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A novel 3D-printed centrifugal ultrafiltration method reveals in vivo glycation of human serum albumin decreases its binding affinity for zinc

Metallomics. 2020-07-01; 
Monica J Jacobs, Cody W Pinger, Andre D Castiaux, Konnor J Maloney, Dana M Spence
Products/Services Used Details Operation
Custom Vector Construction … DNA coding for nanobelt protein was purchased from commercial supplier (Genscript, Nanjing) and sub-cloned into BamH I and Hind III restriction enzyme sites of pET21a vector to yield pET21a-NB using primers: NB-F (5′-GGATCCGGCCCGCATAAAATTGCGCAACTGAA-3 … Get A Quote

摘要

Plasma proteins are covalently modified in vivo by the high-glucose conditions in the bloodstreams of people with diabetes, resulting in changes to both structure and function. Human Serum Albumin (HSA) functions as a carrier-protein in the bloodstream, binding various ligands and tightly regulating their bioavailability. HSA is known to react with glucose via the Maillard reaction, causing adverse effects on its ability to bind and deliver certain ligands, such as metals. Here, the binding between in vivo glycated HSA and zinc (Zn2+) was determined using a novel centrifugal ultrafiltration method that was developed using a 3D-printed device. This method is rapid (90 minutes), capable of high-throughput measure... More

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