Site-directed <it>in vitro </it>immunization leads to a complete human monoclonal IgG4λ that binds specifically to the CDR2 region of CTLA-4 (CD152) without interfering the engagement of natural ligands

Site-directed <it>in vitro </it>immunization leads to a complete human monoclonal IgG4λ that binds specifically to the CDR2 region of CTLA-4 (CD152) without interfering the engagement of natural ligands

<p>Abstract</p> <p>Background</p> <p>The ability to acquire fully human monoclonal antibodies (mAbs) with pre-defined specificities is critical to the development of molecular tags for the analysis of receptor function in addition to promising immunotherapeutics. Yet mo...

Full description

Bibliographic Details
Main Authors: Hsu Shu-Ching, Chen Han-Min, Chu Chishih, Chin Li-Te, Weng Bor-Chun, Chu Chi-Hong
Format: Article
Language:English
Published: BMC 2007-08-01
Series:BMC Biotechnology
Online Access:http://www.biomedcentral.com/1472-6750/7/51
id doaj-8b0505ced79341bf9193676b5d24fb5c
record_format Article
spelling doaj-8b0505ced79341bf9193676b5d24fb5c2020-11-25T03:49:34ZengBMCBMC Biotechnology1472-67502007-08-01715110.1186/1472-6750-7-51Site-directed <it>in vitro </it>immunization leads to a complete human monoclonal IgG4λ that binds specifically to the CDR2 region of CTLA-4 (CD152) without interfering the engagement of natural ligandsHsu Shu-ChingChen Han-MinChu ChishihChin Li-TeWeng Bor-ChunChu Chi-Hong<p>Abstract</p> <p>Background</p> <p>The ability to acquire fully human monoclonal antibodies (mAbs) with pre-defined specificities is critical to the development of molecular tags for the analysis of receptor function in addition to promising immunotherapeutics. Yet most of the arriving affinity maturated and complete human immunoglobulin G (IgG) molecules, which are actually derived from single human B cells, have not widely been used to study the conserved self antigens (Ags) such as CD152 (cytotoxic T lymphocyte antigen-4, CTLA-4) because proper hosts are lacking.</p> <p>Results</p> <p>Here we developed an optimized protocol for site-directed <it>in vitro </it>immunizing peripheral blood mononuclear cells (PBMC) by using a selected epitope of human CD152, an essential receptor involved in down-regulation of T cell activation. The resultant stable trioma cell lines constantly produce anti-CD152 mAb (γ4λhuCD152), which contains variable (V) regions of the heavy chain and the light chain derived from the VH3 and Vλ human germline genes, respectively, and yet displays an unusual IgG4 isotype. Interestingly, γ4λhuCD152 has a basic pI not commonly found in myeloid monoclonal IgG4λs as revealed by the isoelectric focusing (IEF) analysis. Furthermore, γ4λhuCD152 binds specifically, with nanomolar affinity, to an extracellular constituency encompassing the putative second complementarity determining region (CDR2) of CD152, whereby it can react to activated CD3<sup>+ </sup>cells.</p> <p>Conclusion</p> <p>In a context of specific cell depletion and conditioned medium,<it>in vitro </it>induction of human Abs against a conserved self Ag was successfully acquired and a relatively basic mAb, γ4λhuCD152, with high affinity to CDR2 of CD152 was thus obtained. Application of such a human IgG4λ mAb with designated CDR2 specificity may impact upon and prefer for CD152 labeling both <it>in situ </it>and <it>ex situ</it>, as it does not affect the binding of endogenous B7 ligands and can localize into the confined immunological synapse which may otherwise prevent the access of whole IgG1 molecules.</p> http://www.biomedcentral.com/1472-6750/7/51
collection DOAJ
language English
format Article
sources DOAJ
author Hsu Shu-Ching
Chen Han-Min
Chu Chishih
Chin Li-Te
Weng Bor-Chun
Chu Chi-Hong
spellingShingle Hsu Shu-Ching
Chen Han-Min
Chu Chishih
Chin Li-Te
Weng Bor-Chun
Chu Chi-Hong
Site-directed <it>in vitro </it>immunization leads to a complete human monoclonal IgG4λ that binds specifically to the CDR2 region of CTLA-4 (CD152) without interfering the engagement of natural ligands
BMC Biotechnology
author_facet Hsu Shu-Ching
Chen Han-Min
Chu Chishih
Chin Li-Te
Weng Bor-Chun
Chu Chi-Hong
author_sort Hsu Shu-Ching
title Site-directed <it>in vitro </it>immunization leads to a complete human monoclonal IgG4λ that binds specifically to the CDR2 region of CTLA-4 (CD152) without interfering the engagement of natural ligands
