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Glycerol monolaurate inhibition of human B cell activation

by Fosdick, Micaela G. , Zacharias, Zeb R. , Houtman, Jon C. D. , Loftus, Shannon , Phillips, Isabella

in 631/250/1619/40 / 631/250/2152/1566/1618 / Adaptive immunity / Antimicrobial agents / Cell activation / Cell membranes / Cell proliferation / Cytokines / Cytoskeleton / Glycerol / Humanities and Social Sciences / Humans / Immune response / Intracellular signalling / Laurates - pharmacology / Lymphocyte Activation / Lymphocytes B / Lymphocytes T / Monoglycerides / Monoglycerides - metabolism / Monoglycerides - pharmacology / multidisciplinary / Phosphorylation / Science / Science (multidisciplinary) / T-Lymphocytes - metabolism

2022

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Glycerol monolaurate inhibition of human B cell activation

by Fosdick, Micaela G. , Zacharias, Zeb R. , Houtman, Jon C. D. , Loftus, Shannon , Phillips, Isabella

2022

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Glycerol monolaurate inhibition of human B cell activation

by Fosdick, Micaela G. , Zacharias, Zeb R. , Houtman, Jon C. D. , Loftus, Shannon , Phillips, Isabella

2022

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Journal Article

Glycerol monolaurate inhibition of human B cell activation

Fosdick, Micaela G.,

Zacharias, Zeb R.,

Houtman, Jon C. D.,

Loftus, Shannon,

Phillips, Isabella

2022

Overview

Glycerol monolaurate (GML) is a naturally occurring antimicrobial agent used commercially in numerous products and food items. GML is also used as a homeopathic agent and is being clinically tested to treat several human diseases. In addition to its anti-microbial function, GML suppresses immune cell proliferation and inhibits primary human T cell activation. GML suppresses T cell activation by altering membrane dynamics and disrupting the formation of protein clusters necessary for intracellular signaling. The ability of GML to disrupt cellular membranes suggests it may alter other cell types. To explore this possibility, we tested how GML affects human B cells. We found that GML inhibits BCR-induced cytokine production, phosphorylation of signaling proteins, and protein clustering, while also changing cellular membrane dynamics and dysregulating cytoskeleton rearrangement. Although similar, there are also differences between how B cells and T cells respond to GML. These differences suggest that unique intrinsic features of a cell may result in differential responses to GML treatment. Overall, this study expands our understanding of how GML impacts the adaptive immune response and contributes to a broader knowledge of immune modulating monoglycerides.

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Publisher

Nature Publishing Group UK,Nature Publishing Group,Nature Portfolio

Subject

631/250/1619/40

/ 631/250/2152/1566/1618

/ Adaptive immunity

/ Antimicrobial agents

/ Cell activation

/ Cell membranes

/ Cell proliferation