Alzheimer’s Disease & Dementia

Biography

Biography: Asokan Chinnasamy

Abstract

The BC3H1 smooth muscle cells of mice brain, the study was carried out membrane binding. Th is is important in relation to the activity of membrane proteins because losing the activity of such systems will ultimately lead to malfunction or death of the cell. Th e interactions of Serum Amyloid A (SAA) and Serum Amyloid A protofi brils with BC3H1 cells of the mouse are dealt with in detail to study the binding of SAA protofi brils in various conditions. Th e FACScan and MTT assay results have shown the SAA and SAA fi brils binding and cell toxicity with the BC3H1 cells with diff erent concentrations of Serum amyloid P component and Amyloid enhancing factor. Specifi cally, cells were incubated with 1.25-6.25 μM SAA-FITC and SAA protofi brils-FITC assayed. Th e 50% viable BC3H1 cells at 4-6 μM with an LD50 of 3.5 μM. Th e interaction of serum amyloid A fi brils with a cell surface binding site/receptor might alter the local environment to cause cellular dysfunction and to be more favorable for amyloid formation. Th e RAGE (receptor for advanced glycation endproducts) a polyvalent receptor in the immunoglobulin super family has been implicated in binding with the isoform of SAA (SAA1.1) which has the highest fi birillogenic property. Th e present study concludes the SAA fi brils more binding and cell cytotoxicity than SAA protein.