LR4-mediated activation of monocytes by human αS1-casein

Saenger T, Vordenbäumen S, Tahan T, Nienberg C, Bleck E, Schneider M, Jose J

Abstract in digital collection (conference) | Peer reviewed

Abstract

Human milk protein αS1-casein (CSN1S1) was shown to be overexpressed in autoimmune diseases (osteoarthritis, benign prostatic hyperplasia, multiple sclerosis) as well as in cancer. CSN1S1 displays opioid-like activity and modulates the innate immune response of intestinal cells. Recently, it was demonstrated, that CSN1S1 induces the expression of proinflammatory cytokines (IL-1β and IL-6) in monocytic cells via MAPK-p38 signaling [1, 2]. In this study the human TLR4 receptor, a receptor of the innate immune system, was identified as interaction partner of human CSN1S1 inducing expression of cytokines IL-1β, IL-6 and IL-8 in human monocytic cells concentration- and time-dependently [3]. In HEK293 cells cotransfected with TLR4 human CSN1S1 (purified from Escherichia coli) induced secretion of chemokine IL-8. In vitro flow cytometric assay confirmed CSN1S1 - TLR4 receptor interaction. Chemokine secretion as well as binding was not detected for CSN1S1 phosphorylated by protein kinase CK2 as well as denaturated CSN1S1. This supports the hypothesis, that CSN1S1 is a ligand of the TLR4 receptor exerting proinflammatory properties in phosphorylation-dependent manner. In conclusion CSN1S1 could contribute to the development of a potent immune system in breastfed offspring.

Details about the publication

StatusPublished
Release year2016
Language in which the publication is writtenEnglish
Conference2nd Electronic Conference on Medicinal Chemistry, Basel, undefined

Authors from the University of Münster

Jose, Joachim
Professur für Pharmazeutische Chemie (Prof. Jose)
Center of Interdisciplinary Sustainability Research (ZIN)