Uremic mouse model to study vascular calcification and “inflamm-aging”

Author:

Tölle MarkusORCID,Henkel Cornelia,Herrmann JaquelineORCID,Daniel ChristophORCID,Babic MilenORCID,Xia MengdiORCID,Schulz Anna M.ORCID,Amann KerstinORCID,van der Giet MarkusORCID,Schuchardt MirjamORCID

Abstract

AbstractCalcification and chronic inflammation of the vascular wall is a high-risk factor for cardiovascular mortality, especially in patients with chronic uremia. For the reduction or prevention of rapid disease progression, no specific treatment options are currently available. This study aimed to evaluate an adenine-based uremic mouse model for studying medial vessel calcification and senescence-associated secretory phenotype (SASP) changes of aortic tissue to unravel molecular pathogenesis and provide a model for therapy testing. The dietary adenine administration induced a stable and similar degree of chronic uremia in DBA2/N mice with an increase of uremia blood markers such as blood urea nitrogen, calcium, creatinine, alkaline phosphatase, and parathyroid hormone. Also, renal fibrosis and crystal deposits were detected upon adenine feeding. The uremic condition is related to a moderate to severe medial vessel calcification and subsequent elastin disorganization. In addition, expression of osteogenic markers as Bmp-2 and its transcription factor Sox-9 as well as p21 as senescence marker were increased in uremic mice compared to controls. Pro-inflammatory uremic proteins such as serum amyloid A, interleukin (Il)-1β, and Il-6 increased. This novel model of chronic uremia provides a simple method for investigation of signaling pathways in vascular inflammation and calcification and therefore offers an experimental basis for the development of potential therapeutic intervention studies. Graphical abstract

Funder

Ernst und Berta Grimmke Stiftung

Berlin-Institute-of-Health

Sonnenfeld Stiftung

DynAge Focus Area

Nanchong school science and technology strategic cooperation project

Charité - Universitätsmedizin Berlin

Publisher

Springer Science and Business Media LLC

Subject

Genetics (clinical),Drug Discovery,Molecular Medicine

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