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Characterizing amyloid protein conformation with a multi-resonant metasurface based biosensor in the infrared window. | LitMetric

AI Article Synopsis

  • Misfolding of amyloid proteins leads to neurodegeneration and the development of conformational diseases, but effective detection methods have been lacking.
  • A novel metasurface-based biosensor has been proposed to characterize protein conformations using engineered complementary split ring resonators (cSRR) that enhance detection in both near-infrared (NIR) and mid-infrared (MIR) spectra.
  • This biosensor offers sensitive detection of changes in the biolayer's refractive index and thickness in the NIR, and identifies specific molecular conformations in the MIR by recognizing unique spectral bands, aiding in the understanding of protein misfolding at the molecular level.

Article Abstract

Misfolding of amyloid protein will cause neurodegeneration and trigger conformational disease. The lack of an effective detection approach is a brake on unveiling the mechanism of protein misfolding. We theoretically proposed a novel metasurface-based biosensor for characterizing the protein's conformation. The coupling complementary split ring resonator (cSRR) was engineered to manipulate incident waves in the near-infrared (NIR) and mid-infrared (MIR) windows at the same sensing surface. The cSRRs had the advantages of intensifying the electric field and sharpening the resonance profile, resulting in a highly qualified biosensing performance. In the NIR window, the biolayer's refractive index and thickness change were detected by the dual-wavelength, which resolved into an optogeometrical parameter of the amyloid biolayer. In the MIR window, the resonant wave specifically triggered the rotation-vibration transition of amyloid protein molecules with different conformations, which was shown as the unique Amide I and II bands in the fingerprint spectrum. Thus, our proposed biosensor presented sensitive detection of biolayer and specific identification of constituent molecules. It is helpful to interpret the protein's misfolding behavior on the molecular level by associating the biolayer's structure and the constituent molecule's conformational change.

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Source
http://dx.doi.org/10.1364/OE.514894DOI Listing

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