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Citations to this article

Endogenous interleukin 6 production in multiple myeloma patients treated with chimeric monoclonal anti-IL6 antibodies indicates the existence of a positive feed-back loop.
H C van Zaanen, … , H M Lokhorst, M H van Oers
H C van Zaanen, … , H M Lokhorst, M H van Oers
Published September 15, 1996
Citation Information: J Clin Invest. 1996;98(6):1441-1448. https://doi.org/10.1172/JCI118932.
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Research Article Article has an altmetric score of 9

Endogenous interleukin 6 production in multiple myeloma patients treated with chimeric monoclonal anti-IL6 antibodies indicates the existence of a positive feed-back loop.

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Abstract

In vitro as well as in vivo observations have shown that IL6 plays a key role in the pathogenesis of multiple myeloma. Therefore we started a phase I/II dose escalating study with chimeric monoclonal anti-IL6 antibodies (cMab) in multiple myeloma (MM) patients resistant to second-line chemotherapy. Here we describe the pharmacological data as well as a new method for calculating the endogenous IL6 production. The cMab (CLB IL6/8; Kd: 6.25 x 10(-12) M) was given in two cycles of 14 daily infusions, starting on day 1 and day 28. Daily dose: 5 mg in patients 1-3, 10 mg in patients 4-6, and 20 mg in patients 7-9 (total dose 140, 280, and 560 mg of anti-IL6, respectively). Using the pharmacokinetic data of free IL6 and the binding characteristics of the cMab, the endogenous IL6 production could be calculated from day to day using a one-compartment open model. The median half-life time of this antibody was 17.6 d. No human antichimeric antibodies were induced. Pre-treatment median endogenous IL6 production in the MM patients was 60 micrograms/d (range 13.8-230; normal controls < 7 micrograms/d). During treatment with anti-IL6 cMabs, the endogenous IL6 production immediately decreased in all patients to below 3 micrograms/d and never reached the pre-treatment value during the treatment period, except in two patients who developed an active infection, resulting in an IL6 production of 128 and 1,208 micrograms/d, respectively. We concluded that in MM patients endogenous IL6 production is 2-30 times higher than in healthy individuals. The anti-IL6 cMab strongly suppress this endogenous IL6 production, probably by blocking a positive feed-back loop, but this cMab does not prevent infection-induced IL6 production. The chimeric anti-IL6 Mabs have a long half-life time, a low immunogenicity, and are able to block IL6-dependent processes in vivo.

Authors

H C van Zaanen, R P Koopmans, L A Aarden, H J Rensink, J M Stouthard, S O Warnaar, H M Lokhorst, M H van Oers

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Year: 2022 2020 2018 2017 2016 2015 2014 2013 2012 2011 2010 2008 2006 2005 2002 2001 2000 1999 1998 1997 Total
Citations: 1 1 1 1 1 3 3 2 1 6 3 2 2 1 2 1 3 3 4 3 44
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Citations to this article (44)

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Cells 2022
Immunotherapy of multiple myeloma
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Interleukin-6: designing specific therapeutics for a complex cytokine
C Garbers, S Heink, T Korn, S Rose-John
Nature Reviews Drug Discovery 2018
IL-6 promotes CD4 + T-cell and B-cell activation during Plasmodium infection
I Sebina, LG Fogg, KR James, MS Soon, J Akter, BS Thomas, GR Hill, CR Engwerda, A Haque
Parasite Immunology 2017
The Role of Immunotherapy in Multiple Myeloma
M Kocoglu, A Badros
Pharmaceuticals (Basel, Switzerland) 2016
Co-expression of CD40/CD40L On XG1 Multiple Myeloma Cells Promotes IL-6 Autocrine Function
C Qi, S Tian, J Wang, H Ma, K Qian, X Zhang
Cancer Investigation 2015
Autocrine amplification of immature myeloid cells by IL-6 in multiple myeloma-infiltrated bone marrow
T Matthes, B Manfroi, A Zeller, I Dunand-Sauthier, B Bogen, B Huard
Leukemia 2015
A virtual approach to evaluate therapies for management of multiple myeloma induced bone disease: Modelling Therapies for Multiple Myeloma Induced Bone Disease
B Ji, PG Genever, MJ Fagan
International Journal for Numerical Methods in Biomedical Engineering 2015
p38 MAPK inhibits breast cancer metastasis through regulation of stromal expansion: p38 signaling in breast cancer metastasis
B Hong, H Li, M Zhang, J Xu, Y Lu, Y Zheng, J Qian, JT Chang, J Yang, Q Yi
International Journal of Cancer 2014
Mathematical modelling of the pathogenesis of multiple myeloma-induced bone disease: MODELLING THE PATHOLOGY OF MULTIPLE MYELOMA-INDUCED BONE DISEASE
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Y Wang, P Pivonka, PR Buenzli, DW Smith, CR Dunstan
PloS one 2011
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Best Practice & Research Clinical Haematology 2008
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2008
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Mucosal Immunology 2005
Interleukin 6 expression by Hodgkin/Reed-Sternberg cells is associated with the presence of 'B' symptoms and failure to achieve complete remission in patients with advanced Hodgkin's disease
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British Journal of Haematology 2002
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G Ichinowatari, M Yamada, H Yaginuma, K Tsuyuki, A Tanimoto, K Ohuchi
European Journal of Pharmacology 2002
Interleukin-6 is a growth factor for nonmalignant human plasmablasts
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Blood 2001
The acute-phase response varies with time and predicts serum albumin levels in hemodialysis patients
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A combination of anti-interleukin 6 murine monoclonal antibody with dexamethasone and high-dose melphalan induces high complete response rates in advanced multiple myeloma
P Moreau, JL Harousseau, J Wijdenes, N Morineau, N Milpied, R Bataille
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