Activation of Inflammation/NF-κB Signaling in Infants Born to Arsenic-Exposed Mothers

Fry, Rebecca C.; Navasumrit, Panida; Valiathan, Chandni; Svensson, J. Peter; Hogan, Bradley J.; Luo, Manlin; Bhattacharya, Sanchita; Kandjanapa, Krittinee; Soontararuks, Sumitra; Nookabkaew, Sumontha; Mahidol, Chulabhorn; Ruchirawat, Mathuros; Samson, Leona D.

doi:10.1371/journal.pgen.0030207

Cited by 238 publications

(212 citation statements)

References 36 publications

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“…These observations suggest that any pro-inflammatory stimulus or agent that gains entry to the body through different routes could induce the same negative effect on human cognitive functions. In this sense, several reports have shown that acute or chronic exposure to iAs or its methylated metabolites lead to inflammatory responses activation in diverse cell types [15][16][17]; therefore, exposure to arsenicals may increase the risk for cognitive impairment through the induction of a sustained inflammatory response.…”

Section: Introductionmentioning

confidence: 99%

Cortical Astrocytes Acutely Exposed to the Monomethylarsonous Acid (MMAIII) Show Increased Pro-inflammatory Cytokines Gene Expression that is Consistent with APP and BACE-1: Over-expression

et al. 2016

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Long-term exposure to inorganic arsenic (iAs) through drinking water has been associated with cognitive impairment in children and adults; however, the related pathogenic mechanisms have not been completely described. Increased or chronic inflammation in the brain is linked to impaired cognition and neurodegeneration; iAs induces strong inflammatory responses in several cells, but this effect has been poorly evaluated in central nervous system (CNS) cells.Because astrocytes are the most abundant cells in the CNS and play a critical role in brain homeostasis, including regulation of the inflammatory response, any functional impairment in them can be deleterious for the brain. We propose that iAs could induce cognitive impairment through inflammatory response activation in astrocytes. In the present work, rat cortical astrocytes were acutely exposed in vitro to the monomethylated metabolite of iAs (MMA III ), which accumulates in glial cells without compromising cell viability. MMA III LD 50 in astrocytes was 10.52 μM, however, exposure to sub-toxic MMA III concentrations (50 to 1000 nM) significantly increased IL-1β, IL-6, TNF-α, COX-2, and MIF-1 gene expression. These effects were consistent with amyloid precursor protein (APP) and β-secretase (BACE-1) increased gene expression, mainly for those MMA III concentrations that also induced TNF-α over-expression. Other effects of MMA III on cortical astrocytes included increased proliferative and metabolic activity. All tested MMA III concentrations led to an inhibition of intracellular lactate dehydrogenase (LDH) activity. Results suggest that MMA III induces important metabolic and functional changes in astrocytes that may affect brain homeostasis and that inflammation may play a major role in cognitive impairment-related pathogenicity in As-exposed populations.

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Section: Introductionmentioning

confidence: 99%

Cortical Astrocytes Acutely Exposed to the Monomethylarsonous Acid (MMAIII) Show Increased Pro-inflammatory Cytokines Gene Expression that is Consistent with APP and BACE-1: Over-expression

et al. 2016

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“…Several of these loci exhibited dose-response linear relationships between methylation and arsenic exposure including genes encoding oestrogen receptor alpha and a nuclear receptor co-activator, which given the importance of hormonal signalling in fetal development may have health consequences. A study in Thailand [38] compared RNA transcripts in the cord blood of newborns born to mothers differentially exposed to arsenic using microarray analysis. They found that prenatal arsenic exposure had a strong impact on the transcriptome of the newborn, with a subset of 11 transcripts highly predictive of arsenic exposure.…”

Section: Internal Pregnancy Exposome Studiesmentioning

confidence: 99%

“…Rager et al [39•] performed a similar analysis in a Mexican birth cohort; however, they also measured levels of miRNAs, small non-coding RNAs involved in regulation of messenger RNA (mRNA) translation. They identified 12 References selected from PubMed search (see Table 1) and recent reviews [4,45,46] (including citing and cited references) to represent state of the science miRNAs associated with arsenic exposure, many of which were known to have roles in carcinogenesis, and 334 mRNA transcripts including 28 identified in the study of Fry et al [38]. They found that a third of miRNA-mRNA pairings, predicted computationally based on target sequences, were correlated in their analysis.…”

Section: Internal Pregnancy Exposome Studiesmentioning

confidence: 99%

The Pregnancy Exposome

Robinson

Vrijheid

2015

Curr Envir Health Rpt

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The exposome concept takes a holistic approach facilitated by new and emerging technologies to describe 'the totality of human environmental (i.e. non-genetic) exposures from conception onwards, complementing the genome'. It provides a framework to advance the environmental epidemiology field that has until now focused almost exclusively on single-exposure health effects. The exposome includes an external domain, measured by methods including geo-spatial modelling, questionnaire and biomonitoring of external exposures while the internal domain is commonly assessed through molecular omics platforms. The internal domain, in part, reflects the biological response to the external domain. New statistical frameworks are required to integrate and assess exposome-health effects. The pregnancy period is a key starting point to describe the dynamic exposome, due to its heightened sensitivity and potential lifetime impact. A handful of studies have started to move towards an exposome approach in assessing the effects of the multiple exposures during pregnancy on child development. New research projects are underway to test the exposome approach on a large scale.

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“…Critical to understanding the importance of these exposures will be investigation of the associated cellular and physiologic effects to provide biological plausibility to the reported exposure-disease associations. A promising recent example in this regard comes from the work of Fry and colleagues (18), who showed that arsenic exposure in pregnant Thai women was related to differences in gene expression in the cord blood at the time of birth of their child. Among the affected biological pathways were those indicative of stress, inflammation, metal exposure, and apoptosis.…”

Section: Future Perspectivesmentioning

confidence: 99%