Interplay between inflammation and calcification in cardiovascular diseases

Cardiovascular calcification has been linked to all-cause mortality and is a broadly adopted predictor of cardiovascular (CV) events. Rather than a mere by-product of the changing disease environment, calcification impacts actively the disease progression and pathogenesis as it predominates both in early- and late-stages, through mediating tissue biomechanical destabilisation and directly impacting tissue inflammation. However, its clinical contribution to the fate of the disease remains to be elucidated. Emerging body of evidence from both basic and clinical research has demonstrated the significance of the innate immune system in cardiovascular diseases (CVDs). Here, inflammation and calcification are engaged in a vicious cycle particularly at early-stages, whereas in advanced-lesions, large calcifications linked with suppressed inflammation and plaque stability. However, this interaction during disease progression remains largely elusive. The aim of this thesis is to investigate the interplay between inflammation and calcification in advanced atherosclerosis and calcific aortic valve disease (CAVD). Study I explores gene and protein expression signatures and biological pathways of advanced CAVD lesions in order to characterise the underlining mechanisms associated with the disease pathology. Multi-omics integration of overlapping transcriptome/proteome molecules with miRNAs, identified a unique CAVD-related protein-protein 3D layered interaction network. After addition of a metabolite layer, Alzheimer's disease (AD) was identified in the core of the gene-disease network. This study suggests a novel molecular CAVD network potentially linked to amyloid-like structures formation. Study II characterises osteomodulin (OMD) in the context of atherosclerosis, chronic kidney disease (CKD) and CAVD. Plasma OMD levels were correlated with markers of inflammation and bone turnover, with the protein being present in the calcified arterial media of patients with CKD stage 5. Circulating OMD levels were also associated with cardiac valve calcification in the same patients and its positive signal was detected in calcified valve leaflets by immunohistochemistry. In patients with carotid atherosclerosis, plasma OMD levels were increased in association with plaque calcification as assessed by computed tomography. Transcriptomic and proteomic data analysis showed that OMD expression was upregulated in atherosclerotic compared to non-atherosclerotic control arteries, and p