Computationally Designed Epitope-Mediated Imprinted Polymers versus Conventional Epitope Imprints for the Detection of Human Adenovirus in Water and Human Serum Samples.
Ekin SehitGuiyang YaoGiovanni BattocchioRahil RadfarJakob TrimpertMaria-Andrea MroginskiRoderich D SüssmuthZeynep AltintasPublished in: ACS sensors (2024)
Detection of pathogenic viruses for point-of-care applications has attracted great attention since the COVID-19 pandemic. Current virus diagnostic tools are laborious and expensive, while requiring medically trained staff. Although user-friendly and cost-effective biosensors are utilized for virus detection, many of them rely on recognition elements that suffer major drawbacks. Herein, computationally designed epitope-imprinted polymers (eIPs) are conjugated with a portable piezoelectric sensing platform to establish a sensitive and robust biosensor for the human pathogenic adenovirus (HAdV). The template epitope is selected from the knob part of the HAdV capsid, ensuring surface accessibility. Computational simulations are performed to evaluate the conformational stability of the selected epitope. Further, molecular dynamics simulations are executed to investigate the interactions between the epitope and the different functional monomers for the smart design of eIPs. The HAdV epitope is imprinted via the solid-phase synthesis method to produce eIPs using in silico-selected ingredients. The synthetic receptors show a remarkable detection sensitivity (LOD: 10 2 pfu mL -1 ) and affinity (dissociation constant ( K d ): 6.48 × 10 -12 M) for HAdV. Moreover, the computational eIPs lead to around twofold improved binding behavior than the eIPs synthesized with a well-established conventional recipe. The proposed computational strategy holds enormous potential for the intelligent design of ultrasensitive imprinted polymer binders.
Keyphrases
- label free
- molecular dynamics simulations
- monoclonal antibody
- loop mediated isothermal amplification
- endothelial cells
- molecular docking
- molecular dynamics
- solid phase extraction
- working memory
- induced pluripotent stem cells
- high throughput
- molecularly imprinted
- pluripotent stem cells
- transcription factor
- high resolution
- dna binding
- genetic diversity