Noncanonical atherosclerosis as the driving force in tricuspid aortic valve associated aneurysms - A trace collection

Christian Doppler(Johannes Kepler University of Linz), Barbara Meßner(Medical University of Vienna), Teresa Mimler(Johannes Kepler University of Linz), Bruno Schachner, Marlene Rezk(Kepler Universitätsklinikum), Clara Ganhör(Johannes Kepler University of Linz), Christian Wechselberger(Johannes Kepler University of Linz), Marina Müller(Johannes Kepler University of Linz), Špela Puh(Johannes Kepler University of Linz), Johannes Pröll(Johannes Kepler University of Linz), Barbara Arbeithuber(Kepler Universitätsklinikum), Thomas Müller(Universität Innsbruck), Andreas Zierer, David Bernhard(Johannes Kepler University of Linz)
Journal of Lipid Research
January 31, 2023
Cited by 13Open Access
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Abstract

Pathogenic mechanisms in degenerative thoracic aortic aneurysms (TAA) are still unclear. There is an ongoing debate about whether TAAs are caused by uniform or distinct processes, which would obviously have a major impact on future treatment strategies. Clearly, the ultimate outcome of TAA subgroups associated with a tricuspid aortic valve (TAV) or a bicuspid aortic valve (BAV) is the same, namely a TAA. Based on results from our own and others' studies, we decided to compare the different TAAs (TAV and BAV) and controls using a broad array of analyses, i.e., metabolomic analyses, gene expression profiling, protein expression analyses, histological characterization, and matrix-assisted laser desorption ionization imaging. Central findings of the present study are the presence of noncanonical atherosclerosis, pathological accumulation of macrophages, and disturbances of lipid metabolism in the aortic media. Moreover, we have also found that lipid metabolism is impaired systemically. Importantly, all of the above-described phenotypes are characteristic for TAV-TAA only, and not for BAV-TAA. In summary, our results suggest different modes of pathogenesis in TAV- and BAV-associated aneurysms. Intimal atherosclerotic changes play a more central role in TAV-TAA formation than previously thought, particularly as the observed alterations do not follow classical patterns. Atherosclerotic alterations are not limited to the intima but also affect and alter the TAV-TAA media. Further studies are needed to i) clarify patho-relevant intima-media interconnections, ii) define the origin of the systemic alteration of lipid metabolism, and iii) to define valid biomarkers for early diagnosis, disease progression, and successful treatments in TAV-TAAs.


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