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Pharmaceutical immunoglobulin G impairs anti-carcinoma activity of oxaliplatin in colon cancer cells

Yuru Shang, Xianbin Zhang, Lili Lu, Ke Jiang, Mathias Krohn, Stephanie Matschos, Christina Susanne Mullins, Brigitte Vollmar, Dietmar Zechner, Peng Gong, Michael Linnebacher

2021British Journal of Cancer15 citationsDOIOpen Access PDF

Abstract

BACKGROUND: Recent evidence proves that intravenous human immunoglobulin G (IgG) can impair cancer cell viability. However, no study evaluated whether IgG application benefits cancer patients receiving chemotherapeutics. METHODS: Influence of pharmaceutical-grade human IgG on the viability of a series of patient-derived colon cancer cell lines with and without chemotherapeutic intervention was determined. Cell death was analysed flow cytometrically. In addition, the influence of oxaliplatin and IgG on the ERK1/2-signalling pathway was evaluated by western blots. RESULTS: IgG, in combination with chemotherapeutics. We did not observe any significant effects of IgG on tumour cell viability directly; however, human IgG significantly impaired the anti-tumoral effects of oxaliplatin. Primary cancer cell lines express IgG receptors and accumulate human IgG intracellularly. Moreover, while oxaliplatin induced the activation of ERK1/2, the pharmaceutical IgG inhibited ERK1/2 activity. CONCLUSIONS: IgG, can impair the anti-carcinoma activity of oxaliplatin. These data strongly suggest that therapeutic IgG as co-medication might have harmful side effects in cancer patients. The clinical significance of these preclinical observations absolutely advises further preclinical, as well as epidemiological and clinical research.

Topics & Concepts

OxaliplatinColorectal cancerMedicineImmunoglobulin GAntibodyCancerViability assayCancer researchImmunologyPharmacologyCellInternal medicineBiologyBiochemistryMonoclonal and Polyclonal Antibodies ResearchPlatelet Disorders and TreatmentsGlycosylation and Glycoproteins Research