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How human serum albumin‐selective DNA aptamer binds to bovine and canine serum albumins
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AbstractSerum albumin (SA) is the most abundant carrier protein in blood. SA carries a diverse range of nutrients, drugs, and metal ions. It has wide clinical and biochemical applications. Human serum albumin (HSA) can be used as a biomarker for kidney and liver diseases. Aptasensor is one of potential HSA detection methods. HSA‐specific aptamer was selected for HSA detection. In animals, bovine serum albumin (BSA) and canine serum albumins (CSA) share high sequence similarities to HSA. Thus, it is interesting to explore the possibility of using HSA‐selective aptamer for BSA and CSA aptasensor. In this study, molecular dynamics (MD) simulations were initially employed to investigate the binding of aptamer to BSA and CSA in comparison to HSA. Like HSA, both BSA and CSA can bind aptamer, but different binding affinities are observed. BSA shows the tighter binding to aptamer than CSA. Domain III is found to be the aptamer‐binding domain although no specific aptamer conformation is captured. However, in all cases, the aptamer utilizes the 3′‐end to attach on an albumin surface. Both nucleobases and phosphate backbones on a DNA aptamer are important for albumin‐aptamer complexation. Our results imply the possibility of using HSA‐specific aptamer for BSA detection due to tighter binding observed, but may be less effective in CSA. However, the test in actual complicated condition must be further studied.
Title: How human serum albumin‐selective DNA aptamer binds to bovine and canine serum albumins
Description:
AbstractSerum albumin (SA) is the most abundant carrier protein in blood.
SA carries a diverse range of nutrients, drugs, and metal ions.
It has wide clinical and biochemical applications.
Human serum albumin (HSA) can be used as a biomarker for kidney and liver diseases.
Aptasensor is one of potential HSA detection methods.
HSA‐specific aptamer was selected for HSA detection.
In animals, bovine serum albumin (BSA) and canine serum albumins (CSA) share high sequence similarities to HSA.
Thus, it is interesting to explore the possibility of using HSA‐selective aptamer for BSA and CSA aptasensor.
In this study, molecular dynamics (MD) simulations were initially employed to investigate the binding of aptamer to BSA and CSA in comparison to HSA.
Like HSA, both BSA and CSA can bind aptamer, but different binding affinities are observed.
BSA shows the tighter binding to aptamer than CSA.
Domain III is found to be the aptamer‐binding domain although no specific aptamer conformation is captured.
However, in all cases, the aptamer utilizes the 3′‐end to attach on an albumin surface.
Both nucleobases and phosphate backbones on a DNA aptamer are important for albumin‐aptamer complexation.
Our results imply the possibility of using HSA‐specific aptamer for BSA detection due to tighter binding observed, but may be less effective in CSA.
However, the test in actual complicated condition must be further studied.
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