Literature DB >> 22001195

Exposure of pregnant mice to carbon black by intratracheal instillation: toxicogenomic effects in dams and offspring.

Petra Jackson1, Karin S Hougaard, Ulla Vogel, Dongmei Wu, Lorraine Casavant, Andrew Williams, Mike Wade, Carole L Yauk, Håkan Wallin, Sabina Halappanavar.   

Abstract

Exposure to nanomaterials (NM) during sensitive developmental stages may predispose organisms to diseases later in life. However, direct translocation of NM from mother to fetus through the placenta is limited. The present study tests the hypothesis that pulmonary exposure to NM and NM-induced response, such as inflammation during gestation, leads to secondary effects in the fetus. Time-mated C57BL/6BomTac mice were exposed by intratracheal instillation to vehicle (Nanopure water) or one of three concentrations (2.75, 13.5 or 67 μg in 40 μl Nanopure water) of carbon black Printex 90 (CB) on gestational days 7, 10, 15 and 18, to final cumulative doses of 11, 54 or 268 μg/animal. Samples from a subset of male and female newborns were collected on postnatal day 2 (4 days after the last maternal exposure) and from dams 26 to 27 days post-exposure (post-weaning period). Histopathology, DNA microarrays, pathway-specific RT-PCR arrays, focussed RT-PCR, and tissue protein analysis were employed to characterize pulmonary response in dams exposed to CB during pregnancy. Hepatic gene expression in newborns was interpreted in light of the observed biological responses and gene expression changes arising in the lungs of dams following CB exposure. Although retention of CB particles was observed in dams from both the medium and the high dose groups, neutrophil-marked inflammation and altered expression of several cytokines and chemokines, both at the transcriptional and tissue protein levels, was significant only in the high dose group. Analysis of newborn livers by DNA microarrays revealed that female offspring were more sensitive to maternal exposure than male offspring. Cellular signalling, inflammation, cell cycle and lipid metabolism were among the biological pathways affected in female offspring. Males, however, responded with subtle changes in metabolism-related genes. Further investigation is required to determine the long-term health consequences of the gene expression changes in offspring and response to environmental stresses. Crown
Copyright © 2011. Published by Elsevier B.V. All rights reserved.

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Year:  2011        PMID: 22001195     DOI: 10.1016/j.mrgentox.2011.09.018

Source DB:  PubMed          Journal:  Mutat Res        ISSN: 0027-5107            Impact factor:   2.433


  36 in total

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4.  Microvascular and mitochondrial dysfunction in the female F1 generation after gestational TiO2 nanoparticle exposure.

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6.  Gestational nanomaterial exposures: microvascular implications during pregnancy, fetal development and adulthood.

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7.  Maternal nanomaterial exposure: a double threat to maternal uterine health and fetal development?

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8.  Noninvasive intratracheal intubation to study the pathology and physiology of mouse lung.

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9.  Hepatic and pulmonary toxicogenomic profiles in mice intratracheally instilled with carbon black nanoparticles reveal pulmonary inflammation, acute phase response, and alterations in lipid homeostasis.

Authors:  Julie A Bourdon; Sabina Halappanavar; Anne T Saber; Nicklas R Jacobsen; Andrew Williams; Håkan Wallin; Ulla Vogel; Carole L Yauk
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Review 10.  Do all roads lead to Rome? The role of neuro-immune interactions before birth in the programming of offspring obesity.

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