Literature DB >> 7627993

Granulocyte/macrophage-colony-stimulating factor augments the induction of antibodies, especially anti-idiotypic antibodies, to therapeutic monoclonal antibodies.

P Ragnhammar1, J Fagerberg, J E Frödin, P Wersäll, L O Hansson, H Mellstedt.   

Abstract

A group of 86 patients with advanced colorectal carcinoma were treated with the mouse (m) (IgG2A) or chimeric (c) monoclonal antibody (mAb) 17-1A. Prior to therapy, no patient had detectable levels of antibodies to mAb17-1A. All mmAb17-1A-treated patients (n = 76) developed antibodies against both idiotypic and isotypic determinants. Addition of granulocyte/macrophage-colony-stimulating factor (GM-CSF) to mmAb17-1A significantly enhanced the induction of anti-idiotypic (ab2) as well as anti-isotypic antibodies. Of the mmAb17-1A-treated patients, 16 developed type I allergic reactions. These patients had significantly higher concentrations of anti-(mouse Ig) antibodies than patients without type I reactions. Of these 16 patients, 5 had received mmAb17-1A alone; they constituted 9% of this group (5/56). The remaining 11 patients had been given mmAb17-1A together with GM-CSF, and represented 55% of this treatment group (11/20). The difference was statistically significant (P < 0.001). Of 10 patients, 9 (90%) treated with cmAb17-1A and GM-CSF developed ab2. The ab2 concentration in this patient group was significantly lower compared to those treated with mmAb-17A. Anti-(mouse Ig) antibodies caused clinical symptoms requiring therapeutic intervention in fewer than 10% of the patients treated with mmAb17-1A alone. With the addition of GM-CSF, the antibody concentration as well as the frequency of allergic side-effects calling for medical action increased significantly. Significantly more patients with a high ab2 concentration (at least 15 micrograms/ml) 1 month after completion of mAb therapy responded to mAb treatment as compared to those with a low ab2 concentration (P < 0.05). Moreover, patients with a high ab2 concentration (at least 15 micrograms/ml) had a median survival time of 15 months while those with a lower concentration survived for a median time of 9 months (P = 0.01).

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Year:  1995        PMID: 7627993     DOI: 10.1007/bf01525387

Source DB:  PubMed          Journal:  Cancer Immunol Immunother        ISSN: 0340-7004            Impact factor:   6.968


  34 in total

1.  Frequent anti-V-region immune response to mouse B72.3 monoclonal antibody.

Authors:  M B Khazaeli; M N Saleh; T Liu; P M Kaladas; S C Gilman; A F LoBuglio
Journal:  J Clin Immunol       Date:  1992-03       Impact factor: 8.317

Review 2.  The therapeutic use of monoclonal antibodies in colorectal carcinoma.

Authors:  H Mellstedt; J E Frödin; G Masucci; P Ragnhammar; J Fagerberg; A L Hjelm; J Shetye; P Wersäll; A Osterborg
Journal:  Semin Oncol       Date:  1991-10       Impact factor: 4.929

3.  Chimeric antibodies with 17-1A-derived variable and human constant regions.

Authors:  L K Sun; P Curtis; E Rakowicz-Szulczynska; J Ghrayeb; S L Morrison; N Chang; H Koprowski
Journal:  Hybridoma       Date:  1986-07

4.  Towards a network theory of the immune system.

Authors:  N K Jerne
Journal:  Ann Immunol (Paris)       Date:  1974-01

5.  Clinical effects of monoclonal antibodies (MAb 17-1A) in patients with metastatic colorectal carcinomas.

Authors:  J E Frödin; U Harmenberg; P Biberfeld; B Christensson; A K Lefvert; A Rieger; J Shetye; B Wahren; H Mellstedt
Journal:  Hybridoma       Date:  1988-08

6.  Induction of an immune network cascade in cancer patients treated with monoclonal antibodies (ab1). II. Is induction of anti-idiotype reactive T cells (T3) of importance for tumor response to mAb therapy?

Authors:  J Fagerberg; J E Frödin; P Ragnhammar; M Steinitz; H Wigzell; H Mellstedt
Journal:  Cancer Immunol Immunother       Date:  1994-03       Impact factor: 6.968

7.  Human immune response to multiple injections of murine monoclonal IgG.

Authors:  D L Shawler; R M Bartholomew; L M Smith; R O Dillman
Journal:  J Immunol       Date:  1985-08       Impact factor: 5.422

8.  Effect of monoclonal antibody 17-1A and GM-CSF in patients with advanced colorectal carcinoma--long-lasting, complete remissions can be induced.

Authors:  P Ragnhammar; J Fagerberg; J E Frödin; A L Hjelm; C Lindemalm; I Magnusson; G Masucci; H Mellstedt
Journal:  Int J Cancer       Date:  1993-03-12       Impact factor: 7.396

9.  Y and blood group B type 2 glycolipid antigens accumulate in a human gastric carcinoma cell line as detected by monoclonal antibody. Isolation and characterization by mass spectrometry and NMR spectroscopy.

Authors:  M Blaszczyk-Thurin; J Thurin; O Hindsgaul; K A Karlsson; Z Steplewski; H Koprowski
Journal:  J Biol Chem       Date:  1987-01-05       Impact factor: 5.157

Review 10.  Monoclonal antibodies for imaging and therapy.

Authors:  A A Epenetos; C Kosmas
Journal:  Br J Cancer       Date:  1989-02       Impact factor: 7.640
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  4 in total

Review 1.  Monoclonal antibodies in cancer therapy.

Authors:  R Gruber; E Holz; G Riethmüller
Journal:  Springer Semin Immunopathol       Date:  1996

Review 2.  Edrecolomab (monoclonal antibody 17-1A).

Authors:  J C Adkins; C M Spencer
Journal:  Drugs       Date:  1998-10       Impact factor: 9.546

Review 3.  Biological therapy: approaches in colorectal cancer. Strategies to enhance carcinoembryonic antigen (CEA) as an immunogenic target.

Authors:  A P Zbar; N R Lemoine; M Wadhwa; H Thomas; D Snary; W A Kmiot
Journal:  Br J Cancer       Date:  1998-03       Impact factor: 7.640

Review 4.  EpCAM an immunotherapeutic target for gastrointestinal malignancy: current experience and future challenges.

Authors:  M A Chaudry; K Sales; P Ruf; H Lindhofer; M C Winslet
Journal:  Br J Cancer       Date:  2007-02-27       Impact factor: 7.640
  4 in total

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