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Literature DB >> 22801429

Structural features and domain organization of huntingtin fibrils.

Charles W Bugg¹, J Mario Isas, Torsten Fischer, Paul H Patterson, Ralf Langen.

Abstract

Misfolding and aggregation of huntingtin is one of the hallmarks of Huntington disease, but the overall structure of these aggregates and the mechanisms by which huntingtin misfolds remain poorly understood. Here we used site-directed spin labeling and electron paramagnetic resonance (EPR) spectroscopy to study the structural features of huntingtin exon 1 (HDx1) containing 46 glutamine residues in its polyglutamine (polyQ) region. Despite some residual structuring in the N terminus, we find that soluble HDx1 is highly dynamic. Upon aggregation, the polyQ domain becomes strongly immobilized indicating significant tertiary or quaternary packing interactions. Analysis of spin-spin interactions does not show the close contact between same residues that is characteristic of the parallel, in-register structure commonly found in amyloids. Nevertheless, the same residues are still within 20 Å of each other, suggesting that polyQ domains from different molecules come into proximity in the fibrils. The N terminus has previously been found to take up a helical structure in fibrils. We find that this domain not only becomes structured, but that it also engages in tertiary or quaternary packing interactions. The existence of spin-spin interactions in this region suggests that such contacts could be made between N-terminal domains from different molecules. In contrast, the C-terminal domain is dynamic, contains polyproline II structure, and lacks pronounced packing interactions. This region must be facing away from the core of the fibrils. Collectively, these data provide new constraints for building structural models of HDx1 fibrils.

Entities: Chemical Disease Gene

Mesh：

Substances：

Year: 2012 PMID： 22801429 PMCID： PMC3442508 DOI： 10.1074/jbc.M112.353839

Source DB: PubMed Journal: J Biol Chem ISSN： 0021-9258 Impact factor: 5.157

58 in total

1. Fibril structure of human islet amyloid polypeptide.

Authors: Sahar Bedrood; Yiyu Li; J Mario Isas; Balachandra G Hegde; Ulrich Baxa; Ian S Haworth; Ralf Langen
Journal: J Biol Chem Date: 2011-12-20 Impact factor: 5.157

2. Modulation of polyglutamine conformations and dimer formation by the N-terminus of huntingtin.

Authors: Tim E Williamson; Andreas Vitalis; Scott L Crick; Rohit V Pappu
Journal: J Mol Biol Date: 2009-12-21 Impact factor: 5.469

3. Estimation of globular protein secondary structure from circular dichroism.

Authors: S W Provencher; J Glöckner
Journal: Biochemistry Date: 1981-01-06 Impact factor: 3.162

4. The first 17 amino acids of Huntingtin modulate its sub-cellular localization, aggregation and effects on calcium homeostasis.

Authors: Erica Rockabrand; Natalia Slepko; Antonello Pantalone; Vidya N Nukala; Aleksey Kazantsev; J Lawrence Marsh; Patrick G Sullivan; Joan S Steffan; Stefano L Sensi; Leslie Michels Thompson
Journal: Hum Mol Genet Date: 2006-11-29 Impact factor: 6.150

5. The aggregation-enhancing huntingtin N-terminus is helical in amyloid fibrils.

Authors: V N Sivanandam; Murali Jayaraman; Cody L Hoop; Ravindra Kodali; Ronald Wetzel; Patrick C A van der Wel
Journal: J Am Chem Soc Date: 2011-03-07 Impact factor: 15.419

6. Inhibiting the nucleation of amyloid structure in a huntingtin fragment by targeting α-helix-rich oligomeric intermediates.

Authors: Rakesh Mishra; Murali Jayaraman; Bartholomew P Roland; Elizabeth Landrum; Timothy Fullam; Ravindra Kodali; Ashwani K Thakur; Irene Arduini; Ronald Wetzel
Journal: J Mol Biol Date: 2011-12-09 Impact factor: 5.469

7. Slow amyloid nucleation via α-helix-rich oligomeric intermediates in short polyglutamine-containing huntingtin fragments.

