PDBsum entry 4feb

Signaling protein

PDB id

4feb

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Contents

			Protein chain

					402 a.a.

			Metals

					_NA ×6


					_ZN ×38

			Waters ×137

PDB id:

4feb

Links

Name:

Signaling protein

Title:

Crystal structure of htt36q3h-ex1-x1-c2(beta)

Structure:

Maltose-binding periplasmic protein,huntingtin. Chain: a, b, c. Synonym: mbp,mmbp,maltodextrin-binding protein,huntington disease protein,hd protein. Engineered: yes. Mutation: yes

Source:

Escherichia coli o157:h7, homo sapiens. Human. Organism_taxid: 83334, 9606. Gene: male, z5632, ecs5017, htt, hd, it15. Expressed in: escherichia coli. Expression_system_taxid: 511693.

Resolution:

2.80Å

R-factor:

0.231

R-free:

0.275

Authors:

M.Kim

Key ref:

M.Kim (2013). Beta conformation of polyglutamine track revealed by a crystal structure of Huntingtin N-terminal region with insertion of three histidine residues. Prion, 7, 221-228. PubMed id: 23370273 DOI: 10.4161/pri.23807

Date:

29-May-12

Release date:

13-Mar-13

PROCHECK

	Headers

	References

Protein chains

P0AEY0 (MALE_ECO57) - Maltose/maltodextrin-binding periplasmic protein from Escherichia coli O157:H7

Seq: Struc:					396 a.a. 402 a.a.*

Protein chains

P42858 (HD_HUMAN) - Huntingtin from Homo sapiens

Seq: Struc:

Seq: Struc:

Seq: Struc:

Seq: Struc:

Seq: Struc:

Seq: Struc:

Seq: Struc:					3142 a.a. 402 a.a.*

Key:

PfamA domain

Secondary structure

CATH domain

* PDB and UniProt seqs differ at 10 residue positions (black crosses)

DOI no: 10.4161/pri.23807	Prion 7:221-228 (2013)
PubMed id: 23370273

Beta conformation of polyglutamine track revealed by a crystal structure of Huntingtin N-terminal region with insertion of three histidine residues.
M.Kim.

ABSTRACT

Huntington disease is an autosomal-dominant neurodegenerative disorder caused by a polyglutamine (polyQ) expansion (> 35Q) in the first exon (EX1) of huntingtin protein (Htt). mHtt protein is thought to adopt one or more toxic conformation(s) that are involved in pathogenic interactions in cells . However, the structure of mHtt is not known. Here, we present a near atomic resolution structure of mHtt36Q-EX1. To facilitate crystallization, three histidine residues (3H) were introduced within the Htt36Q stretch resulting in the sequence of Q 7HQHQHQ 27. The Htt36Q3H region adopts α-helix, loop, β-hairpin conformations. Furthermore, we observed interactions between the backbone of the Htt36Q3H β-strand with the aromatic residues mimicking putative-toxic interactions with other proteins. Our findings support previous predictions that the expanded mHtt-polyQ region adopts a β-sheet structure. Detailed structural information about mHtt improves our understanding of the pathogenic mechanisms in HD and other polyQ expansion disorders and may form the basis for rational design of small molecules that target toxic conformations of disease-causing proteins.