Recombining germline-derived CDR sequences for creating diverse single-framework antibody libraries

Söderlind, Eskil; Strandberg, Leif; Jirholt, Pernilla; Kobayashi, Norihiro; Alexeiva, Vessela; Åberg, Anna Maria; Nilsson, Anna; Jansson, Bo; Ohlin, Mats; Wingren, Christer; Danielsson, Lena; Carlsson, Roland; Borrebaeck, Carl A K

Recombining germline-derived CDR sequences for creating diverse single-framework antibody libraries

Mark

Söderlind, Eskil ^LU ; Strandberg, Leif ^LU ; Jirholt, Pernilla ^LU ; Kobayashi, Norihiro ; Alexeiva, Vessela ; Åberg, Anna Maria ^LU ; Nilsson, Anna ; Jansson, Bo ^LU ; Ohlin, Mats ^LU

and Wingren, Christer ^LU , et al. (2000) In Nature Biotechnology 18(8). p.852-856

Abstract: We constructed a single-chain Fv antibody library that permits human complementarity-determining region (CDR) gene fragments of any germline to be incorporated combinatorially into the appropriate positions of the variable-region frameworks VH-DP47 and VL-DPL3. A library of 2 x 10⁹ independent transformants was screened against haptens, peptides, carbohydrates, and proteins, and the selected antibody fragments exhibited dissociation constants in the subnanomolar range. The antibody genes in this library were built on a single master framework into which diverse CDRs were allowed to recombine. These CDRs were sampled from in vivo-processed gene sequences, thus potentially optimizing the levels of correctly folded and... (More); We constructed a single-chain Fv antibody library that permits human complementarity-determining region (CDR) gene fragments of any germline to be incorporated combinatorially into the appropriate positions of the variable-region frameworks VH-DP47 and VL-DPL3. A library of 2 x 10⁹ independent transformants was screened against haptens, peptides, carbohydrates, and proteins, and the selected antibody fragments exhibited dissociation constants in the subnanomolar range. The antibody genes in this library were built on a single master framework into which diverse CDRs were allowed to recombine. These CDRs were sampled from in vivo-processed gene sequences, thus potentially optimizing the levels of correctly folded and functional molecules, and resulting in a molecule exhibiting a lower computed immunogenicity compared to naive immunoglobulins. Using the modularized assembly process to incorporate foreign sequences into an immunoglobulin scaffold, it is possible to vary as many as six CDRs at the same time, creating genetic and funcfional variation in antibody molecules.
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Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/2f40154d-08d6-406d-80e4-e58ddb724997

author

Söderlind, Eskil ^LU ; Strandberg, Leif ^LU ; Jirholt, Pernilla ^LU ; Kobayashi, Norihiro ; Alexeiva, Vessela ; Åberg, Anna Maria ^LU ; Nilsson, Anna ; Jansson, Bo ^LU ; Ohlin, Mats ^LU

and Wingren, Christer ^LU , et al. (More)

Söderlind, Eskil ^LU ; Strandberg, Leif ^LU ; Jirholt, Pernilla ^LU ; Kobayashi, Norihiro ; Alexeiva, Vessela ; Åberg, Anna Maria ^LU ; Nilsson, Anna ; Jansson, Bo ^LU ; Ohlin, Mats ^LU

; Wingren, Christer ^LU ; Danielsson, Lena ^LU ; Carlsson, Roland ^LU and Borrebaeck, Carl A K ^LU (Less)

organization

Department of Immunotechnology

publishing date

2000

type

Contribution to journal

publication status

published

keywords

Antibody engineering, Diversity, In vitro evolution, Recombination

in

Nature Biotechnology

volume

18

issue

8

pages

5 pages

publisher

Nature Publishing Group

external identifiers

pmid:10932154
scopus:0033883409

ISSN

1087-0156

DOI

10.1038/78458

language

English

LU publication?

yes

id

2f40154d-08d6-406d-80e4-e58ddb724997

date added to LUP

2016-04-19 14:03:45

date last changed

2024-02-18 14:47:05

@article{2f40154d-08d6-406d-80e4-e58ddb724997,
  abstract     = {{<p>We constructed a single-chain Fv antibody library that permits human complementarity-determining region (CDR) gene fragments of any germline to be incorporated combinatorially into the appropriate positions of the variable-region frameworks VH-DP47 and VL-DPL3. A library of 2 x 10<sup>9</sup> independent transformants was screened against haptens, peptides, carbohydrates, and proteins, and the selected antibody fragments exhibited dissociation constants in the subnanomolar range. The antibody genes in this library were built on a single master framework into which diverse CDRs were allowed to recombine. These CDRs were sampled from in vivo-processed gene sequences, thus potentially optimizing the levels of correctly folded and functional molecules, and resulting in a molecule exhibiting a lower computed immunogenicity compared to naive immunoglobulins. Using the modularized assembly process to incorporate foreign sequences into an immunoglobulin scaffold, it is possible to vary as many as six CDRs at the same time, creating genetic and funcfional variation in antibody molecules.</p>}},
  author       = {{Söderlind, Eskil and Strandberg, Leif and Jirholt, Pernilla and Kobayashi, Norihiro and Alexeiva, Vessela and Åberg, Anna Maria and Nilsson, Anna and Jansson, Bo and Ohlin, Mats and Wingren, Christer and Danielsson, Lena and Carlsson, Roland and Borrebaeck, Carl A K}},
  issn         = {{1087-0156}},
  keywords     = {{Antibody engineering; Diversity; In vitro evolution; Recombination}},
  language     = {{eng}},
  number       = {{8}},
  pages        = {{852--856}},
  publisher    = {{Nature Publishing Group}},
  series       = {{Nature Biotechnology}},
  title        = {{Recombining germline-derived CDR sequences for creating diverse single-framework antibody libraries}},
  url          = {{http://dx.doi.org/10.1038/78458}},
  doi          = {{10.1038/78458}},
  volume       = {{18}},
  year         = {{2000}},
}

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Recombining germline-derived CDR sequences for creating diverse single-framework antibody libraries