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The CEA/CD3-Bispecific Antibody MEDI-565 (MT111) Binds a Nonlinear Epitope in the Full-Length but Not a Short Splice Variant of CEA
by
Oberst, Michael D.
, Wu, Herren
, Lekstrom, Kristen
, Brohawn, Philip
, Baeuerle, Patrick A.
, Coats, Steven R.
, Hammond, Scott A.
, Peng, Li
, Morehouse, Chris
, Dall’Acqua, William
, Huang, Jiaqi
, Damschroder, Melissa
, Yao, Yihong
in
Adult
/ Aged
/ Alternative splicing
/ Amino Acid Sequence
/ Amino acids
/ Animals
/ Antibodies
/ Antibodies, Bispecific - immunology
/ Antibodies, Monoclonal, Humanized - immunology
/ Antibody Specificity
/ Antigenic determinants
/ Antigens
/ Biology
/ Biotechnology
/ Bispecific antibodies
/ Cancer
/ Cancer treatment
/ Carcinoembryonic antigen
/ Carcinoembryonic Antigen - chemistry
/ Carcinoembryonic Antigen - genetics
/ Carcinoembryonic Antigen - immunology
/ CD3 antigen
/ CD3 Complex - immunology
/ Cell adhesion & migration
/ CHO Cells
/ Colorectal cancer
/ Cricetinae
/ Cricetulus
/ Data processing
/ Engineering
/ Epitope Mapping
/ Epitopes
/ Epitopes - immunology
/ Gene Expression Regulation, Neoplastic
/ HEK293 Cells
/ Homology
/ Homozygosity
/ Humans
/ Immunoglobulins
/ Immunology
/ Li Peng
/ Lymphocytes
/ Lymphocytes T
/ Medical prognosis
/ Medicine
/ Mice
/ Middle Aged
/ Models, Molecular
/ Molecular Sequence Data
/ mRNA
/ Mutagenesis
/ Neoplasms - genetics
/ Neoplasms - pathology
/ Neuroendocrine tumors
/ Polymerase chain reaction
/ Polypeptides
/ Protein Isoforms - chemistry
/ Protein Isoforms - genetics
/ Protein Isoforms - immunology
/ Protein Structure, Tertiary
/ Proteins
/ RNA, Messenger - genetics
/ RNA, Messenger - metabolism
/ Single nucleotide polymorphisms
/ Single-nucleotide polymorphism
/ T cell receptors
/ T cells
/ T-Lymphocytes - cytology
/ T-Lymphocytes - immunology
/ Tumors
/ Young Adult
2012
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The CEA/CD3-Bispecific Antibody MEDI-565 (MT111) Binds a Nonlinear Epitope in the Full-Length but Not a Short Splice Variant of CEA
by
Oberst, Michael D.
, Wu, Herren
, Lekstrom, Kristen
, Brohawn, Philip
, Baeuerle, Patrick A.
, Coats, Steven R.
, Hammond, Scott A.
, Peng, Li
, Morehouse, Chris
, Dall’Acqua, William
, Huang, Jiaqi
, Damschroder, Melissa
, Yao, Yihong
in
Adult
/ Aged
/ Alternative splicing
/ Amino Acid Sequence
/ Amino acids
/ Animals
/ Antibodies
/ Antibodies, Bispecific - immunology
/ Antibodies, Monoclonal, Humanized - immunology
/ Antibody Specificity
/ Antigenic determinants
/ Antigens
/ Biology
/ Biotechnology
/ Bispecific antibodies
/ Cancer
/ Cancer treatment
/ Carcinoembryonic antigen
/ Carcinoembryonic Antigen - chemistry
/ Carcinoembryonic Antigen - genetics
/ Carcinoembryonic Antigen - immunology
/ CD3 antigen
/ CD3 Complex - immunology
/ Cell adhesion & migration
/ CHO Cells
/ Colorectal cancer
/ Cricetinae
/ Cricetulus
/ Data processing
/ Engineering
/ Epitope Mapping
/ Epitopes
/ Epitopes - immunology
/ Gene Expression Regulation, Neoplastic
/ HEK293 Cells
/ Homology
/ Homozygosity
/ Humans
/ Immunoglobulins
/ Immunology
/ Li Peng
/ Lymphocytes
/ Lymphocytes T
/ Medical prognosis
/ Medicine
/ Mice
/ Middle Aged
/ Models, Molecular
/ Molecular Sequence Data
/ mRNA
/ Mutagenesis
/ Neoplasms - genetics
/ Neoplasms - pathology
/ Neuroendocrine tumors
/ Polymerase chain reaction
/ Polypeptides
/ Protein Isoforms - chemistry
/ Protein Isoforms - genetics
/ Protein Isoforms - immunology
/ Protein Structure, Tertiary
/ Proteins
/ RNA, Messenger - genetics
/ RNA, Messenger - metabolism
/ Single nucleotide polymorphisms
/ Single-nucleotide polymorphism
/ T cell receptors
/ T cells
/ T-Lymphocytes - cytology
/ T-Lymphocytes - immunology
/ Tumors
/ Young Adult
2012
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The CEA/CD3-Bispecific Antibody MEDI-565 (MT111) Binds a Nonlinear Epitope in the Full-Length but Not a Short Splice Variant of CEA
by
Oberst, Michael D.