Authors: Murali Jayaraman; Ravindra Kodali; Bankanidhi Sahoo; Ashwani K Thakur; Anand Mayasundari; Rakesh Mishra; Cynthia B Peterson; Ronald Wetzel
Journal: J Mol Biol Date: 2011-12-09 Impact factor: 5.469

8. Stacked sets of parallel, in-register beta-strands of beta2-microglobulin in amyloid fibrils revealed by site-directed spin labeling and chemical labeling.

Authors: Carol L Ladner; Min Chen; David P Smith; Geoffrey W Platt; Sheena E Radford; Ralf Langen
Journal: J Biol Chem Date: 2010-03-24 Impact factor: 5.157

9. Polyglutamine induced misfolding of huntingtin exon1 is modulated by the flanking sequences.

Authors: Vinal V Lakhani; Feng Ding; Nikolay V Dokholyan
Journal: PLoS Comput Biol Date: 2010-04-29 Impact factor: 4.475

10. Serines 13 and 16 are critical determinants of full-length human mutant huntingtin induced disease pathogenesis in HD mice.

Authors: Xiaofeng Gu; Erin R Greiner; Rakesh Mishra; Ravindra Kodali; Alex Osmand; Steven Finkbeiner; Joan S Steffan; Leslie Michels Thompson; Ronald Wetzel; X William Yang
Journal: Neuron Date: 2009-12-24 Impact factor: 17.173

45 in total

1. Protofilament Structure and Supramolecular Polymorphism of Aggregated Mutant Huntingtin Exon 1.

Authors: Jennifer C Boatz; Talia Piretra; Alessia Lasorsa; Irina Matlahov; James F Conway; Patrick C A van der Wel
Journal: J Mol Biol Date: 2020-06-27 Impact factor: 5.469

2. Unmasking the roles of N- and C-terminal flanking sequences from exon 1 of huntingtin as modulators of polyglutamine aggregation.

Authors: Scott L Crick; Kiersten M Ruff; Kanchan Garai; Carl Frieden; Rohit V Pappu
Journal: Proc Natl Acad Sci U S A Date: 2013-11-26 Impact factor: 11.205

Structural features and domain organization of huntingtin fibrils.

1. Fibril structure of human islet amyloid polypeptide.

2. Modulation of polyglutamine conformations and dimer formation by the N-terminus of huntingtin.

3. Estimation of globular protein secondary structure from circular dichroism.

4. The first 17 amino acids of Huntingtin modulate its sub-cellular localization, aggregation and effects on calcium homeostasis.

5. The aggregation-enhancing huntingtin N-terminus is helical in amyloid fibrils.

6. Inhibiting the nucleation of amyloid structure in a huntingtin fragment by targeting α-helix-rich oligomeric intermediates.

7. Slow amyloid nucleation via α-helix-rich oligomeric intermediates in short polyglutamine-containing huntingtin fragments.

8. Stacked sets of parallel, in-register beta-strands of beta2-microglobulin in amyloid fibrils revealed by site-directed spin labeling and chemical labeling.

9. Polyglutamine induced misfolding of huntingtin exon1 is modulated by the flanking sequences.

10. Serines 13 and 16 are critical determinants of full-length human mutant huntingtin induced disease pathogenesis in HD mice.

1. Protofilament Structure and Supramolecular Polymorphism of Aggregated Mutant Huntingtin Exon 1.

2. Unmasking the roles of N- and C-terminal flanking sequences from exon 1 of huntingtin as modulators of polyglutamine aggregation.

3. Conformational switching in PolyGln amyloid fibrils resulting from a single amino acid insertion.

4. Serine phosphorylation suppresses huntingtin amyloid accumulation by altering protein aggregation properties.

5. Investigating the structural impact of the glutamine repeat in huntingtin assembly.

6. Formation and Structure of Wild Type Huntingtin Exon-1 Fibrils.

Review 7. The emerging role of the first 17 amino acids of huntingtin in Huntington's disease.

8. Architecture of polyglutamine-containing fibrils from time-resolved fluorescence decay.

9. Acetylation within the First 17 Residues of Huntingtin Exon 1 Alters Aggregation and Lipid Binding.

10. β-hairpin-mediated nucleation of polyglutamine amyloid formation.