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Browsing UGC Funded Project by Author "Chakraborty, Santanu"
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Item Asporin function in aortic endothelial cell mineralization and calcification(2019-02-14) Chakraborty, SantanuWorldwide, calcific aortic valve disease is one of the leading causes of morbidity and mortality among patients with cardiac abnormalities. Aortic valve mineralization and calcification are the key events of adult calcific aortic valve disease manifestation and functional insufficiency. Due to heavy mineralization and calcification, adult aortic valvular cusps show disorganized and dispersed stratification concomitant with deposition of calcific nodules with severely compromised adult valve function. Interestingly, shared gene regulatory pathways are identified between bone forming cells and heart valve cells during development. Asporin, a small leucine rich proteoglycan, acts to inhibit mineralization in periodontal ligament cells and is also detected in normal murine adult aortic valve leaflets with unknown function. Therefore, to understand the Asporin function in aortic cusp mineralization and calcification, adult avian aortic valvular interstitial cell culture system is established and osteogenesis has been induced in these cells successfully. Upon induction of osteogenesis, reduced expression of Asporin mRNA and increased expression of bone and osteogenesis markers are detected compared to cells maintained without osteogenic induction. Moreover, addition of human recombinant Asporin protein also reduces the mineralization level in cultured adult aortic valve cells with induced osteogenesis. Therefore, we have identified Asporin as a natural anti-calcific molecule with a therapeutic potential in the treatment of human calcific aortic valve disease.