Humanized antibodies against CD3
First Claim
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1. A humanized antibody comprising a humanized heavy chain and humanized light chain, wherein:
- (1) the humanized heavy chain variable region comprise three complementarity determining regions (CDRS) from the mouse M291 heavy chain and a framework from a human acceptor antibody heavy chain, optionally having one or more human framework residues that interact with one of the CDRs substituted with mouse framework residues from corresponding positions in the M291 heavy chain variable region framework, and (2) the humanized light chain variable region comprises three complementarity determining regions from the mouse M291 light chain and a framework from a human acceptor antibody light chain optionally having one or more human framework residues that interact with one of the CDRs substituted with mouse framework residues from corresponding positions in the M291 light chain variable region framework; and
the humanized antibody specifically binds to a CD3 antigen on the surface of T cells, wherein the mouse M291 antibody has a heavy chain with a variable region of sequence SEQ. ID. No. 11 and a light chain with a variable region of sequence SEQ. ID. No. 9.
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Abstract
The invention provides bispecific antibodies with selective cytotoxicity against malignant B-cells. The bispecific antibodies bind to an effector cell antigen and to a 28/32 kDa heterodimeric protein on the surface of malignant B-cells. The invention also includes the monospecific components of the bispecific antibodies, humanized versions thereof, and humanized bispecific antibodies. The invention further provides therapeutic and diagnostic methods employing these antibodies.
44 Citations
9 Claims
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1. A humanized antibody comprising a humanized heavy chain and humanized light chain, wherein:
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(1) the humanized heavy chain variable region comprise three complementarity determining regions (CDRS) from the mouse M291 heavy chain and a framework from a human acceptor antibody heavy chain, optionally having one or more human framework residues that interact with one of the CDRs substituted with mouse framework residues from corresponding positions in the M291 heavy chain variable region framework, and (2) the humanized light chain variable region comprises three complementarity determining regions from the mouse M291 light chain and a framework from a human acceptor antibody light chain optionally having one or more human framework residues that interact with one of the CDRs substituted with mouse framework residues from corresponding positions in the M291 light chain variable region framework; and
the humanized antibody specifically binds to a CD3 antigen on the surface of T cells, wherein the mouse M291 antibody has a heavy chain with a variable region of sequence SEQ. ID. No. 11 and a light chain with a variable region of sequence SEQ. ID. No. 9. - View Dependent Claims (2, 3, 4, 5, 6, 7)
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8. A humanized antibody that specifically binds to a CD3 antigen on the surface of T cells, comprising a pair of humanized heavy chains and humanized light chains, wherein the humanized light chain variable region comprises the amino acid sequence of
FIG. 5A (upper lines) (SEQ. ID. No. 8) and the humanized heavy chain variable region comprises the amino acid sequence ofFIG. 5B (upper lines) (SEQ. ID. No. 10).
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9. A bispecific antibody comprising;
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a first Fab′
fragment comprising the humanized heavy chain variable region comprises the amino acid sequence ofFIG. 5B (upper lines) (SEQ. ID. No.
10) and the humanized light chain variable region comprises the amino acid sequence ofFIG. 5A (upper lines) (SEQ. ID. No.
8),a second Fab′
fragment comprising the heavy chain variable region shown inFIG. 4B (upper) (SEQ ID NO.
3) and the light chain variable region shown inFIG. 4A (upper) (SEQ ID NO.
1)wherein the first Fab′
fragment specifically binds to the CD3 antigen and the second Fab′
fragment specifically binds to the 28/32 kDa heterodimeric antigen on the surface of the malignant B cells.
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Specification