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3IOT

Huntingtin amino-terminal region with 17 Gln residues - crystal C92-b

Summary for 3IOT
Entry DOI10.2210/pdb3iot/pdb
Related3IO4 3IO6 3IOR 3IOU 3IOV 3IOW
DescriptorMaltose-binding periplasmic protein,Huntingtin, ZINC ION, CALCIUM ION (3 entities in total)
Functional Keywordshuntingtin, htt-ex1, hd, sugar transport, transport, apoptosis, disease mutation, nucleus, phosphoprotein, signaling protein
Biological sourceEscherichia coli (strain K12)
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Cellular locationCytoplasm: P42858
Total number of polymer chains3
Total formula weight148899.53
Authors
Kim, M.W. (deposition date: 2009-08-14, release date: 2009-09-29, Last modification date: 2023-09-06)
Primary citationKim, M.W.,Chelliah, Y.,Kim, S.W.,Otwinowski, Z.,Bezprozvanny, I.
Secondary structure of Huntingtin amino-terminal region.
Structure, 17:1205-1212, 2009
Cited by
PubMed Abstract: Huntington's disease is a genetic neurodegenerative disorder resulting from polyglutamine (polyQ) expansion (>36Q) within the first exon of Huntingtin (Htt) protein. We applied X-ray crystallography to determine the secondary structure of the first exon (EX1) of Htt17Q. The structure of Htt17Q-EX1 consists of an amino-terminal alpha helix, poly17Q region, and polyproline helix formed by the proline-rich region. The poly17Q region adopts multiple conformations in the structure, including alpha helix, random coil, and extended loop. The conformation of the poly17Q region is influenced by the conformation of neighboring protein regions, demonstrating the importance of the native protein context. We propose that the conformational flexibility of the polyQ region observed in our structure is a common characteristic of many amyloidogenic proteins. We further propose that the pathogenic polyQ expansion in the Htt protein increases the length of the random coil, which promotes aggregation and facilitates abnormal interactions with other proteins in cells.
PubMed: 19748341
DOI: 10.1016/j.str.2009.08.002
PDB entries with the same primary citation
Experimental method
X-RAY DIFFRACTION (3.5 Å)
Structure validation

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