Human and porcine aortic valve endothelial and interstitial cell isolation and characterization

Nehl, Denise; Goody, Philip Roger; Maus, Katharina; Pfeifer, Alexander; Aikawa, Elena; Bakthiary, Farhad; Zimmer, Sebastian; Nickenig, Georg; Jansen, Felix; Hosen, Mohammed Rabiul

doi:10.3389/fcvm.2023.1151028

Cited by 3 publications

(1 citation statement)

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“…The most common example of the transitional phenotype in blood vessels and heart valves is the EndoMT, which is notable for the expression of both endothelial (e.g., CD31 or VEGFR2) and mesenchymal (e.g., α-SMA or fibroblast-associated protein) markers. The EndoMT has been reported as a spontaneous phenomenon in human umbilical vein endothelial cells cultured on an uncoated dish [40], as an inflammation-or ECM-induced molecular event in primary culture of VECs [41][42][43], as a physiological process indispensable for prenatal development of the heart [44][45][46], and also in the AVs obtained from the patients with CAS [47][48][49]. However, there have been no reports on whether the En-doMT occurs after the implantation of xenogeneic or tissue-engineered implants, including BHVs.…”

Section: Discussionmentioning

confidence: 99%

Embedding and Backscattered Scanning Electron Microscopy (EM-BSEM) Is Preferential over Immunophenotyping in Relation to Bioprosthetic Heart Valves

Kostyunin,

Glushkova,

Velikanova

et al. 2023

IJMS

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Hitherto, calcified aortic valves (AVs) and failing bioprosthetic heart valves (BHVs) have been investigated by similar approaches, mostly limited to various immunostaining techniques. Having employed multiple immunostaining combinations, we demonstrated that AVs retain a well-defined cellular hierarchy even at severe stenosis, whilst BHVs were notable for the stochastic degradation of the extracellular matrix (ECM) and aggressive infiltration by ECM-digesting macrophages. Leukocytes (CD45+) comprised ≤10% cells in the AVs but were the predominant cell lineage in BHVs (≥80% cells). Albeit cells with uncertain immunophenotype were rarely encountered in the AVs (≤5% cells), they were commonly found in BHVs (≥80% cells). Whilst cell conversions in the AVs were limited to the endothelial-to-mesenchymal transition (represented by CD31+α-SMA+ cells) and the formation of endothelial-like (CD31+CD68+) cells at the AV surface, BHVs harboured numerous macrophages with a transitional phenotype, mostly CD45+CD31+, CD45+α-SMA+, and CD68+α-SMA+. In contrast to immunostaining, which was unable to predict cell function in the BHVs, our whole-specimen, nondestructive electron microscopy approach (EM-BSEM) was able to distinguish between quiescent and matrix-degrading macrophages, foam cells, and multinucleated giant cells to conduct the ultrastructural analysis of organelles and the ECM, and to preserve tissue integrity. Hence, we suggest EM-BSEM as a technique of choice for studying the cellular landscape of BHVs.

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