Rapid induction of apoptosis in B-cell lymphoma by functionally isolated human antibodies

Fransson, Johan; Tornberg, UC; Borrebaeck, Carl; Carlsson, Roland; Frendeus, B

Rapid induction of apoptosis in B-cell lymphoma by functionally isolated human antibodies

Mark

Fransson, Johan ^LU ; Tornberg, UC ; Borrebaeck, Carl ^LU ; Carlsson, Roland ^LU and Frendeus, B (2006) In International Journal of Cancer 119(2). p.349-358

Abstract: Novel panning and screening methodology was devised to isolate high affinity human recombinant scFv antibody fragments with functionally associated properties in B lymphoma cells. The approach was used to generate a panel of apoptosis-inducing antibodies specific for antigens differentially expressed in B lymphoma vs. T leukaemia cells. The selections resulted in an antibody pool with near perfect selectivity (> 99%) for the B lymphoma target cells. Randomly picked clones (72) revealed 7 unique antibody genotypes. Six of these rapidly induced apoptosis in target cells. Following the conversion to full IgGs, the antibodies were shown to be specific for HLA-DR/DP, the B-cell receptor p chain and for CD54/ICAM-1. The latter receptor was... (More); Novel panning and screening methodology was devised to isolate high affinity human recombinant scFv antibody fragments with functionally associated properties in B lymphoma cells. The approach was used to generate a panel of apoptosis-inducing antibodies specific for antigens differentially expressed in B lymphoma vs. T leukaemia cells. The selections resulted in an antibody pool with near perfect selectivity (> 99%) for the B lymphoma target cells. Randomly picked clones (72) revealed 7 unique antibody genotypes. Six of these rapidly induced apoptosis in target cells. Following the conversion to full IgGs, the antibodies were shown to be specific for HLA-DR/DP, the B-cell receptor p chain and for CD54/ICAM-1. The latter receptor was not previously associated with apoptotic properties in B-cell lymphomas. Anti-ICAM-1 IgG induced apoptosis in a broad range of B lymphoma cell lines and were shown by immunohistochemistry to bind strongly to B lymphoma tissue obtained from 5 different B lymphoma patients. The recombinant IgG antibodies had affinities in the subnanomolar (0.3 nM) to nanomolar (3 nM) range. The described technology is generally applicable for the rapid isolation of high affinity human antibodies with specificity for differentially expressed cell surface receptors with intrinsic negative or positive signalling properties from naive phage libraries. (c) 2006 Wiley-Liss, Inc. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/406062

author

Fransson, Johan ^LU ; Tornberg, UC ; Borrebaeck, Carl ^LU ; Carlsson, Roland ^LU and Frendeus, B

organization

Department of Immunotechnology

publishing date

2006

type

Contribution to journal

publication status

published

subject

Cancer and Oncology

keywords

intercellular, apoptosis, antibody library, phage display, B lymphoma, adhesion molecule-1

in

International Journal of Cancer

volume

119

issue

2

pages

349 - 358

publisher

John Wiley & Sons Inc.

external identifiers

wos:000238267300014
pmid:16477633
scopus:33745220111

ISSN

0020-7136

DOI

10.1002/ijc.21829

language

English

LU publication?

yes

id

0a41254e-efcf-4e97-bad1-f3950d689454 (old id 406062)

date added to LUP

2016-04-01 12:31:51

date last changed

2022-01-27 06:21:56

@article{0a41254e-efcf-4e97-bad1-f3950d689454,
  abstract     = {{Novel panning and screening methodology was devised to isolate high affinity human recombinant scFv antibody fragments with functionally associated properties in B lymphoma cells. The approach was used to generate a panel of apoptosis-inducing antibodies specific for antigens differentially expressed in B lymphoma vs. T leukaemia cells. The selections resulted in an antibody pool with near perfect selectivity (&gt; 99%) for the B lymphoma target cells. Randomly picked clones (72) revealed 7 unique antibody genotypes. Six of these rapidly induced apoptosis in target cells. Following the conversion to full IgGs, the antibodies were shown to be specific for HLA-DR/DP, the B-cell receptor p chain and for CD54/ICAM-1. The latter receptor was not previously associated with apoptotic properties in B-cell lymphomas. Anti-ICAM-1 IgG induced apoptosis in a broad range of B lymphoma cell lines and were shown by immunohistochemistry to bind strongly to B lymphoma tissue obtained from 5 different B lymphoma patients. The recombinant IgG antibodies had affinities in the subnanomolar (0.3 nM) to nanomolar (3 nM) range. The described technology is generally applicable for the rapid isolation of high affinity human antibodies with specificity for differentially expressed cell surface receptors with intrinsic negative or positive signalling properties from naive phage libraries. (c) 2006 Wiley-Liss, Inc.}},
  author       = {{Fransson, Johan and Tornberg, UC and Borrebaeck, Carl and Carlsson, Roland and Frendeus, B}},
  issn         = {{0020-7136}},
  keywords     = {{intercellular; apoptosis; antibody library; phage display; B lymphoma; adhesion molecule-1}},
  language     = {{eng}},
  number       = {{2}},
  pages        = {{349--358}},
  publisher    = {{John Wiley & Sons Inc.}},
  series       = {{International Journal of Cancer}},
  title        = {{Rapid induction of apoptosis in B-cell lymphoma by functionally isolated human antibodies}},
  url          = {{http://dx.doi.org/10.1002/ijc.21829}},
  doi          = {{10.1002/ijc.21829}},
  volume       = {{119}},
  year         = {{2006}},
}

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Rapid induction of apoptosis in B-cell lymphoma by functionally isolated human antibodies