4.6 Article

Electrochemical DNA Biosensor That Detects Early Celiac Disease Autoantibodies

期刊

SENSORS
卷 21, 期 8, 页码 -

出版社

MDPI
DOI: 10.3390/s21082671

关键词

celiac disease; celiac disease autoantibodies; E-DNA-based biosensors; biosensor; celiac disease autoantibody epitope; celiac disease diagnostics

资金

  1. Metropolitan State University of Denver undergraduate research program

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Diagnosing celiac disease (CD) is challenging due to overlapping symptoms with other diseases and invasive diagnostics. A proposed less invasive method using an electrochemical DNA biosensor for CD-specific autoantibodies shows promise in detecting CD-specific patient-derived AABs, with the potential to improve diagnostic tools in the future.
Although it is estimated that more than one million Americans have celiac disease (CD), it remains challenging to diagnose. CD, an autoimmune and inflammatory response following the ingestion of gluten-containing foods, has symptoms overlapping with other diseases and requires invasive diagnostics. The gold standard for CD diagnosis involves serologic blood tests followed by invasive confirmatory biopsies. Here, we propose a less invasive method using an electrochemical DNA (E-DNA) biosensor for CD-specific autoantibodies (AABs) circulating in blood. In our approach, CD-specific AABs bind a synthetic neoepitope, causing a conformational change in the biosensor, as well as a change in the environment of an attached redox reporter, producing a measurable current reduction. We assessed the biosensor's ability to detect CD-specific patient-derived AABs in physiological buffer as well as buffer supplemented with bovine serum. Our biosensor was able to detect AABs in a dose-dependent manner; increased signal change correlated with increased AAB concentration with an apparent dissociation constant of 0.09 +/- 0.03 units/mL of AABs. Furthermore, we found our biosensor to be target-specific, with minimal off-target binding of multiple unrelated biomarkers. Future efforts aimed at increasing sensitivity in complex media may build upon the biosensor design presented here to further improve CD AAB detection and CD diagnostic tools.

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