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PDBsum entry 4zy2
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Hydrolase/hydrolase inhibitor
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PDB id
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4zy2
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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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X-ray crystal structure of pfa-m17 in complex with hydroxamic acid- based inhibitor 10o
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Structure:
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Probable m17 family aminopeptidase. Chain: a, b, c, d, e, f, g, h, i, j, k, l. Fragment: unp residues 84-605. Engineered: yes. Mutation: yes
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Source:
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Plasmodium falciparum fcb1/columbia. Organism_taxid: 186763. Strain: isolate fcb1 / columbia. Expressed in: escherichia coli. Expression_system_taxid: 511693.
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Resolution:
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2.10Å
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R-factor:
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0.196
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R-free:
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0.239
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Authors:
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N.Drinkwater,S.Mcgowan
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Key ref:
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N.Drinkwater
et al.
(2016).
Potent dual inhibitors of Plasmodium falciparum M1 and M17 aminopeptidases through optimization of S1 pocket interactions.
Eur J Med Chem,
110,
43-64.
PubMed id:
DOI:
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Date:
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21-May-15
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Release date:
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30-Mar-16
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PROCHECK
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Headers
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References
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A0A0L7M119
(A0A0L7M119_PLAF4) -
leucyl aminopeptidase from Plasmodium falciparum (isolate Dd2)
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Seq:
Struc:
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606 a.a.
519 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.3.4.11.5
- prolyl aminopeptidase.
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Reaction:
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Release of a N-terminal proline from a peptide.
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Cofactor:
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Mn(2+)
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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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Eur J Med Chem
110:43-64
(2016)
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PubMed id:
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Potent dual inhibitors of Plasmodium falciparum M1 and M17 aminopeptidases through optimization of S1 pocket interactions.
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N.Drinkwater,
N.B.Vinh,
S.N.Mistry,
R.S.Bamert,
C.Ruggeri,
J.P.Holleran,
S.Loganathan,
A.Paiardini,
S.A.Charman,
A.K.Powell,
V.M.Avery,
S.McGowan,
P.J.Scammells.
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ABSTRACT
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Malaria remains a global health problem, and though international efforts for
treatment and eradication have made some headway, the emergence of
drug-resistant parasites threatens this progress. Antimalarial therapeutics
acting via novel mechanisms are urgently required. Plasmodium falciparum M1 and
M17 are neutral aminopeptidases which are essential for parasite growth and
development. Previous work in our group has identified inhibitors capable of
dual inhibition of PfA-M1 and PfA-M17, and revealed further regions within the
protease S1 pockets that could be exploited in the development of ligands with
improved inhibitory activity. Herein, we report the structure-based design and
synthesis of novel hydroxamic acid analogues that are capable of potent
inhibition of both PfA-M1 and PfA-M17. Furthermore, the developed compounds
potently inhibit Pf growth in culture, including the multi-drug resistant strain
Dd2. The ongoing development of dual PfA-M1/PfA-M17 inhibitors continues to be
an attractive strategy for the design of novel antimalarial therapeutics.
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Links
