Biobanking: Objectives, Requirements, and Future Challenges-Experiences from the Munich Vascular Biobank

Overview

Journal J Clin Med

Specialty General Medicine

Date 2019 Feb 21

PMID 30781475

Citations 21

Authors

Jaroslav Pelisek

Renate Hegenloh

Sabine Bauer

Susanne Metschl

Jessica Pauli

Nadiya Glukha

Albert Busch

Benedikt Reutersberg

Michael Kallmayer

Matthias Trenner

Heiko Wendorff

Pavlos Tsantilas

Sofie Schmid

Christoph Knappich

Christoph Schaeffer

Thomas Stadlbauer

Gabor Biro

Uta Wertern

Franz Meisner

Kerstin Stoklasa

Anna-Leonie Menges

Oksana Radu

Sabine Dallmann-Sieber

Angelos Karlas

Eva Knipfer

Christian Reeps

Alexander Zimmermann

Lars Maegdefessel

Hans-Henning Eckstein

Affiliations

Soon will be listed here.

Abstract

Collecting biological tissue samples in a biobank grants a unique opportunity to validate diagnostic and therapeutic strategies for translational and clinical research. In the present work, we provide our long-standing experience in establishing and maintaining a biobank of vascular tissue samples, including the evaluation of tissue quality, especially in formalin-fixed paraffin-embedded specimens (FFPE). Our Munich Vascular Biobank includes, thus far, vascular biomaterial from patients with high-grade carotid artery stenosis ( = 1567), peripheral arterial disease ( = 703), and abdominal aortic aneurysm ( = 481) from our Department of Vascular and Endovascular Surgery (January 2004⁻December 2018). Vascular tissue samples are continuously processed and characterized to assess tissue morphology, histological quality, cellular composition, inflammation, calcification, neovascularization, and the content of elastin and collagen fibers. Atherosclerotic plaques are further classified in accordance with the American Heart Association (AHA), and plaque stability is determined. In order to assess the quality of RNA from FFPE tissue samples over time (2009⁻2018), RNA integrity number (RIN) and the extent of RNA fragmentation were evaluated. Expression analysis was performed with two housekeeping genes-glyceraldehyde 3-phosphate dehydrogenase () and beta-actin ()-using TaqMan-based quantitative reverse-transcription polymerase chain reaction (qRT)-PCR. FFPE biospecimens demonstrated unaltered RNA stability over time for up to 10 years. Furthermore, we provide a protocol for processing tissue samples in our Munich Vascular Biobank. In this work, we demonstrate that biobanking is an important tool not only for scientific research but also for clinical usage and personalized medicine.

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