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Literature DB >> 19699209

Examining polyglutamine peptide length: a connection between collapsed conformations and increased aggregation.

Abstract

Abnormally expanded polyglutamine domains in proteins are associated with several neurodegenerative diseases, of which the best known is Huntington's. Expansion of the polyglutamine domain facilitates aggregation of the affected protein, and several studies directly link aggregation to neurotoxicity. The age of onset of disease is inversely correlated with the length of the polyglutamine domain; this correlation motivates an examination of the role of the length of the domain on aggregation. In this investigation, peptides containing 8 to 24 glutamines were synthesized, and their conformational and aggregation properties were examined. All peptides lacked secondary structure. Fluorescence resonance energy transfer studies revealed that the peptides became increasingly collapsed as the number of glutamine residues increased. The effective persistence length was estimated to decrease from approximately 11 to approximately 7 A as the number of glutamines increased from 8 to 24. A comparison of our data with theoretical results suggests that phosphate-buffered saline is a good solvent for Q8 and Q12, a theta solvent for Q16, and a poor solvent for Q20 and Q24. By dynamic light scattering, we observed that Q16, Q20, and Q24, but not Q8 or Q12, immediately formed soluble aggregates upon dilution into phosphate-buffered saline at 37 degrees C. Thus, Q16 stands at the transition point between good and poor solvent and between stable and aggregation-prone peptide. Examination of aggregates by transmission electron microscopy, along with kinetic assays for sedimentation, provided evidence indicating that soluble aggregates mature into sedimentable aggregates. Together, the data support a mechanism of aggregation in which monomer collapse is accompanied by formation of soluble oligomers; these soluble species lack regular secondary structure but appear morphologically similar to the sedimentable aggregates into which they eventually mature.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Substances：
Peptides
polyglutamine

Year: 2009 PMID： 19699209 PMCID： PMC2764006 DOI： 10.1016/j.jmb.2009.08.034

Source DB: PubMed Journal: J Mol Biol ISSN： 0022-2836 Impact factor: 5.469

48 in total

1. Neurodegeneration. A glutamine-rich trail leads to transcription factors.

Authors: Richard N Freiman; Robert Tjian
Journal: Science Date: 2002-06-21 Impact factor: 47.728

2. Failure of Energy Transfer between Identical Aromatic Molecules on Excitation at the Long Wave Edge of the Absorption Spectrum.

Authors: G Weber; M Shinitzky
Journal: Proc Natl Acad Sci U S A Date: 1970-04 Impact factor: 11.205

3. Cooperative effects of cofilin (ADF) on actin structure suggest allosteric mechanism of cofilin function.

Authors: Andrey A Bobkov; Andras Muhlrad; Dmitry A Pavlov; Kaveh Kokabi; Atilgan Yilmaz; Emil Reisler
Journal: J Mol Biol Date: 2005-12-09 Impact factor: 5.469

4. Identification of anti-prion compounds as efficient inhibitors of polyglutamine protein aggregation in a zebrafish model.

Authors: Niclas W Schiffer; Sarah A Broadley; Thomas Hirschberger; Paul Tavan; Hans A Kretzschmar; Armin Giese; Christian Haass; F Ulrich Hartl; Bettina Schmid
Journal: J Biol Chem Date: 2006-12-14 Impact factor: 5.157

5. Polyglutamine aggregation behavior in vitro supports a recruitment mechanism of cytotoxicity.

Authors: S Chen; V Berthelier; W Yang; R Wetzel
Journal: J Mol Biol Date: 2001-08-03 Impact factor: 5.469

6. Fluorescence correlation spectroscopy shows that monomeric polyglutamine molecules form collapsed structures in aqueous solutions.

Authors: Scott L Crick; Murali Jayaraman; Carl Frieden; Ronald Wetzel; Rohit V Pappu
Journal: Proc Natl Acad Sci U S A Date: 2006-10-30 Impact factor: 11.205

7. Structural and functional analysis of ataxin-2 and ataxin-3.

Authors: Mario Albrecht; Michael Golatta; Ullrich Wüllner; Thomas Lengauer
Journal: Eur J Biochem Date: 2004-08

Review 8. Polyglutamine neurodegeneration: protein misfolding revisited.

Authors: Aislinn J Williams; Henry L Paulson
Journal: Trends Neurosci Date: 2008-09-06 Impact factor: 13.837

9. Aggregated polyglutamine peptides delivered to nuclei are toxic to mammalian cells.

Authors: Wen Yang; John R Dunlap; Richard B Andrews; Ronald Wetzel
Journal: Hum Mol Genet Date: 2002-11-01 Impact factor: 6.150

10. Pathogenic and non-pathogenic polyglutamine tracts have similar structural properties: towards a length-dependent toxicity gradient.

Authors: Fabrice A C Klein; Annalisa Pastore; Laura Masino; Gabrielle Zeder-Lutz; Hélène Nierengarten; Mustapha Oulad-Abdelghani; Danièle Altschuh; Jean-Louis Mandel; Yvon Trottier
Journal: J Mol Biol Date: 2007-05-18 Impact factor: 5.469

55 in total

1. Dynamic imaging by fluorescence correlation spectroscopy identifies diverse populations of polyglutamine oligomers formed in vivo.

Authors: Monica Beam; M Catarina Silva; Richard I Morimoto
Journal: J Biol Chem Date: 2012-06-05 Impact factor: 5.157

Examining polyglutamine peptide length: a connection between collapsed conformations and increased aggregation.

1. Neurodegeneration. A glutamine-rich trail leads to transcription factors.

2. Failure of Energy Transfer between Identical Aromatic Molecules on Excitation at the Long Wave Edge of the Absorption Spectrum.

3. Cooperative effects of cofilin (ADF) on actin structure suggest allosteric mechanism of cofilin function.

4. Identification of anti-prion compounds as efficient inhibitors of polyglutamine protein aggregation in a zebrafish model.

5. Polyglutamine aggregation behavior in vitro supports a recruitment mechanism of cytotoxicity.

6. Fluorescence correlation spectroscopy shows that monomeric polyglutamine molecules form collapsed structures in aqueous solutions.

7. Structural and functional analysis of ataxin-2 and ataxin-3.

Review 8. Polyglutamine neurodegeneration: protein misfolding revisited.

9. Aggregated polyglutamine peptides delivered to nuclei are toxic to mammalian cells.

10. Pathogenic and non-pathogenic polyglutamine tracts have similar structural properties: towards a length-dependent toxicity gradient.

1. Dynamic imaging by fluorescence correlation spectroscopy identifies diverse populations of polyglutamine oligomers formed in vivo.

Review 2. Modifiers and mechanisms of multi-system polyglutamine neurodegenerative disorders: lessons from fly models.

3. Sequence-dependent stability test of a left-handed β-helix motif.

4. Net charge per residue modulates conformational ensembles of intrinsically disordered proteins.

Review 5. Physical chemistry of polyglutamine: intriguing tales of a monotonous sequence.

6. Q&A: repeat-containing proteins.

Review 7. New pathologic mechanisms in nucleotide repeat expansion disorders.

8. Structural motif of polyglutamine amyloid fibrils discerned with mixed-isotope infrared spectroscopy.

Review 9. Fibrillogenesis of huntingtin and other glutamine containing proteins.

Review 10. Describing sequence-ensemble relationships for intrinsically disordered proteins.