Literature DB >> 21807994

In vivo molecular imaging of peripheral amyloidosis using heparin-binding peptides.

Jonathan S Wall1, Tina Richey, Alan Stuckey, Robert Donnell, Sallie Macy, Emily B Martin, Angela Williams, Keiichi Higuchi, Stephen J Kennel.   

Abstract

Heparan sulfate proteoglycans (HSPGs) are ubiquitous components of pathologic amyloid deposits in the organs of patients with disorders such as Alzheimer's disease or systemic light chain (AL) or reactive (AA) amyloidosis. Molecular imaging methods for early detection are limited and generally unavailable outside the United Kingdom. Therefore, there is an urgent need to develop novel, specific amyloidophilic radiotracers for imaging to assist in diagnosis, prognostication, and monitoring response to therapy. Amyloid-associated HSPG can be differentiated from HSPG found in surrounding healthy cells and tissues by the preferential binding of certain HS-reactive single chain variable fragments and therefore, represents a biomarker that can be targeted specifically with appropriate reagents. Using a murine model of AA amyloidosis, we have examined the in vivo amyloid reactivity of seven heparin-binding peptides by using single photon emission and X-ray computed tomographic imaging, microautoradiography, and tissue biodistribution measurements. All of the peptides bound amyloid deposits within 1 h post-injection, but the extent of the reactivity differed widely, which was evidenced by image quality and grain density in autoradiographs. One radiolabeled peptide bound specifically to murine AA amyloid in the liver, spleen, kidney, adrenal, heart, and pancreas with such avidity that it was observed in single photon emission tomography images as late as 24 h post-injection. In addition, a biotinylated form of this peptide was shown histochemically to bind human AA, ALκ, ALλ, transthyretin amyloidosis (ATTR), and Aβ amyloid deposits in tissue sections. These basic heparin-binding peptides recognize murine and human amyloid deposits in both in vivo and ex vivo tissues and therefore, have potential as radiotracers for the noninvasive molecular imaging of amyloid deposits in situ.

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Year:  2011        PMID: 21807994      PMCID: PMC3161606          DOI: 10.1073/pnas.1103247108

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  52 in total

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3.  In vivo fragmentation of heparan sulfate by heparanase overexpression renders mice resistant to amyloid protein A amyloidosis.

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4.  The minimal functional sequence of protamine.

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Review 5.  Islet amyloid: a long-recognized but underappreciated pathological feature of type 2 diabetes.

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6.  Transgenic mouse model of AA amyloidosis.

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Authors:  A Rydh; O Suhr; S O Hietala; K R Ahlström; M B Pepys; P N Hawkins
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Review 10.  Amyloidosis.

Authors:  Mark B Pepys
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  35 in total

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4.  Mechanistic insights into the pH-dependent membrane peptide ATRAM.

Authors:  Vanessa P Nguyen; Loganathan Palanikumar; Stephen J Kennel; Daiane S Alves; Yujie Ye; Jonathan S Wall; Mazin Magzoub; Francisco N Barrera
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5.  Phagocyte depletion inhibits AA amyloid accumulation in AEF-induced huIL-6 transgenic mice.

Authors:  Stephen J Kennel; Sally Macy; Craig Wooliver; Ying Huang; Tina Richey; Eric Heidel; Jonathan S Wall
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6.  A novel method for quantifying peripheral tissue amyloid load by using the radiolabeled amyloidophilic peptide, p5.

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7.  Preliminary characterization of a novel peptide-Fc-fusion construct for targeting amyloid deposits.

Authors:  James S Foster; Richa Koul-Tiwari; Angela Williams; Emily B Martin; Tina Richey; Alan Stuckey; Sallie Macy; Stephen J Kennel; Jonathan S Wall
Journal:  Amyloid       Date:  2017-03       Impact factor: 7.141

8.  Tc-99m Radiolabeled Peptide p5 + 14 is an Effective Probe for SPECT Imaging of Systemic Amyloidosis.

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Review 9.  Heparin-binding Peptides as Novel Therapies to Stop SARS-CoV-2 Cellular Entry and Infection.

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10.  Peptide p5 binds both heparinase-sensitive glycosaminoglycans and fibrils in patient-derived AL amyloid extracts.

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