title_short Site-directed <it>in vitro </it>immunization leads to a complete human monoclonal IgG4λ that binds specifically to the CDR2 region of CTLA-4 (CD152) without interfering the engagement of natural ligands
title_full Site-directed <it>in vitro </it>immunization leads to a complete human monoclonal IgG4λ that binds specifically to the CDR2 region of CTLA-4 (CD152) without interfering the engagement of natural ligands
title_fullStr Site-directed <it>in vitro </it>immunization leads to a complete human monoclonal IgG4λ that binds specifically to the CDR2 region of CTLA-4 (CD152) without interfering the engagement of natural ligands
title_full_unstemmed Site-directed <it>in vitro </it>immunization leads to a complete human monoclonal IgG4λ that binds specifically to the CDR2 region of CTLA-4 (CD152) without interfering the engagement of natural ligands
title_sort site-directed <it>in vitro </it>immunization leads to a complete human monoclonal igg4λ that binds specifically to the cdr2 region of ctla-4 (cd152) without interfering the engagement of natural ligands
publisher BMC
series BMC Biotechnology
issn 1472-6750
publishDate 2007-08-01
description <p>Abstract</p> <p>Background</p> <p>The ability to acquire fully human monoclonal antibodies (mAbs) with pre-defined specificities is critical to the development of molecular tags for the analysis of receptor function in addition to promising immunotherapeutics. Yet most of the arriving affinity maturated and complete human immunoglobulin G (IgG) molecules, which are actually derived from single human B cells, have not widely been used to study the conserved self antigens (Ags) such as CD152 (cytotoxic T lymphocyte antigen-4, CTLA-4) because proper hosts are lacking.</p> <p>Results</p> <p>Here we developed an optimized protocol for site-directed <it>in vitro </it>immunizing peripheral blood mononuclear cells (PBMC) by using a selected epitope of human CD152, an essential receptor involved in down-regulation of T cell activation. The resultant stable trioma cell lines constantly produce anti-CD152 mAb (γ4λhuCD152), which contains variable (V) regions of the heavy chain and the light chain derived from the VH3 and Vλ human germline genes, respectively, and yet displays an unusual IgG4 isotype. Interestingly, γ4λhuCD152 has a basic pI not commonly found in myeloid monoclonal IgG4λs as revealed by the isoelectric focusing (IEF) analysis. Furthermore, γ4λhuCD152 binds specifically, with nanomolar affinity, to an extracellular constituency encompassing the putative second complementarity determining region (CDR2) of CD152, whereby it can react to activated CD3<sup>+ </sup>cells.</p> <p>Conclusion</p> <p>In a context of specific cell depletion and conditioned medium,<it>in vitro </it>induction of human Abs against a conserved self Ag was successfully acquired and a relatively basic mAb, γ4λhuCD152, with high affinity to CDR2 of CD152 was thus obtained. Application of such a human IgG4λ mAb with designated CDR2 specificity may impact upon and prefer for CD152 labeling both <it>in situ </it>and <it>ex situ</it>, as it does not affect the binding of endogenous B7 ligands and can localize into the confined immunological synapse which may otherwise prevent the access of whole IgG1 molecules.</p>
url http://www.biomedcentral.com/1472-6750/7/51
work_keys_str_mv AT hsushuching sitedirecteditinvitroitimmunizationleadstoacompletehumanmonoclonaligg4lthatbindsspecificallytothecdr2regionofctla4cd152withoutinterferingtheengagementofnaturalligands
AT chenhanmin sitedirecteditinvitroitimmunizationleadstoacompletehumanmonoclonaligg4lthatbindsspecificallytothecdr2regionofctla4cd152withoutinterferingtheengagementofnaturalligands
AT chuchishih sitedirecteditinvitroitimmunizationleadstoacompletehumanmonoclonaligg4lthatbindsspecificallytothecdr2regionofctla4cd152withoutinterferingtheengagementofnaturalligands
AT chinlite sitedirecteditinvitroitimmunizationleadstoacompletehumanmonoclonaligg4lthatbindsspecificallytothecdr2regionofctla4cd152withoutinterferingtheengagementofnaturalligands
AT wengborchun sitedirecteditinvitroitimmunizationleadstoacompletehumanmonoclonaligg4lthatbindsspecificallytothecdr2regionofctla4cd152withoutinterferingtheengagementofnaturalligands
AT chuchihong sitedirecteditinvitroitimmunizationleadstoacompletehumanmonoclonaligg4lthatbindsspecificallytothecdr2regionofctla4cd152withoutinterferingtheengagementofnaturalligands
_version_ 1724494712473124864

Similar Items