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PDBsum entry 4r6t
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Hydrolase/hydrolase inhibitor
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PDB id
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4r6t
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PDB id:
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| Name: |
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Hydrolase/hydrolase inhibitor
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Title:
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Structure of the m17 leucyl aminopeptidase from malaria complexed with a hydroxamic acid-based inhibitor
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Structure:
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M17 leucyl aminopeptidase. Chain: a, b, c, d, e, f, g, h, i, j, k, l. Engineered: yes
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Source:
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Plasmodium falciparum 3d7. Organism_taxid: 36329. Gene: lap, pf14_0439. Expressed in: escherichia coli. Expression_system_taxid: 511693.
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Resolution:
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2.60Å
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R-factor:
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0.214
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R-free:
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0.269
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Authors:
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N.Drinkwater,S.Mcgowan
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Key ref:
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S.N.Mistry
et al.
(2014).
Two-pronged attack: dual inhibition of Plasmodium falciparum M1 and M17 metalloaminopeptidases by a novel series of hydroxamic acid-based inhibitors.
J Med Chem,
57,
9168-9183.
PubMed id:
DOI:
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Date:
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26-Aug-14
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Release date:
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29-Oct-14
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PROCHECK
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Headers
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References
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Q8IL11
(Q8IL11_PLAF7) -
Leucine aminopeptidase from Plasmodium falciparum (isolate 3D7)
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Seq:
Struc:
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605 a.a.
514 a.a.*
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Key: |
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PfamA domain |
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Secondary structure |
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CATH domain |
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*
PDB and UniProt seqs differ
at 3 residue positions (black
crosses)
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Enzyme class 2:
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E.C.3.4.11.1
- leucyl aminopeptidase.
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Reaction:
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Release of an N-terminal amino acid, Xaa-|-Xbb-, in which Xaa is preferably Leu, but may be other amino acids including Pro although not Arg or Lys, and Xbb may be Pro.
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Cofactor:
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Zn(2+)
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Enzyme class 3:
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E.C.3.4.13.-
- ?????
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Note, where more than one E.C. class is given (as above), each may
correspond to a different protein domain or, in the case of polyprotein
precursors, to a different mature protein.
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DOI no:
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J Med Chem
57:9168-9183
(2014)
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PubMed id:
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Two-pronged attack: dual inhibition of Plasmodium falciparum M1 and M17 metalloaminopeptidases by a novel series of hydroxamic acid-based inhibitors.
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S.N.Mistry,
N.Drinkwater,
C.Ruggeri,
K.K.Sivaraman,
S.Loganathan,
S.Fletcher,
M.Drag,
A.Paiardini,
V.M.Avery,
P.J.Scammells,
S.McGowan.
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ABSTRACT
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Plasmodium parasites, the causative agents of malaria, have developed resistance
to most of our current antimalarial therapies, including artemisinin combination
therapies which are widely described as our last line of defense. Antimalarial
agents with a novel mode of action are urgently required. Two Plasmodium
falciparum aminopeptidases, PfA-M1 and PfA-M17, play crucial roles in the
erythrocytic stage of infection and have been validated as potential
antimalarial targets. Using compound-bound crystal structures of both enzymes,
we have used a structure-guided approach to develop a novel series of inhibitors
capable of potent inhibition of both PfA-M1 and PfA-M17 activity and parasite
growth in culture. Herein we describe the design, synthesis, and evaluation of a
series of hydroxamic acid-based inhibitors and demonstrate the compounds to be
exciting new leads for the development of novel antimalarial therapeutics.
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Links
