Persistence of Intraluminal Thrombus Makes Saccular Aneurysm More Biologically Active than Fusiform in an Experimental Rat Model.


Journal

Journal of vascular research
ISSN: 1423-0135
Titre abrégé: J Vasc Res
Pays: Switzerland
ID NLM: 9206092

Informations de publication

Date de publication:
2020
Historique:
received: 29 07 2019
accepted: 26 01 2020
pubmed: 31 3 2020
medline: 15 9 2020
entrez: 31 3 2020
Statut: ppublish

Résumé

Saccular aneurysms are thought to have a worse prognosis than fusiform aneurysms in humans, due to hemodynamic reasons. However, data comparing hemodynamic and biology in saccular and fusiform aneurysms are lacking. The main objective was to evaluate the impact of aneurysm morphology on intra-luminal thrombus (ILT) formation and activity. Forty Lewis rats were ran-domly divided into 2 groups of 20: "saccular" (Group A) and "fusiform" (Group B) aneurysms. Decellularized thoracic aortas from guinea pigs were xenografted to create saccular or fusiform aneurysms. Final imaging evaluation of the aneurysms was carried out during the third week, by quantitative Doppler ultrasound and magnetic resonance imaging. Assays of myeloperoxidase (MPO), platelet factor 4 (PF4), advanced oxidation protein products (AOPPs) iron and matrix metallopeptidase-9 (MMP-9) were performed as biological criteria. Quantitatively, saccular aneurysms are characterized by a more thicker ILT, lower inflow velocities and more important relative backflow velocities as compared to fusiform aneurysms. Compared to fusiform, saccular aneurysms released significantly more MPO (p = 0.004), PF4 (p = 0.02), AOPPs (p < 0.002), iron (p < 0.0001) and MMP-9 (p < 0.04). Experimental saccular and fusiform aneurysms show differential specific hemodynamics, which seem to impact the histology and the biology of the ILT in each type of aneurysm.

Identifiants

pubmed: 32222706
pii: 000506159
doi: 10.1159/000506159
doi:

Substances chimiques

Advanced Oxidation Protein Products 0
Platelet Factor 4 37270-94-3
Iron E1UOL152H7
Peroxidase EC 1.11.1.7
Matrix Metalloproteinase 9 EC 3.4.24.35
Mmp9 protein, rat EC 3.4.24.35

Types de publication

Comparative Study Journal Article Research Support, Non-U.S. Gov't

Langues

eng

Sous-ensembles de citation

IM

Pagination

164-176

Informations de copyright

© 2020 S. Karger AG, Basel.

Auteurs

Harry Etienne (H)

UMR 1148, Inserm-Denis Diderot University, Hôpital Xavier Bichat, Paris, France, h.etienne@hotmail.fr.

Clément Journé (C)

UMR 1148, Inserm-Denis Diderot University, Hôpital Xavier Bichat, Paris, France.
UMS 34, Fédération de Recherche en Imagerie Multimodalités, Paris, France.

Aymeric Rouchaud (A)

Université Limoges, CNRS, XLIM, UMR 7252, Limoges, France.
Department of interventional neuroradiology, CHU Dupuytren, Limoges, France.

Jean Senemaud (J)

UMR 1148, Inserm-Denis Diderot University, Hôpital Xavier Bichat, Paris, France.
Department of Vascular, Thoracic Surgery and Lung Transplantation, Hôpital Xavier Bichat, Paris, France.

Liliane Louedec (L)

UMR 1148, Inserm-Denis Diderot University, Hôpital Xavier Bichat, Paris, France.

Quentin Pellenc (Q)

UMR 1148, Inserm-Denis Diderot University, Hôpital Xavier Bichat, Paris, France.
Department of Vascular, Thoracic Surgery and Lung Transplantation, Hôpital Xavier Bichat, Paris, France.

Raphaël Coscas (R)

Department of Vascular Surgery, Ambroise Paré University Hospital, AP-HP, Boulogne-Billancourt, France.

Laurent Gouya (L)

Paris Diderot University, INSERM U1149, Hème, fer et pathologies inflammatoires, Assistance Publique des Hôpitaux de Paris, Hôpital Louis Mourier, Paris, France.

Sébastien Dupont (S)

UMR 1148, Inserm-Denis Diderot University, Hôpital Xavier Bichat, Paris, France.

Jean-Baptiste Michel (JB)

UMR 1148, Inserm-Denis Diderot University, Hôpital Xavier Bichat, Paris, France.

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Classifications MeSH