A proteomic atlas of the neointima identifies novel druggable targets for 
preventive therapy

Wierer, Michael; Werner, Julia; Wobst, Jana; Kastrati, Adnan; Cepele, Ganildo; Aherrahrou, Redouane; Sager, Hendrik B.; Erdmann, Jeanette; Dichgans, Martin; Flockerzi, Veit; Civelek, Mete; Dietrich, Alexander; Mann, Matthias; Schunkert, Heribert; Kessler, Thorsten

doi:10.1093/eurheartj/ehab140

Datensatz

DATENSATZ AKTIONENEXPORT

Zur Ablage hinzufügen

Lokale TagsFreigabegeschichteDetailsÜbersicht

Freigegeben

Zeitschriftenartikel

A proteomic atlas of the neointima identifies novel druggable targets for preventive therapy

MPG-Autoren

/persons/resource/persons195388

Wierer, Michael
Mann, Matthias / Proteomics and Signal Transduction, Max Planck Institute of Biochemistry, Max Planck Society;

/persons/resource/persons78356

Mann, Matthias
Mann, Matthias / Proteomics and Signal Transduction, Max Planck Institute of Biochemistry, Max Planck Society;

Externe Ressourcen

Es sind keine externen Ressourcen hinterlegt

Volltexte (beschränkter Zugriff)

Für Ihren IP-Bereich sind aktuell keine Volltexte freigegeben.

Volltexte (frei zugänglich)

Es sind keine frei zugänglichen Volltexte in PuRe verfügbar

Ergänzendes Material (frei zugänglich)

Es sind keine frei zugänglichen Ergänzenden Materialien verfügbar

Zitation

Wierer, M., Werner, J., Wobst, J., Kastrati, A., Cepele, G., Aherrahrou, R., et al. (2021). A proteomic atlas of the neointima identifies novel druggable targets for preventive therapy. European Heart Journal, 42(18), 1773-1785. doi:10.1093/eurheartj/ehab140.

Zitierlink: https://hdl.handle.net/21.11116/0000-0008-D0E3-C

Zusammenfassung

Aims In-stent restenosis is a complication after coronary stenting associated with morbidity and mortality. Here, we sought to investigate the molecular processes underlying neointima formation and to identify new treatment and prevention targets.
Methods and results Neointima formation was induced by wire injury in mouse femoral arteries. High-accuracy proteomic measurement of single femoral arteries to a depth of about 5000 proteins revealed massive proteome remodelling, with more than half of all proteins exhibiting expression differences between injured and non-injured vessels. We observed major changes in the composition of the extracellular matrix and cell migration processes. Among the latter, we identified the classical transient receptor potential channel 6 (TRPC6) to drive neointima formation. While Trpc6(-)(/-) mice presented reduced neointima formation compared to wild-type mice (1.44 +/- 0.39 vs. 2.16 +/- 0.48, P=0.01), activating or repressing TRPC6 in human vascular smooth muscle cells resulted in increased [vehicle 156.9 +/- 15.8 vs. 1-oleoyl-2-acetyl-sn-glycerol 179.1 +/- 8.07 (10(3) pixels), P = 0.01] or decreased migratory capacity [vehicle 130.0 +/- 26.1 vs. SAR7334 111.4 +/- 38.0 (103 pixels), P= 0.04], respectively. In a cohort of individuals with angiographic follow-up (n=3068, males: 69.9%, age: 59 +/- 11 years, follow-up 217.1 +/- 156.4 days), homozygous carriers of a common genetic variant associated with elevated TRPC6 expression were at increased risk of restenosis after coronary stenting (adjusted odds ratio 1.49, 95% confidence interval 1.08-2.05; P=0.01).
Conclusions Our study provides a proteomic atlas of the healthy and injured arterial wall that can be used to define novel factors for therapeutic targeting. We present TRPC6 as an actionable target to prevent neointima formation secondary to vascular injury and stent implantation.
[GRAPHICS]
.