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Dive into the research topics where Jose Saldanha is active.

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Featured researches published by Jose Saldanha.


Molecular Immunology | 1994

Humanization of a mouse anti-human interleukin-6 receptor antibody comparing two methods for selecting human framework regions

Koh Sato; Masayuki Tsuchiya; Jose Saldanha; Yasuo Koishihara; Yoshiyuki Ohsugi; Tadamitsu Kishimoto; Mary M. Bendig

Mouse monoclonal antibody AUK12-20 binds to human IL-6 receptor and inhibits IL-6 functions. It has been humanized by CDR-grafting for therapeutic use. In the design of reshaped human AUK12-20 VL region, the human framework regions (FRs) from the human Bence-Jones protein REI were used. The reshaped human AUK12-20 light chain, in combination with chimeric AUK12-20 heavy chain, bound to antigen as well as chimeric AUK12-20 antibody. In the design of reshaped human AUK12-20 VH region, two sets of the human FRs were chosen and compared. One set was from the consensus amino acid sequence for human VH regions subgroup (HSG)-I and the other set was from human antibody HAX, the most similar human VH region found in a database of human immunoglobulin sequences. The HSG-I-based and the HAX-based reshaped human AUK12-20 heavy chains in combination with the reshaped human AUK12-20 light chain, showed approximately 90 and 100% antigen-binding and competition-binding activities as compared to the chimeric or mouse AUK12-20 heavy chains. Most importantly, these humanized antibodies inhibited the IL-6-dependent tumor cell growth as well as the original mouse antibody suggesting that these humanized antibodies could be efficacious in human patients. Our results show that both approaches for the design of reshaped human antibodies can be used for successful humanization. The approach based on FRs from the most similar individual human antibody, however, seemed to be best for designing a reshaped human antibody that mimicked as closely as possible the original mouse antibody.


Archive | 2003

Antibody and antibody fragments for inhibiting the growth of tumors

Neil I. Goldstein; Nicholas A. Giorgio; Steven Tarran Jones; Jose Saldanha


Archive | 1992

Reconstituted human antibody against human interleukin 6 receptor

Masayuki Tsuchiya; Koh Sato; Mary Margaret Bendig; Steven Tarran Jones; Jose Saldanha


Archive | 1995

Humanized antibodies against leukocyte adhesion molecule vla-4

Mary M. Bendig; Olivier Leger; Jose Saldanha; Tarran S. Jones; Theodore A. Yednock


Archive | 2004

Reshaped human antibody to human interleukin-6 receptor

Masayuki Tsuchiya; Koh Sato; Mary Margaret Bendig; Steven Tarran Jones; Jose Saldanha


Archive | 1992

Reshaped human to human interleukin-6 receptor

Masayuki Tsuchiya; Koh Sato; Mary Margaret Bendig; Steven Tarran Jones; Jose Saldanha


European Journal of Immunology | 1993

Optimization of primers for cloning libraries of mouse immunoglobulin genes using the polymerase chain reaction.

Catherine A. Kettleborough; Jose Saldanha; Keith H. Ansell; Mary M. Bendig


Archive | 1999

FAPalpha-specific antibody with improved producibility

John Edward Park; Pilar Garin-Chesa; Uwe Bamberger; Wolfgang J. Rettig; Olivier Leger; Jose Saldanha


Molecular Immunology | 1999

A single backmutation in the human kIV framework of a previously unsuccessfully humanized antibody restores the binding activity and increases the secretion in cos cells

Jose Saldanha; Andrew C. R. Martin; Olivier Leger


Archive | 1992

Humanized and chimeric monoclonal antibodies

Mary M. Bendig; Catherine A. Kettleborough; Jose Saldanha

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Mary M. Bendig

Medical Research Council

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Tarran S. Jones

Millennium Pharmaceuticals

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Koh Sato

Chugai Pharmaceutical Co.

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John Edward Park

Garvan Institute of Medical Research

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