Publications by authors named "Griffin Spychalski"

Article Synopsis
  • Isolating specific subpopulations of extracellular vesicles (EVs) is challenging due to their small size, varying surface markers, and the high number of background EVs in samples like blood.
  • The use of track etched magnetic nanopore (TENPO) chips offers a solution with improved sorting precision and resistance to clogging, but there has been no detailed study on optimizing design parameters for efficiency.
  • By combining simulations and experiments, researchers identified key design factors, enhancing the ability to isolate target EVs while significantly reducing background noise, confirming the method's effectiveness across various cancer models.
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The isolation of specific subpopulations of extracellular vesicles (EVs) based on their expression of surface markers poses a significant challenge due to their nanoscale size (< 800 nm), their heterogeneous surface marker expression, and the vast number of background EVs present in clinical specimens (10 -10 EVs/mL in blood). Highly parallelized nanomagnetic sorting using track etched magnetic nanopore (TENPO) chips has achieved precise immunospecific sorting with high throughput and resilience to clogging. However, there has not yet been a systematic study of the design parameters that control the trade-offs in throughput, target EV recovery, and specificity in this approach.

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Article Synopsis
  • Sphingosine-1-phosphate (S1P) is crucial for maintaining the barrier function of endothelial cells, especially under different flow conditions in blood vessels.
  • Researchers used a microfluidic system to simulate the flow dynamics at vessel bifurcations, finding that specific hemodynamic forces improve the stability of endothelial barriers when combined with S1P.
  • The study highlights that the protective effects of these fluid forces on endothelial cells depend on S1P receptor signaling and emphasizes the importance of understanding how blood flow interacts with vascular health.
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Sprouting angiogenesis-the infiltration and extension of endothelial cells from pre-existing blood vessels-helps orchestrate vascular growth and remodeling. It is now agreed that fluid forces, such as laminar shear stress due to unidirectional flow in straight vessel segments, are important regulators of angiogenesis. However, regulation of angiogenesis by the different flow dynamics that arise due to vessel branching, such as impinging flow stagnation at the base of a bifurcating vessel, are not well understood.

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Endothelial barrier function is known to be regulated by a number of molecular mechanisms; however, the role of biomechanical signals associated with blood flow is comparatively less explored. Biomimetic microfluidic models comprised of vessel analogues that are lined with endothelial cells (ECs) have been developed to help answer several fundamental questions in endothelial mechanobiology. However, previously described microfluidic models have been primarily restricted to single straight or two parallel vessel analogues, which do not model the bifurcating vessel networks typically present in physiology.

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Surface wrinkles formed by the buckling of a strained stiff layer attached to a soft elastomer foundation have been widely used in a variety of applications. Micropatterning of wrinkled topographies is, however, limited by process/system complexities. In this article, we report an approach to write surface wrinkles with desired pattern geometries on poly(dimethylsiloxane) (PDMS) elastomers using a commercial infrared laser engraver with a spot size of 127 μm.

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Microfluidic systems have emerged as a new class of perfusable in vitro culture models that have helped advance and refine our understanding of microvascular function. Cutting-edge microfluidic models have successfully integrated principles from quantitative analysis of vascular function, in vitro flow chambers, microfabrication techniques, and 3D tissue scaffolds. Here, we review the evolution of microfluidic systems, namely their progression from 2D planar microchannel arrays to 3D microtissue analogs, and highlight their recent contributions in elucidating the role of biomolecular transport and fluid mechanical stimuli in controlling angiogenesis.

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