Literature DB >> 26241117

Probing Site-Specific Structural Information of Peptides at Model Membrane Interface In Situ.

Bei Ding1, Afra Panahi1, Jia-Jung Ho2, Jennifer E Laaser2, Charles L Brooks1, Martin T Zanni2, Zhan Chen1.   

Abstract

Isotope labeling is a powerful technique to probe detailed structures of biological molecules with a variety of analytical methods such as NMR and vibrational spectroscopies. It is important to obtain molecular structural information on biological molecules at interfaces such as cell membranes, but it is challenging to use the isotope labeling method to study interfacial biomolecules. Here, by individually (13)C═(16)O labeling ten residues of a peptide, Ovispirin-1, we have demonstrated for the first time that a site-specific environment of membrane associated peptide can be probed by the submonolayer surface sensitive sum frequency generation (SFG) vibrational spectroscopy in situ. With the peptide associated with a single lipid bilayer, the sinusoidal trend of the SFG line width and peak-center frequency suggests that the peptide is located at the interface beneath the lipid headgroup region. The constructive interferences between the isotope labeled peaks and the main peptide amide I peak contributed by the unlabeled components were used to determine the membrane orientation of the peptide. From the SFG spectral peak-center frequency, line width, and polarization dependence of the isotope labeled units, we deduced structural information on individual units of the peptide associated with a model cell membrane. We also performed molecular dynamics (MD) simulations to understand peptide-membrane interactions. The physical pictures described by simulation agree well with the SFG experimental result. This research demonstrates the feasibility and power of using isotope labeling SFG to probe molecular structures of interfacial biological molecules in situ in real time.

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Year:  2015        PMID: 26241117      PMCID: PMC5859116          DOI: 10.1021/jacs.5b04024

Source DB:  PubMed          Journal:  J Am Chem Soc        ISSN: 0002-7863            Impact factor:   15.419


  65 in total

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3.  Phase-sensitive sum-frequency vibrational spectroscopy and its application to studies of interfacial alkyl chains.

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Authors:  Andrew P Boughton; Pei Yang; Valerie M Tesmer; Bei Ding; John J G Tesmer; Zhan Chen
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6.  Orientation determination of protein helical secondary structures using linear and nonlinear vibrational spectroscopy.

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7.  SFG analysis of surface bound proteins: a route towards structure determination.

Authors:  Tobias Weidner; David G Castner
Journal:  Phys Chem Chem Phys       Date:  2013-08-14       Impact factor: 3.676

8.  Site-specific orientation of an α-helical peptide ovispirin-1 from isotope-labeled SFG spectroscopy.

Authors:  Bei Ding; Jennifer E Laaser; Yuwei Liu; Pengrui Wang; Martin T Zanni; Zhan Chen
Journal:  J Phys Chem B       Date:  2013-11-14       Impact factor: 2.991

9.  Two-dimensional sum-frequency generation reveals structure and dynamics of a surface-bound peptide.

Authors:  Jennifer E Laaser; David R Skoff; Jia-Jung Ho; Yongho Joo; Arnaldo L Serrano; Jay D Steinkruger; Padma Gopalan; Samuel H Gellman; Martin T Zanni
Journal:  J Am Chem Soc       Date:  2014-01-08       Impact factor: 15.419

Review 10.  In situ molecular level studies on membrane related peptides and proteins in real time using sum frequency generation vibrational spectroscopy.

Authors:  Shuji Ye; Khoi Tan Nguyen; Stéphanie V Le Clair; Zhan Chen
Journal:  J Struct Biol       Date:  2009-03-21       Impact factor: 2.867

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2.  Ultrafast energy relaxation dynamics of amide I vibrations coupled with protein-bound water molecules.

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Journal:  RSC Adv       Date:  2018-01-03       Impact factor: 4.036

Review 5.  Polarization-Dependent Heterodyne-Detected Sum-Frequency Generation Spectroscopy as a Tool to Explore Surface Molecular Orientation and Ångström-Scale Depth Profiling.

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  5 in total

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