Utilization of an Artery‐on‐a‐Chip to Unravel Novel Regulators and Therapeutic Targets in Vascular Diseases

Author:

Paloschi Valentina12ORCID,Pauli Jessica12,Winski Greg3,Wu Zhiyuan14,Li Zhaolong1,Botti Lorenzo5,Meucci Sandro6,Conti Pierangelo5,Rogowitz Felix7,Glukha Nadiya1,Hummel Nora1,Busch Albert18,Chernogubova Ekaterina3,Jin Hong3,Sachs Nadja1,Eckstein Hans‐Henning1,Dueck Anne29,Boon Reinier A.101112,Bausch Andreas R.13,Maegdefessel Lars123

Affiliation:

1. Department for Vascular and Endovascular Surgery Technical University of Munich 80333 Munich Germany

2. German Center for Cardiovascular Research DZHK Partner Site Munich Heart Alliance 80336 Berlin Germany

3. Department of Medicine, Cardiovascular Unit Karolinska Institute 171 77 Stockholm Sweden

4. Department of Vascular Surgery Beijing Hospital National Center of Gerontology Institute of Geriatric Medicine Chinese Academy of Medical Science Beijing 10073 P. R. China

5. Department of Engineering and Applied Sciences University of Bergamo Bergamo 24129 Italy

6. Micronit Microtechnologies Enschede 15 7521 The Netherlands

7. FLUIGENT Deutschland GmbH 07743 Jena Germany

8. Division of Vascular and Endovascular Surgery Department for Visceral Thoracic and Vascular Surgery Medical Faculty Carl Gustav Carus and University Hospital Technical University Dresden 01069 Dresden Germany

9. Institute of Pharmacology and Toxicology Technical University of Munich 80333 Munich Germany

10. Department of Physiology Amsterdam Cardiovascular Sciences (ACS) Amsterdam UMC VU University Medical Center Amsterdam 1081 HV The Netherlands

11. Institute of Cardiovascular Regeneration Center of Molecular Medicine Goethe‐University 60323 Frankfurt Germany

12. German Center for Cardiovascular Research DZHK Partner Site Frankfurt Rhine‐Main 10785 Berlin Germany

13. Department of Cellular Biophysics Technical University of Munich 80333 Munich Germany

Abstract

AbstractIn this study, organ‐on‐chip technology is used to develop an in vitro model of medium‐to‐large size arteries, the artery‐on‐a‐chip (AoC), with the objective to recapitulate the structure of the arterial wall and the relevant hemodynamic forces affecting luminal cells. AoCs exposed either to in vivo‐like shear stress values or kept in static conditions are assessed to generate a panel of novel genes modulated by shear stress. Considering the crucial role played by shear stress alterations in carotid arteries affected by atherosclerosis (CAD) and abdominal aortic aneurysms (AAA) disease development/progression, a patient cohort of hemodynamically relevant specimens is utilized, consisting of diseased and non‐diseased (internal control) vessel regions from the same patient. Genes activated by shear stress follow the same expression pattern in non‐diseased segments of human vessels. Single cell RNA sequencing (scRNA‐seq) enables to discriminate the unique cell subpopulations between non‐diseased and diseased vessel portions, revealing an enrichment of flow activated genes in structural cells originating from non‐diseased specimens. Furthermore, the AoC served as a platform for drug‐testing. It reproduced the effects of a therapeutic agent (lenvatinib) previously used in preclinical AAA studies, therefore extending the understanding of its therapeutic effect through a multicellular structure.

Funder

National Institutes of Health

Bayerisches Staatsministerium für Wissenschaft, Forschung und Kunst

Deutsche Forschungsgemeinschaft

Vetenskapsrådet

Publisher

Wiley

Subject

Pharmaceutical Science,Biomedical Engineering,Biomaterials

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