Abstract

The vascular basement membrane—a thin, elastic layer of extracellular matrix separating and encasing vascular cells—provides biological and mechanical cues to endothelial cells, pericytes, and migrating leukocytes. In contrast, experimental scaffolds typically used to replicate basement membranes are stiff and bio-inert. Here, we present thin, porated polyethylene glycol hydrogels to replicate human vascular basement membranes. Like commercial transwells, our hydrogels are approximately 10μm thick, but like basement membranes, the hydrogels presented here are elastic (E: 50-80kPa) and contain a dense network of small pores. Moreover, the inclusion of bioactive domains introduces receptor-mediated biochemical signaling. We compare elastic hydrogels to common culture substrates (E: >2GPa) for human endothelial cell and pericyte monolayers and bilayers to replicate postcapillary venules in vitro. Our data demonstrate that substrate elasticity facilitates differences in vascular phenotype, supporting expression of vascular markers that are increasingly replicative of venules. Endothelial cells differentially express vascular markers, like EphB4, and leukocyte adhesion molecules, such as ICAM-1, with decreased mechanical stiffness. With porated PEG hydrogels we demonstrate the ability to evaluate and observe leukocyte recruitment across endothelial cell and pericyte monolayers and bilayers, reporting that basement membrane scaffolds can significantly alter the rate of vascular migration in experimental systems. Overall, this study demonstrates the creation and utility of a new and accessible method to recapture the mechanical and biological complexity of human basement membranes in vitro.

Highlights

  • The vascular basement membrane (BM) is a highly specialized layer of extracellular matrix in the sub-endothelial space

  • This study, and the use and attainment of human cells were approved by Yale University and its Human Investigation Committee (HIC) of the Institutional Review Board (IRB) as part of the Human Research Protection Program

  • All advertisements for volunteers were approved by the Yale University HIC IRB protocol # 0902004786 and written informed consent was obtained from all human volunteers prior to blood collection

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Summary

Introduction

The vascular basement membrane (BM) is a highly specialized layer of extracellular matrix in the sub-endothelial space. The BM plays two critical roles: it provides a structural scaffold for resident vascular cells and provides localized mechanical and biological signals to resident and migrating cells. In its role as a scaffold, endothelial cells (ECs) adhere to the luminal face of the BM, whereas perivascular pericytes (PCs) are located in the abluminal portion of the vessel. The BM ranges in thickness from 50 to 300nm; ECs and PCs utilize the pores or voids within the BM to make contact with one another [1]. Collagen IV, laminin-8, and laminin-10 are PLOS ONE | DOI:10.1371/journal.pone.0171386. Collagen IV, laminin-8, and laminin-10 are PLOS ONE | DOI:10.1371/journal.pone.0171386 February 24, 2017

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