Emergence of Delayed Methylmercury Toxicity after Perinatal Exposure in Metallothionein-Null and Wild-Type C57BL Mice

Yoshida, Minoru; Shimizu, Natsuki; Suzuki, Megumi; Watanabe, Chiho; Satoh, Masahiko; Mori, Keiichiro; Yasutake, Akira

doi:10.1289/ehp.10906

Cited by 23 publications

(14 citation statements)

References 40 publications

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“…We cannot explain how the emergence of delayed neurobehavioral effects resulted from postnatal exposure to Hg 0 at present. In the present study, as described in previous paper (Yoshida et al, 2008), physiological events with acceleration of the aging process may contribute to the delayed Hg 0 toxicity due to postnatal exposure. However, age-related behavioral changes need to be clarified in further experiments.…”

Section: Discussionsupporting

confidence: 65%

“…On the other hand, the emergence of behavioral effects that accompany the aging process after exposure of offspring to low-level Hg 0 has not been studied in detail. However, results revealed that although the behavioral effects are slight, exposure to Hg 0 during developing periods resulted in the emergence of delayed Hg 0 toxicity in older mice, as well as the emergence of delayed methylmercury toxicity after perinatal exposure (Yoshida et al, 2008). The central nervous system is known to be susceptible to mercury and that exposure to Hg 0 causes more severe damage to offspring than adults.…”

Section: Discussionmentioning

confidence: 96%

“…Few animal studies have addressed the latency period of toxicity after exposure to mercury. Recently, Yoshida et al (2008) reported the existence of a long latency period in MT-I/II null mice after perinatal exposure to low-level methylmercury, in which the behavioral effects emerged long after the leveling-off of brain mercury levels. On the other hand, the emergence of behavioral effects that accompany the aging process after exposure of offspring to low-level Hg 0 has not been studied in detail.…”

Section: Discussionmentioning

confidence: 99%

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Emergence of delayed behavioral effects in offspring mice exposed to low levels of mercury vapor during the lactation period

et al. 2013

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-This study examined the emergence of delayed behavioral effects in offspring mice exposed to low levels of mercury vapor (Hg 0 ) during the lactation period. Female offspring of mice were repeatedly exposed to Hg 0 at 0.057 mg/m 3 , similar to the current threshold value (TLV), for 24 hr until the 20 th day postpartum. The behavioral effects were evaluated with locomotor activity in the open field (OPF), learning activity in the passive avoidance response (PA) and spatial learning ability in the Morris water maze (MM) at the ages of 3 and 15 months. Hg 0 -exposed mice did not differ from controls in the three behavioral measurements at 3 months of age, and no neurobehavioral effects were observed. On the other hand, the mice exhibited significantly more central locomotion in the OPF task when tested at 15 months of age, but no abnormality in other behavioral performance. Immediately after postnatal exposure, the brain mercury concentration of offspring was about 150 times that of the control, in which the concentrations were approximately 0.4 μg/g. The results indicate that mice exposed to Hg 0 at concentrations around TLV during the developing period resulted in the emergence of delayed behavioral effects at a later stage in life.

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Section: Discussionsupporting

confidence: 65%

Section: Discussionmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 99%

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Emergence of delayed behavioral effects in offspring mice exposed to low levels of mercury vapor during the lactation period

et al. 2013

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“…C. elegans express nearly 50 GSTs (van Rossum et al , 2001), approximately 10 HSPs of the HSP70 family (Heschl and Baillie, 1989), and 2 MTs (Freedman et al , 1993). Our results indicate that some of the same mechanisms are involved in detoxification in C. elegans as have been identified in other model systems (Sacco et al , 1997; Schlawicke Engstrom et al , 2008; Yoshida et al , 2008). …”

Section: Discussionsupporting

confidence: 83%

“…Due to their high cysteine content, MTs have a strong affinity for MeHg. Additionally, MeHg has been shown to induce MT expression (Rising et al , 1995; Tsui and Wang, 2005) and alterations in behavior of MT-null animals (Yoshida et al , 2008). Although GSH, HSP, and MT have been implicated in resistance to MeHg toxicity, researchers have yet to elucidate their precise roles in detoxification.…”

Section: Introductionmentioning

confidence: 99%

Hormetic effect of methylmercury on Caenorhabditis elegans

Helmcke

Aschner

2010

Toxicology and Applied Pharmacology

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Research has demonstrated the toxic effects of methylmercury (MeHg), yet molecular mechanisms underlying its toxicity are not completely understood. Caenorhabditis elegans (C. elegans) offers a unique biological model to explore mechanisms of MeHg toxicity given many advantages associated with its ease of use and genetic power. Since our previous work indicated neurotoxic resistance of C. elegans to MeHg, the present study was designed to examine molecular mechanisms associated with this resistance. We hypothesized MeHg would induce expression of gst, hsp or mtl in vivo since glutathione (GSH), heat shock proteins (HSPs), and metallothioneins (MTs) have shown involvement in MeHg toxicity. Our studies demonstrated a modest, but significant increase in fluorescence in gst-4::GFP and mtl-1::GFP strains at an acute, low L1 MeHg exposure, whereas chronic L4 MeHg exposure induced expression of gst-4::GFP and hsp-4::GFP. Knockout gst-4 animals showed no alterations in lethality sensitivity compared to wildtype animals whereas mtl knockouts displayed increased sensitivity to MeHg exposure. GSH levels were increased by acute MeHg treatment and depleted with chronic exposure. We also demonstrate that MeHg induces hormesis, a phenotype whereby a sublethal exposure to MeHg rendered C. elegans resistant to subsequent exposure to the organometal. The involvement of gst-4, hsp-4, mtl-1, and mtl-2 in hormesis was examined. An increase in gst-4::GFP expression after a low-dose acute exposure to MeHg indicated that gst-4 may be involved in this response. Our results implicate GSH, HSPs, and MTs in protecting C. elegans from MeHg toxicity and show a potential role of gst-4 in MeHg-induced hormesis.

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The Role of Thyroid Modulation by Methylmercury in Developmental Neurotoxicity

Mori

Yoshida

2012

Methylmercury and Neurotoxicity

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Emergence of Delayed Methylmercury Toxicity after Perinatal Exposure in Metallothionein-Null and Wild-Type C57BL Mice

Cited by 23 publications

References 40 publications

Emergence of delayed behavioral effects in offspring mice exposed to low levels of mercury vapor during the lactation period

Emergence of delayed behavioral effects in offspring mice exposed to low levels of mercury vapor during the lactation period

Hormetic effect of methylmercury on Caenorhabditis elegans

The Role of Thyroid Modulation by Methylmercury in Developmental Neurotoxicity

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