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* Residue conservation analysis
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PDB id:
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Immune system
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Title:
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Catalytic elimination antibody 34e4 in complex with hapten
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Structure:
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Catalytic antibody fab 34e4 light chain. Chain: l, a, c, e. Engineered: yes. Other_details: the variable domain (residues 1-107) is from a murine source and the constant domain (residues 108-214) is from a human source.. Catalytic antibody fab 34e4 heavy chain. Chain: h, b, d, f. Engineered: yes.
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Source:
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Mus musculus, homo sapiens. House mouse, human. Organism_taxid: 10090,9606. Strain: ,. Expressed in: escherichia coli. Expression_system_taxid: 562.
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Biol. unit:
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Tetramer (from
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Resolution:
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2.50Å
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R-factor:
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0.204
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R-free:
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0.240
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Authors:
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E.W.Debler,S.Ito,A.Heine,I.A.Wilson
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Key ref:
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E.W.Debler
et al.
(2005).
Structural origins of efficient proton abstraction from carbon by a catalytic antibody.
Proc Natl Acad Sci U S A,
102,
4984-4989.
PubMed id:
DOI:
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Date:
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15-Nov-04
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Release date:
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05-Apr-05
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PROCHECK
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Headers
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References
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DOI no:
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Proc Natl Acad Sci U S A
102:4984-4989
(2005)
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PubMed id:
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Structural origins of efficient proton abstraction from carbon by a catalytic antibody.
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E.W.Debler,
S.Ito,
F.P.Seebeck,
A.Heine,
D.Hilvert,
I.A.Wilson.
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ABSTRACT
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Antibody 34E4 catalyzes the conversion of benzisoxazoles to salicylonitriles
with high rates and multiple turnovers. The crystal structure of its complex
with the benzimidazolium hapten at 2.5-angstroms resolution shows that a
combination of hydrogen bonding, pi stacking, and van der Waals interactions is
exploited to position both the base, Glu(H50), and the substrate for efficient
proton transfer. Suboptimal placement of the catalytic carboxylate, as observed
in the 2.8-angstroms structure of the Glu(H50)Asp variant, results in
substantially reduced catalytic efficiency. In addition to imposing high
positional order on the transition state, the antibody pocket provides a highly
structured microenvironment for the reaction in which the carboxylate base is
activated through partial desolvation, and the highly polarizable transition
state is stabilized by dispersion interactions with the aromatic residue
Trp(L91) and solvation of the leaving group oxygen by external water. The
enzyme-like efficiency of general base catalysis in this system directly
reflects the original hapten design, in which a charged guanidinium moiety was
strategically used to elicit an accurately positioned functional group in an
appropriate reaction environment and suggests that even larger catalytic effects
may be achievable by extending this approach to the induction of acid-base pairs
capable of bifunctional catalysis.
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Selected figure(s)
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Figure 2.
Fig. 2. Antibody-combining site of 34E4 bound to hapten.
The heavy and light chains are colored in blue and green,
respectively. Two of the active-site water molecules are
designated S1 and S21. The 3F[o]-2F[c]  [A]-weighted electron
density map around the hapten and key active-site residues is
contoured at 1.3 . Hydrogen bonds are
shown as broken lines. TrpL91 forms a cation-  interaction
with the guanidinium moiety of the hapten. CDR H3 is omitted for
clarity.
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Figure 4.
Fig. 4. Stereoview of the antibody-combining site of the
34E4-hapten complex. Hydrogen bonds are shown as broken lines,
and heavy and light chains are colored in blue and green,
respectively. The hapten is sandwiched between two aromatic
residues TrpL91 and TyrH100D. GluH50 forms a bidentate salt
bridge to the guanidinium moiety of the hapten. The CDRs of the
light and heavy chains are labeled L1-L3 and H1-H3, respectively.
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Figures were
selected
by an automated process.
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Literature references that cite this PDB file's key reference
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PubMed id
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Reference
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I.V.Korendovych,
D.W.Kulp,
Y.Wu,
H.Cheng,
H.Roder,
and
W.F.DeGrado
(2011).
Design of a switchable eliminase.
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Proc Natl Acad Sci U S A,
108,
6823-6827.
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PDB code:
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G.Kiss,
D.Röthlisberger,
D.Baker,
and
K.N.Houk
(2010).
Evaluation and ranking of enzyme designs.
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Protein Sci,
19,
1760-1773.
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M.P.Frushicheva,
J.Cao,
Z.T.Chu,
and
A.Warshel
(2010).
Exploring challenges in rational enzyme design by simulating the catalysis in artificial kemp eliminase.
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Proc Natl Acad Sci U S A,
107,
16869-16874.
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A.N.Alexandrova,
and
W.L.Jorgensen
(2009).
Origin of the activity drop with the E50D variant of catalytic antibody 34E4 for Kemp elimination.
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J Phys Chem B,
113,
497-504.
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E.W.Debler,
R.Müller,
D.Hilvert,
and
I.A.Wilson
(2009).
An aspartate and a water molecule mediate efficient acid-base catalysis in a tailored antibody pocket.
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Proc Natl Acad Sci U S A,
106,
18539-18544.
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PDB codes:
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D.Röthlisberger,
O.Khersonsky,
A.M.Wollacott,
L.Jiang,
J.DeChancie,
J.Betker,
J.L.Gallaher,
E.A.Althoff,
A.Zanghellini,
O.Dym,
S.Albeck,
K.N.Houk,
D.S.Tawfik,
and
D.Baker
(2008).
Kemp elimination catalysts by computational enzyme design.
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Nature,
453,
190-195.
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PDB code:
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E.W.Debler,
R.Müller,
D.Hilvert,
and
I.A.Wilson
(2008).
Conformational isomerism can limit antibody catalysis.
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J Biol Chem,
283,
16554-16560.
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PDB codes:
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P.A.Sigala,
D.A.Kraut,
J.M.Caaveiro,
B.Pybus,
E.A.Ruben,
D.Ringe,
G.A.Petsko,
and
D.Herschlag
(2008).
Testing geometrical discrimination within an enzyme active site: constrained hydrogen bonding in the ketosteroid isomerase oxyanion hole.
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J Am Chem Soc,
130,
13696-13708.
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PDB codes:
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T.Tuttle,
and
W.Thiel
(2008).
OMx-D: semiempirical methods with orthogonalization and dispersion corrections. Implementation and biochemical application.
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Phys Chem Chem Phys,
10,
2159-2166.
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E.W.Debler,
G.F.Kaufmann,
R.N.Kirchdoerfer,
J.M.Mee,
K.D.Janda,
and
I.A.Wilson
(2007).
Crystal structures of a quorum-quenching antibody.
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J Mol Biol,
368,
1392-1402.
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PDB codes:
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P.C.Ke
(2007).
Fiddling the string of carbon nanotubes with amphiphiles.
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Phys Chem Chem Phys,
9,
439-447.
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D.A.Kraut,
P.A.Sigala,
B.Pybus,
C.W.Liu,
D.Ringe,
G.A.Petsko,
and
D.Herschlag
(2006).
Testing electrostatic complementarity in enzyme catalysis: hydrogen bonding in the ketosteroid isomerase oxyanion hole.
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PLoS Biol,
4,
e99.
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PDB codes:
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The most recent references are shown first.
Citation data come partly from CiteXplore and partly
from an automated harvesting procedure. Note that this is likely to be
only a partial list as not all journals are covered by
either method. However, we are continually building up the citation data
so more and more references will be included with time.
Where a reference describes a PDB structure, the PDB
code is
shown on the right.
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Links