, Wu, Herren
, Lekstrom, Kristen
, Brohawn, Philip
, Baeuerle, Patrick A.
, Coats, Steven R.
, Hammond, Scott A.
, Peng, Li
, Morehouse, Chris
, Dall’Acqua, William
, Huang, Jiaqi
, Damschroder, Melissa
, Yao, Yihong
in
Adult
/ Aged
/ Alternative splicing
/ Amino Acid Sequence
/ Amino acids
/ Animals
/ Antibodies
/ Antibodies, Bispecific - immunology
/ Antibodies, Monoclonal, Humanized - immunology
/ Antibody Specificity
/ Antigenic determinants
/ Antigens
/ Biology
/ Biotechnology
/ Bispecific antibodies
/ Cancer
/ Cancer treatment
/ Carcinoembryonic antigen
/ Carcinoembryonic Antigen - chemistry
/ Carcinoembryonic Antigen - genetics
/ Carcinoembryonic Antigen - immunology
/ CD3 antigen
/ CD3 Complex - immunology
/ Cell adhesion & migration
/ CHO Cells
/ Colorectal cancer
/ Cricetinae
/ Cricetulus
/ Data processing
/ Engineering
/ Epitope Mapping
/ Epitopes
/ Epitopes - immunology
/ Gene Expression Regulation, Neoplastic
/ HEK293 Cells
/ Homology
/ Homozygosity
/ Humans
/ Immunoglobulins
/ Immunology
/ Li Peng
/ Lymphocytes
/ Lymphocytes T
/ Medical prognosis
/ Medicine
/ Mice
/ Middle Aged
/ Models, Molecular
/ Molecular Sequence Data
/ mRNA
/ Mutagenesis
/ Neoplasms - genetics
/ Neoplasms - pathology
/ Neuroendocrine tumors
/ Polymerase chain reaction
/ Polypeptides
/ Protein Isoforms - chemistry
/ Protein Isoforms - genetics
/ Protein Isoforms - immunology
/ Protein Structure, Tertiary
/ Proteins
/ RNA, Messenger - genetics
/ RNA, Messenger - metabolism
/ Single nucleotide polymorphisms
/ Single-nucleotide polymorphism
/ T cell receptors
/ T cells
/ T-Lymphocytes - cytology
/ T-Lymphocytes - immunology
/ Tumors
/ Young Adult
2012
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The CEA/CD3-Bispecific Antibody MEDI-565 (MT111) Binds a Nonlinear Epitope in the Full-Length but Not a Short Splice Variant of CEA
Journal Article
The CEA/CD3-Bispecific Antibody MEDI-565 (MT111) Binds a Nonlinear Epitope in the Full-Length but Not a Short Splice Variant of CEA
2012
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Overview
MEDI-565 (also known as MT111) is a bispecific T-cell engager (BiTE®) antibody in development for the treatment of patients with cancers expressing carcinoembryonic antigen (CEA). MEDI-565 binds CEA on cancer cells and CD3 on T cells to induce T-cell mediated killing of cancer cells. To understand the molecular basis of human CEA recognition by MEDI-565 and how polymorphisms and spliced forms of CEA may affect MEDI-565 activity, we mapped the epitope of MEDI-565 on CEA using mutagenesis and homology modeling approaches. We found that MEDI-565 recognized a conformational epitope in the A2 domain comprised of amino acids 326-349 and 388-410, with critical residues F(326), T(328), N(333), V(388), G(389), P(390), E(392), I(408), and N(410). Two non-synonymous single-nucleotide polymorphisms (SNPs) (rs10407503, rs7249230) were identified in the epitope region, but they are found at low homozygosity rates. Searching the National Center for Biotechnology Information GenBank® database, we further identified a single, previously uncharacterized mRNA splice variant of CEA that lacks a portion of the N-terminal domain, the A1 and B1 domains, and a large portion of the A2 domain. Real-time quantitative polymerase chain reaction analysis of multiple cancers showed widespread expression of full-length CEA in these tumors, with less frequent but concordant expression of the CEA splice variant. Because the epitope was largely absent from the CEA splice variant, MEDI-565 did not bind or mediate T-cell killing of cells solely expressing this form of CEA. In addition, the splice variant did not interfere with MEDI-565 binding or activity when co-expressed with full-length CEA. Thus MEDI-565 may broadly target CEA-positive tumors without regard for expression of the short splice variant of CEA. Together our data suggest that MEDI-565 activity will neither be impacted by SNPs nor by a splice variant of CEA.
Publisher
Public Library of Science,Public Library of Science (PLoS)
Subject
/ Aged
/ Animals
/ Antibodies, Bispecific - immunology
/ Antibodies, Monoclonal, Humanized - immunology
/ Antigens
/ Biology
/ Cancer
/ Carcinoembryonic Antigen - chemistry
/ Carcinoembryonic Antigen - genetics
/ Carcinoembryonic Antigen - immunology
/ Epitopes
/ Gene Expression Regulation, Neoplastic
/ Homology
/ Humans
/ Li Peng
/ Medicine
/ Mice
/ mRNA
/ Protein Isoforms - chemistry
/ Protein Isoforms - immunology
/ Proteins
/ Single nucleotide polymorphisms
/ Single-nucleotide polymorphism
/ T cells
/ Tumors
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