ISDA: 2CIO

Deposition Date 2006-03-24

Release Date 2006-05-18

Last Version Date 2023-12-13

Entry Detail

PDB ID:

2CIO

Keywords:

HYDROLASE/INHIBITOR

Title:

The high resolution x-ray structure of papain complexed with fragments of the Trypanosoma brucei cysteine protease inhibitor ICP.

Biological Source:

Source Organism(s):

TRYPANOSOMA BRUCEI (Taxon ID: 5691)
CARICA PAPAYA (Taxon ID: 3649)

Expression System(s):

Escherichia coli bl21(de3)

Method Details:

Experimental Method:

X-RAY DIFFRACTION

Resolution:

1.50 Å

R-Value Free:

0.22

R-Value Work:

0.17

R-Value Observed:

0.17

Space Group:

P 21 21 21

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Macromolecular Entities

Structures with similar UniProt ID

Protein Blast

Polymer Type:polypeptide(L)
Molecule:PAPAIN
Chain IDs:A
Chain Length:212
Number of Molecules:1
Biological Source:CARICA PAPAYA

UniProt ID:P00784 Pfam ID:PF00112 EC:3.4.22.2

Structures with similar UniProt ID

Protein Blast

Polymer Type:polypeptide(L)
Molecule:INHIBITOR OF CYSTEINE PEPTIDA
Gene (Uniprot):ICP
Chain IDs:B
Chain Length:121
Number of Molecules:1
Biological Source:TRYPANOSOMA BRUCEI

UniProt ID:Q868H0 Pfam ID:PF09394

Modified Residue

Compound ID	Chain ID	Parent Comp ID	Details	2D Image
OCS	A	CYS	CYSTEINESULFONIC ACID

Ligand Molecules

ACT

GOL

Primary Citation

High-Resolution Complex of Papain with Remnants of a Cysteine Protease Inhibitor Derived from Trypanosoma Brucei

Alphey, M.S, Hunter, W.N.Show

Acta Crystallogr. Sect. F Struct. Biol. Cryst. Commun. 62 504 ? (2006)

PMID: 16754967 DOI: 10.1107/S1744309106014849

Abstact

Attempts to cocrystallize the cysteine protease papain derived from the latex of Carica papaya with an inhibitor of cysteine proteases (ICP) from Trypanosoma brucei were unsuccessful. However, crystals of papain that diffracted to higher resolution, 1.5 A, than other crystals of this archetypal cysteine protease were obtained, so the analysis was continued. Surprisingly, the substrate-binding cleft was occupied by two short peptide fragments which have been assigned as remnants of ICP. Comparisons reveal that these peptides bind in the active site in a manner similar to that of the human cysteine protease inhibitor stefin B when it is complexed to papain. The assignment of the fragment sequences is consistent with the specificity of the protease.

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Protein

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Primary Citation of related structures

Abstact

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