Transmembrane signals and protooncogene induction evoked by carcinogenic metals and prevented by zinc.

Smith, Jeffrey B.; Smith, Lucinda; Pijuan, Vivian; Zhuang, Yingxin; Chen, Yueh-Chu

doi:10.1289/ehp.94102s3181

Cited by 33 publications

(3 citation statements)

References 84 publications

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“…Several studies have demonstrated that metals with chemical characteristics similar to Cd 2+ protect against the biochemical and toxic effects of Cd 2+ in a competitive manner [4,38]. The results obtained with Fura-2-loaded cells resembled those observed in I sc -and Cl --transport experiments [14], since pre-treatment with Zn 2+ or Ni 2+ at 400 M completely removed [DCa 2+ ] Cd .…”

Section: Interaction Studiesmentioning

confidence: 69%

Evidence for cadmium mobilization of intracellular calcium through a divalent cation receptor in renal distal epithelial A6 cells

Faurskov

Bjerregaard

2002

Pfl�gers Archiv European Journal of Physiology

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The effect of Cd(2+) on intracellular Ca(2+) homeostasis was examined in renal epithelial A6 cells loaded with Fura-2. Cd(2+) (10 microM to 1 mM) produced a transient spike in cytosolic Ca(2+) in a dose-dependent manner. The phospholipase C inhibitor U73122 and the cation receptor agonist, neomycin, both diminish Cd(2+)-evoked increase in intracellular Ca(2+) ([deltaCa(2+)](Cd)). Further, thapsigargin, an inhibitor of intracellular Ca(2+)-ATPases, significantly reduced [deltaCa(2+)](Cd). Extending these observations, inositol-3-phosphate (IP(3)) binding studies showed that the resting level of intracellular IP(3) underwent a 1.45-fold increase when exposed to Cd(2+). Furthermore, we found that the Cd(2+)-related heavy metals, Zn(2+) and Ni(2+), were even more potent inducers of Ca(2+) mobilization and IP(3) generation than Cd(2+). It can be concluded that Cd(2+), and possibly Zn(2+) and Ni(2+), may act as agonists of a cation-sensing receptor (CSR) belonging to G-protein receptors capable of mediating IP(3) release of Ca(2+) from intracellular stores. The CSR receptor in A6 epithelia could not be stimulated with neomycin or Gd(3+), suggesting that the receptor is different from the calcium-sensing receptor.

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Section: Interaction Studiesmentioning

confidence: 69%

Evidence for cadmium mobilization of intracellular calcium through a divalent cation receptor in renal distal epithelial A6 cells

Faurskov

Bjerregaard

2002

Pfl�gers Archiv European Journal of Physiology

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“…Previous studies showed that nickel-induced signal transduction pathways involved c-Myc, Ras, c-Jun, and NFκB [6,[8][9][10]. They can be activated via Ras/MEK/ERK pathway [15] or P13K/Akt pathway [16].…”

Section: Discussionmentioning

confidence: 99%

“…It is likely to involve in genetic and epigenetic routes. Previous studies reported that nickel can produce oxidative DNA damage, inhibit DNA repair activity [5], effect signal transduction pathways, such as blocking Ca 2+ channels, and release stores of free intracellular Ca 2+ in a variety of systems, inactivate c-Myc, Ras, c-Jun, and NFκB [6][7][8][9][10]. Epigenetic effects of nickel includes the induction of DNA methylation and histone deacetylation, as well as activation or silencing of certain genes, especially those involved in cellular response to hypoxia [5,11].…”

mentioning

confidence: 99%

Identification of Differentially Expressed Genes in Lung Tissues of Nickel-Exposed Rats Using Suppression Subtractive Hybridization

Zhang

Fan

et al. 2010

Biol Trace Elem Res

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Occupational exposure to nickel compound, such as nickel refining, electroplating, and in conjunction with other metals, is harmful to the health, causing respiratory distress, and lung and nasal cancer. In this work, the different gene expression patterns of lung tissues from nickel-exposed rats and controls were investigated. The suppression subtractive hybridization (SSH) method was used to generate two subtracted cDNA libraries with gene transcripts differentially expressed after nickel inducing. Dot-blot hybridizations were used to confirm differential ratios of expression of obtained SSH clones. Out of 768 unique SSH clones, which were chosen randomly from the two subtraction libraries (384 of each), 319 could be verified as differentially expressed. According to blast screening and functional annotation, 28% genes in nickel-induced cDNA library were related to cell differentiation, whereas 21% in driver library were related to oxygen transport. Two novel expressed sequence tags (ESTs; NCBI Accession No. FC809414 and No. FC809411) in nickel-induced cDNA library were obtained. The genes detected in the present study are probably important genes associated with nickel-induced lung cancer.

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Calcium-independent effects of cadmium on actin assembly in mesangial and vascular smooth muscle cells

Wang

Chin

Templeton

1996

Cell Motil. Cytoskeleton

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Several metal ions are known to cause depolymerization of the actin cytoskeleton under some circumstances. We found that in renal mesangial and vascular smooth muscle cells, micromolar concentrations of Cd2+ result in loss of phalloidin‐stainable filamentous (F‐) actin. The decrease in F‐actin was not accompanied by a corresponding increase in G‐actin. The decrease in total actin could be accounted for in part by an inhibition by Cd2+ of total protein (and actin) synthesis after 6 to 8 h without an effect on actin degradation, and the equilibrium between F‐ and G‐actin was shifted to maintain near‐constant levels of G‐actin. However, Cd2+ caused significant decreases in F‐actin at earlier times, indicating effects on the polymerization equilibrium independent of those on actin synthesis. Only picomolar concentrations of free intracellular Cd2+ occur in these experiments. However, it is this Cd2+ pool which is responsible for F‐actin depolymerization because equal cellular concentrations of cadmium delivered as Cd‐metallothionein have no effect. The effect is also very specific for Cd2+ and under the same conditions neither Mg2+, Mn2+, Co2+, Ni2+, Cu2+, Zn2+, nor Hg2+ result in any loss of F‐actin. Addition of Cd2+ to mesangial and vascular smooth muscle cells had no immediate effect on free intracellular calcium concentrations ([Ca2+]i) even though Ca2+‐signalling pathways were intact as shown with vasopressin and endothelin. Exposure to 10 μM CdCl2 for 8 h nevertheless caused an increase in [Ca2+]i to > 250 nM and increases in [Ca2+]i achieved with ionophores alone were sufficient to decrease F‐actin concentrations. However, a rise in [Ca2+]i is not necessary for actin depolymerization. Depletion of cellular Ca2+ by treatment with thapsigargin did not protect F‐actin against Cd2+; the effect of Cd2+ was enhanced in cells unable to increase their [Ca2+]i. We conclude that depolymerization of F‐actin by Cd2+ in smooth muscle and mesangial cells is metal‐specific, Ca2+‐independent, and accompanied by a depletion of total actin protein. © 1996 Wiley‐Liss, Inc.

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Transmembrane signals and protooncogene induction evoked by carcinogenic metals and prevented by zinc.

Cited by 33 publications

References 84 publications

Evidence for cadmium mobilization of intracellular calcium through a divalent cation receptor in renal distal epithelial A6 cells

Evidence for cadmium mobilization of intracellular calcium through a divalent cation receptor in renal distal epithelial A6 cells

Identification of Differentially Expressed Genes in Lung Tissues of Nickel-Exposed Rats Using Suppression Subtractive Hybridization

Calcium-independent effects of cadmium on actin assembly in mesangial and vascular smooth muscle cells

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