| Literature DB >> 29741092 |
Xingqing Xiao1, Zhifeng Kuang, Joseph M Slocik, Sirimuvva Tadepalli2, Michael Brothers, Steve Kim, Peter A Mirau, Claire Butkus, Barry L Farmer, Srikanth Singamaneni2, Carol K Hall1, Rajesh R Naik.
Abstract
Sensors for human health and performance monitoring require biological recognition elements (BREs) at device interfaces for the detection of key molecular biomarkers that are measurable biological state indicators. BREs, including peptides, antibodies, and nucleic acids, bind to biomarkers in the vicinity of the sensor surface to create a signal proportional to the biomarker concentration. The discovery of BREs with the required sensitivity and selectivity to bind biomarkers at low concentrations remains a fundamental challenge. In this study, we describe an in-silico approach to evolve higher sensitivity peptide-based BREs for the detection of cardiac event marker protein troponin I (cTnI) from a previously identified BRE as the parental affinity peptide. The P2 affinity peptide, evolved using our in-silico method, was found to have ∼16-fold higher affinity compared to the parent BRE and ∼10 fM (0.23 pg/mL) limit of detection. The approach described here can be applied towards designing BREs for other biomarkers for human health monitoring.Entities:
Keywords: LSPR; biorecognition elements; biosensor; computational modeling; phage displayed peptides; troponin I
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Year: 2018 PMID: 29741092 DOI: 10.1021/acssensors.8b00159
Source DB: PubMed Journal: ACS Sens ISSN: 2379-3694 Impact factor: 7.711