4.8 Article

Hydrogels Containing Gradients in Vascular Density Reveal Dose-Dependent Role of Angiocrine Cues on Stem Cell Behavior

Journal

ADVANCED FUNCTIONAL MATERIALS
Volume 31, Issue 51, Pages -

Publisher

WILEY-V C H VERLAG GMBH
DOI: 10.1002/adfm.202101541

Keywords

gradients; hydrogels; microfluidics; patterning; stem cells; vascularization

Funding

  1. NIH [R01 CA197488, F31 DK117514, T32 EB019944, R01 DK099528, R21 EB01848]
  2. NSF [GRFP DGE-1144245]
  3. Department of Chemical & Biomolecular Engineering at the University of Illinois at Urbana-Champaign
  4. Illinois Scholars Undergraduate Research Program at the University of Illinois at Urbana-Champaign
  5. Carl R. Woese Institute for Genomic Biology at the University of Illinois at Urbana-Champaign

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Biomaterials mimicking microenvironmental signals from the stem cell niche could improve platforms regulating stem cell behavior. Vascular-derived signals offer an important alternative signaling axis, but dose-dependent relationships between angiocrine signals and stem cell fate are difficult to determine in animal models and 2D cell cultures. This study uses microfluidic devices to create 3D hydrogels with lateral gradients in vascular density, revealing spatial patterns of HSC phenotype in response to angiocrine signals and showcasing the influence of local angiocrine signals on HSC fate.
Biomaterials that replicate patterns of microenvironmental signals from the stem cell niche offer the potential to refine platforms to regulate stem cell behavior. While significant emphasis has been placed on understanding the effects of biophysical and biochemical cues on stem cell fate, vascular-derived or angiocrine cues offer an important alternative signaling axis for biomaterial-based stem cell platforms. Elucidating dose-dependent relationships between angiocrine cues and stem cell fate are largely intractable in animal models and 2D cell cultures. In this study, microfluidic mixing devices are leveraged to generate 3D hydrogels containing lateral gradients in vascular density alongside murine hematopoietic stem cells (HSCs). Regional differences in vascular density can be generated via embossed gradients in cell, matrix, or growth factor density. HSCs co-cultured alongside vascular gradients reveal spatial patterns of HSC phenotype in response to angiocrine signals. Notably, decreased Akt signaling in high vessel density regions led to increased expansion of lineage-positive hematopoietic cells. This approach offers a combinatorial tool to rapidly screen a continuum of microenvironments with varying vascular, biophysical, and biochemical cues to reveal the influence of local angiocrine signals on HSC fate.

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