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PDBsum entry 1fvd
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Immunoglobulin
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PDB id
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1fvd
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Contents |
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* Residue conservation analysis
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References listed in PDB file
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Key reference
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Title
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X-Ray structures of the antigen-Binding domains from three variants of humanized anti-P185her2 antibody 4d5 and comparison with molecular modeling.
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Authors
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C.Eigenbrot,
M.Randal,
L.Presta,
P.Carter,
A.A.Kossiakoff.
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Ref.
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J Mol Biol, 1993,
229,
969-995.
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PubMed id
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Abstract
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The X-ray structures of 1 Fv and 2 Fab humanized anti-p185HER2 antibody
fragments (IgG1-kappa) have been determined at a resolution between 2.7 A and
2.2 A. The antibodies are three different versions of a human antibody framework
onto which the antigen recognition loops from a murine antibody (4D5) have been
grafted. The sequences of the three versions differ in the framework region at
positions L55, H78 and H102. The version 8 Fv fragment crystallizes in space
group P2(1) with cell parameters a = 37.6 A, b = 63.4 A, c = 90.2 A, beta = 98.2
degrees, with two molecules per asymmetric unit, and has been refined against
data 10.0 A-2.2 A to an R-factor of 18.3%. Versions 4 and 7 Fabs crystallize in
space group P1 with cell parameters a = 39.2 A, b = 80.2 A, c = 86.1 A, alpha =
113.1 degrees, beta = 92.7 A, gamma = 102.6 A and two molecules per asymmetric
unit. Version 4 has been refined against data 10.0 A-2.5 A resolution to an
R-factor of 17.9%. Version 7 has been refined against data 10 A-2.7 A to an
R-factor of 17.1%. The X-ray structures have been used to assess the accuracy of
structural predictions made via molecular modeling, and they confirm the
structural role of certain framework residues and the conformations of five of
six complementarity determining regions (CDRS). The average deviation of the
model from the X-ray structures is within the range observed among the X-ray
structures for 81% of the C alpha atoms. Of the hydrogen bonds common to the
X-ray structures, 94% of the main-chain-main-chain and 79% of the
main-chain-side-chain ones were predicted by the model. The side-chain
conformation was predicted correctly for 79% of the buried residues. The third
CDR in the heavy chain is variable, differing by up to 8 A between molecules
within an asymmetric unit. The structural relationship between variable domains
of light and heavy chains is not significantly altered by the absence of
constant domains in the Fv molecule. The antigen-binding potential of an unusual
light chain sequence has been confirmed. The arginine at position 66 interacts
with the first light chain CDR, but in a fashion somewhat different than
predicted. A substitution of a leucine for an alanine side-chain directed
between the beta-sheets has only relatively small and local effects.(ABSTRACT
TRUNCATED AT 400 WORDS)
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Secondary reference #1
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Title
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Humanization of an anti-P185her2 antibody for human cancer therapy.
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Authors
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P.Carter,
L.Presta,
C.M.Gorman,
J.B.Ridgway,
D.Henner,
W.L.Wong,
A.M.Rowland,
C.Kotts,
M.E.Carver,
H.M.Shepard.
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Ref.
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Proc Natl Acad Sci U S A, 1992,
89,
4285-4289.
[DOI no: ]
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PubMed id
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