and function for viability assessments.…”

Section: Discussionmentioning

confidence: 99%

The potential of label-free nonlinear optical molecular microscopy to non-invasively characterize the viability of engineered human tissue constructs

et al. 2014

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Nonlinear optical molecular imaging and quantitative analytic methods were developed to non-invasively assess the viability of tissue-engineered constructs manufactured from primary human cells. Label-free optical measures of local tissue structure and biochemistry characterized morphologic and functional differences between controls and stressed constructs. Rigorous statistical analysis accounted for variability between human patients. Fluorescence intensity-based spatial assessment and metabolic sensing differentiated controls from thermally-stressed and from metabolically-stressed constructs. Fluorescence lifetime-based sensing differentiated controls from thermally-stressed constructs. Unlike traditional histological (found to be generally reliable, but destructive) and biochemical (non-invasive, but found to be unreliable) tissue analyses, label-free optical assessments had the advantages of being both non-invasive and reliable. Thus, such optical measures could serve as reliable manufacturing release criteria for cell-based tissue-engineered constructs prior to human implantation, thereby addressing a critical regulatory need in regenerative medicine.

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“…mitochondria, lysosomes or ribosomes), very often, the ECM can be imaged as well, for example elastin rsif.royalsocietypublishing.org J R Soc Interface 10: 20130263 fibres [63]. In a study by Dittmar et al [110], two-photon AF was used to assess cell viability which is an important parameter in TE to evaluate the effect of environmental conditions on cell behaviour. Live and dead cells could be distinguished spectrally, and viable cells showed predominantly blue fluorescence ( peak emission around 470 nm), whereas dead cells appeared to mainly emit green fluorescent light (approx.…”

Section: Autofluorescence Imagingmentioning

confidence: 99%

Taking a deep look: modern microscopy technologies to optimize the design and functionality of biocompatible scaffolds for tissue engineering in regenerative medicine

Vielreicher

Schürmann

Detsch

et al. 2013

J. R. Soc. Interface.

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This review focuses on modern nonlinear optical microscopy (NLOM) methods that are increasingly being used in the field of tissue engineering (TE) to image tissue non-invasively and without labelling in depths unreached by conventional microscopy techniques. With NLOM techniques, biomaterial matrices, cultured cells and their produced extracellular matrix may be visualized with high resolution. After introducing classical imaging methodologies such as µCT, MRI, optical coherence tomography, electron microscopy and conventional microscopy two-photon fluorescence (2-PF) and second harmonic generation (SHG) imaging are described in detail (principle, power, limitations) together with their most widely used TE applications. Besides our own cell encapsulation, cell printing and collagen scaffolding systems and their NLOM imaging the most current research articles will be reviewed. These cover imaging of autofluorescence and fluorescence-labelled tissue and biomaterial structures, SHG-based quantitative morphometry of collagen I and other proteins, imaging of vascularization and online monitoring techniques in TE. Finally, some insight is given into state-of-the-art three-photon-based imaging methods (e.g. coherent anti-Stokes Raman scattering, third harmonic generation). This review provides an overview of the powerful and constantly evolving field of multiphoton microscopy, which is a powerful and indispensable tool for the development of artificial tissues in regenerative medicine and which is likely to gain importance also as a means for general diagnostic medical imaging.

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Assessment of Cell Viability in Three-Dimensional Scaffolds Using Cellular Auto-Fluorescence

Cited by 53 publications

References 39 publications

A Simple High Efficiency Intra-Islet Transduction Protocol Using Lentiviral Vectors

A Simple High Efficiency Intra-Islet Transduction Protocol Using Lentiviral Vectors

The potential of label-free nonlinear optical molecular microscopy to non-invasively characterize the viability of engineered human tissue constructs

Taking a deep look: modern microscopy technologies to optimize the design and functionality of biocompatible scaffolds for tissue engineering in regenerative medicine

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