Abstract

BackgroundEngineered nanoparticles are smaller than 100 nm and designed to improve or creating even new physico-chemical properties. Consequently, toxicological properties of materials may change as size reaches the nm size-range. We examined outcomes related to the central nervous system in the offspring following maternal inhalation exposure to nanosized carbon black particles (Printex 90).MethodsTime-mated mice (NMRI) were exposed by inhalation, for 45 min/day to 0, 4.6 or 37 mg/m3 aerosolized carbon black on gestation days 4–18, i.e. for a total of 15 days. Outcomes included maternal lung inflammation (differential cell count in bronchoalveolar lavage fluid and Saa3 mRNA expression in lung tissue), offspring neurohistopathology and behaviour in the open field test.ResultsCarbon black exposure did not cause lung inflammation in the exposed females, measured 11 or 28–29 days post-exposure. Glial fibrillary acidic protein (GFAP) expression levels were dose-dependently increased in astrocytes around blood vessels in the cerebral cortex and hippocampus in six weeks old offspring, indicative of reactive astrogliosis. Also enlarged lysosomal granules were observed in brain perivascular macrophages (PVMs) in the prenatally exposed offspring. The number of parvalbumin-positive interneurons and the expression levels of parvalbumin were decreased in the motor and prefrontal cortices at weaning and 120 days of age in the prenatally exposed offspring. In the open field test, behaviour was dose-dependently altered following maternal exposure to Printex 90, at 90 days of age. Prenatally exposed female offspring moved a longer total distance, and especially males spent significantly longer time in the central zone of the maze. In the offspring, the described effects were long-lasting as they were present at all time points investigated.ConclusionThe present study reports for the first time that maternal inhalation exposure to Printex 90 carbon black induced dose-dependent denaturation of PVM and reactive astrocytes, similarly to the findings observed following maternal exposure to Printex 90 by airway instillation. Of note, some of the observed effects have striking similarities with those observed in mouse models of neurodevelopmental disorders.

Highlights

  • Engineered nanoparticles are smaller than 100 nm and designed to improve or creating even new physico-chemical properties

  • Exposure characteristics Filter measurements demonstrated that the time-mated animals were exposed to a mean total suspended particle mass concentration: below the detection limit (LOD 0.08 mg/m3), 4.79 ± 1.86, or 33.87 ± 14.77 mg/m3 carbon black for the control, low, and high exposure level, respectively

  • Saa3 mRNA levels in Printex 90 exposed females were not statistically significantly different from air exposed controls, a non-significant dose-effect relationship was observed at postnatal day (PND) 9 (Fig. 2)

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Summary

Introduction

Engineered nanoparticles are smaller than 100 nm and designed to improve or creating even new physico-chemical properties. We examined outcomes related to the central nervous system in the offspring following maternal inhalation exposure to nanosized carbon black particles (Printex 90). Toxicity studies of engineered nanomaterials, such as carbon black nanoparticles (CB-NP), may provide insight into the potential health impacts of carbonaceous soot particles in ambient air pollution, especially those in the ultrafine and fine range [5]. Activation of the maternal immune response during pregnancy, by injection of influenza virus, polyinosinic-polycytidilic acid (poly(I:C)), or lipopolysaccharide (LPS), are established mouse models that demonstrate the causal relationship between maternal inflammation and changes in brain development and cognitive function in the offspring [20,21,22]. The developing nervous system may be especially sensitive to maternal particle exposure [17, 30], via direct or indirect mechanistic pathways

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