Quantifying the impact of PFOA exposure on B-cell development and antibody production

Author:

Taylor Krystal D1,Woodlief Tracey L1,Ahmed Aya1,Hu Qing1,Duncker Patrick C2,DeWitt Jamie C1ORCID

Affiliation:

1. Department of Pharmacology & Toxicology, Brody School of Medicine, East Carolina University , Greenville, North Carolina 27834-4300, USA

2. Cytek Biosciences, Mid-Atlantic Region , Fremont, California 94538-6407, USA

Abstract

Abstract Per- and polyfluoroalkyl substances (PFAS) are synthetic chemicals; the vast majority are environmentally and biologically persistent, and some have demonstrated toxicity, including cancer, effects on metabolism, endocrine disruption, and immune dysfunction. Suppression of T-cell-dependent antibody responses (TDAR) has been observed in numerous studies of PFAS but mechanisms remain elusive. Evidence from our work suggests that B cells and how they use energy are impacted by PFAS exposure. We hypothesize that a well-studied and immunotoxic PFAS, perfluorooctanoic acid (PFOA), alters B-cell subclasses and markers of their metabolism. Adult male and female C57BL/6 mice were given PFOA (0 or 7.5 mg/kg) via gavage for 15 days, a duration and dose sufficient to suppress the TDAR. After dosing and immunization of subgroups, spleens were prepared to quantify B-cell subsets. Flow cytometric analysis revealed decreased numbers of plasmablasts, follicular, naïve, and overall B-cell subclasses in female PFOA-exposed groups. Male PFOA-exposed groups had a significant increase in follicular B cells and other subsets had decreases, including in the overall number of B cells. Twenty-four hours after naïve B-cell isolation and ex vivo activation, metabolic measurements revealed a 5-fold increase in metabolic markers in response to stimulation in PFOA-exposed groups compared with controls. These findings suggest that B-cell development and survival may be hindered by PFOA exposure, but that activation of the remaining B cells was not. Based on these findings, PFOA-mediated suppression of the primary IgM antibody response results changes to specific subsets of B cells.

Funder

National Institute of Environmental Health Sciences

NC State University Center for Environmental and Human Health Effects of PFAS

East Carolina University

NC State University

Publisher

Oxford University Press (OUP)

Subject

Toxicology

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