Literature DB >> 22953757

High-resolution structural insights into bone: a solid-state NMR relaxation study utilizing paramagnetic doping.

Kamal H Mroue1, Neil MacKinnon, Jiadi Xu, Peizhi Zhu, Erin McNerny, David H Kohn, Michael D Morris, Ayyalusamy Ramamoorthy.   

Abstract

The hierarchical heterogeneous architecture of bone imposes significant challenges to structural and dynamic studies conducted by traditional biophysical techniques. High-resolution solid-state nuclear magnetic resonance (SSNMR) spectroscopy is capable of providing detailed atomic-level structural insights into such traditionally challenging materials. However, the relatively long data-collection time necessary to achieve a reliable signal-to-noise ratio (S/N) remains a major limitation for the widespread application of SSNMR on bone and related biomaterials. In this study, we attempt to overcome this limitation by employing the paramagnetic relaxation properties of copper(II) ions to shorten the (1)H intrinsic spin-lattice (T(1)) relaxation times measured in natural-abundance (13)C cross-polarization (CP) magic-angle-spinning (MAS) NMR experiments on bone tissues for the purpose of accelerating the data acquisition time in SSNMR. To this end, high-resolution solid-state (13)C CPMAS experiments were conducted on type I collagen (bovine tendon), bovine cortical bone, and demineralized bovine cortical bone, each in powdered form, to measure the (1)H T(1) values in the absence and in the presence of 30 mM Cu(II)(NH(4))(2)EDTA. Our results show that the (1)H T(1) values were successfully reduced by a factor of 2.2, 2.9, and 3.2 for bovine cortical bone, type I collagen, and demineralized bone, respectively, without reducing the spectral resolution and thus enabling faster data acquisition. In addition, paramagnetic quenching of particular (13)C NMR resonances on exposure to Cu(2+) ions in the absence of mineral was also observed, potentially suggesting the relative proximity of three main amino acids in the protein backbone (glycine, proline, and alanine) to the bone mineral surface.

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Year:  2012        PMID: 22953757      PMCID: PMC3460063          DOI: 10.1021/jp307935g

Source DB:  PubMed          Journal:  J Phys Chem B        ISSN: 1520-5207            Impact factor:   2.991


  48 in total

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3.  Cooperative deformation of mineral and collagen in bone at the nanoscale.

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4.  Fast acquisition of multi-dimensional spectra in solid-state NMR enabled by ultra-fast MAS.

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5.  Sensitivity enhancement using paramagnetic relaxation in MAS solid-state NMR of perdeuterated proteins.

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6.  Quantitative monitoring of extracellular matrix production in bone implants by 13C and 31P solid-state nuclear magnetic resonance spectroscopy.

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  19 in total

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2.  Application of paramagnetic relaxation enhancements to accelerate the acquisition of 2D and 3D solid-state NMR spectra of oriented membrane proteins.

Authors:  Songlin Wang; T Gopinath; Gianluigi Veglia
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Review 4.  Use of paramagnetic systems to speed-up NMR data acquisition and for structural and dynamic studies.

Authors:  Vojč Kocman; Giacomo M Di Mauro; Gianluigi Veglia; Ayyalusamy Ramamoorthy
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7.  Acceleration of natural-abundance solid-state MAS NMR measurements on bone by paramagnetic relaxation from gadolinium-DTPA.

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8.  Paramagnetic doping of a 7TM membrane protein in lipid bilayers by Gd³⁺-complexes for solid-state NMR spectroscopy.

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9.  Shortening spin-lattice relaxation using a copper-chelated lipid at low-temperatures - A magic angle spinning solid-state NMR study on a membrane-bound protein.

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10.  Crystallinity and compositional changes in carbonated apatites: Evidence from 31P solid-state NMR, Raman, and AFM analysis.

Authors:  John-David P McElderry; Peizhi Zhu; Kamal H Mroue; Jiadi Xu; Barbara Pavan; Ming Fang; Guisheng Zhao; Erin McNerny; David H Kohn; Renny T Franceschi; Mark M Banaszak Holl; Mary M J Tecklenburg; Ayyalusamy Ramamoorthy; Michael D Morris
Journal:  J Solid State Chem       Date:  2013-10       Impact factor: 3.498

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