Particulate metal bioaccessibility in physiological fluids and cell culture media: Toxicological perspectives

Bérénice Leclercq; Laurent Yves Alleman; Esperanza Perdrix; Véronique Riffault; Mélanie Happillon; Alain Strecker; Jean-Marc Lo-Guidice; Guillaume Garçon; Patrice Coddeville

doi:10.1016/j.envres.2017.03.029

Particulate metal bioaccessibility in physiological fluids and cell culture media: Toxicological perspectives

Environ Res. 2017 Jul:156:148-157. doi: 10.1016/j.envres.2017.03.029. Epub 2017 Mar 27.

Authors

Bérénice Leclercq¹, Laurent Yves Alleman², Esperanza Perdrix³, Véronique Riffault³, Mélanie Happillon⁴, Alain Strecker⁵, Jean-Marc Lo-Guidice⁴, Guillaume Garçon⁴, Patrice Coddeville³

Affiliations

¹ IMT Lille Douai, Univ. Lille, SAGE - Département Sciences de l'Atmosphère et Génie de l'Environnement, F-59000 Lille, France; Univ. Lille, CHU Lille, Institut Pasteur de Lille, EA4483-IMPECS, France.
² IMT Lille Douai, Univ. Lille, SAGE - Département Sciences de l'Atmosphère et Génie de l'Environnement, F-59000 Lille, France. Electronic address: laurent.alleman@imt-lille-douai.fr.
³ IMT Lille Douai, Univ. Lille, SAGE - Département Sciences de l'Atmosphère et Génie de l'Environnement, F-59000 Lille, France.
⁴ Univ. Lille, CHU Lille, Institut Pasteur de Lille, EA4483-IMPECS, France.
⁵ CH Wattrelos, Wattrelos, France.

PMID: 28342961
DOI: 10.1016/j.envres.2017.03.029

Abstract

According to the literature, tiny amounts of transition metals in airborne fine particles (PM_2.5) may induce proinflammatory cell response through reactive oxygen species production. The solubility of particle-bound metals in physiological fluids, i.e. the metal bioaccessibility is driven by factors such as the solution chemical composition, the contact time with the particles, and the solid-to-liquid phase ratio (S/L). In this work, PM_2.5-bound metal bioaccessibility was assessed in various physiological-like solutions including cell culture media in order to evidence the potential impact on normal human bronchial epithelial cells (NHBE) when studying the cytotoxicity and inflammatory responses of PM_2.5 towards the target bronchial compartment. Different fluids (H₂O, PBS, LHC-9 culture medium, Gamble and human respiratory mucus collected from COPD patients), various S/L conditions (from 1/6000 to 1/100,000) and exposure times (6, 24 and 72h) were tested on urban PM_2.5 samples. In addition, metals' total, soluble and insoluble fractions from PM_2.5 in LHC-9 were deposited on NHBE cells (BEAS-2B) to measure their cytotoxicity and inflammatory potential (i.e., G6PDH activity, secretion of IL-6 and IL-8). The bioaccessibility is solution-dependent. A higher salinity or organic content may increase or inhibit the bioaccessibiliy according to the element, as observed in the complex mucus matrix. Decreasing the S/L ratio also affect the bioaccessibility depending on the solution tested while the exposure time appears less critical. The LHC-9 culture medium appears to be a good physiological proxy as it induces metal bioaccessibilities close to the mucus values and is little affected by S/L ratios or exposure time. Only the insoluble fraction can be linked to the PM_2.5-induced cytotoxicity. By contrast, both soluble and insoluble fractions can be related to the secretion of cytokines. The metal bioaccessibility in LHC-9 of the total, soluble, and insoluble fractions of the PM_2.5 under study did not explain alone, the cytotoxicity nor the inflammatory response observed in BEAS-2B cells. These findings confirm the urgent need to perform further toxicological studies to better evaluate the synergistic effect of both bioaccessible particle-bound metals and organic species.

Keywords: Bioaccessibility; Cytotoxicity; Inflammation; Mucus; Trace metals.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Air Pollutants / adverse effects*
Cell Culture Techniques
Cells, Cultured
Culture Media / analysis
Environmental Monitoring
Humans
Inhalation Exposure*
Metals / adverse effects*
Particle Size
Particulate Matter / adverse effects*
Reactive Oxygen Species / metabolism
Seasons

Substances

Air Pollutants
Culture Media
Metals
Particulate Matter
Reactive Oxygen Species