COX-2 Regulates the Insulin-Like Growth Factor I-Induced Potentiation of Zn2+-Toxicity in Primary Cortical Culture

Im, Joo-Young; Kim, Doyeun; Lee, Kang-Woo; Kim, Jung-Bin; Lee, Ja-Kyeong; Kim, Joo Young; Lee, Young Ik; Ha, Kwon‐Soo; Joe, Cheol O.; Han, Pyung Lim

doi:10.1124/mol.66.3.

Cited by 215 publications

(285 citation statements)

References 48 publications

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“…Similarly, although there is increased apoptotic cell death in the brain of TCDD-exposed larvae (Dong et al 2002), the developing spinal cord does not show the widespread cell death as observed with pyrene exposure. Most important, although CYP1A knockdown failed to modulate TCDD toxicity (Carney et al 2004), the onset of pyrene toxicity was markedly delayed in CYP1A morphants. Most evidence suggests that TCDD toxicity is related to its poor metabolism by CYP enzymes and concomitant bioaccumulation with persistent, futile AhR activation.…”

Section: Discussionmentioning

confidence: 99%

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Aryl Hydrocarbon Receptor–Independent Toxicity of Weathered Crude Oil during Fish Development

Incardona

Carls

Teraoka

et al. 2005

Environ Health Perspect

354

269

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Polycyclic aromatic hydrocarbons (PAHs), derived largely from fossil fuels and their combustion, are pervasive contaminants in rivers, lakes, and nearshore marine habitats. Studies after the Exxon Valdez oil spill demonstrated that fish embryos exposed to low levels of PAHs in weathered crude oil develop a syndrome of edema and craniofacial and body axis defects. Although mechanisms leading to these defects are poorly understood, it is widely held that PAH toxicity is linked to aryl hydrocarbon receptor (AhR) binding and cytochrome P450 1A (CYP1A) induction. Using zebrafish embryos, we show that the weathered crude oil syndrome is distinct from the well-characterized AhR-dependent effects of dioxin toxicity. Blockade of AhR pathway components with antisense morpholino oligonucleotides demonstrated that the key developmental defects induced by weathered crude oil exposure are mediated by low-molecular-weight tricyclic PAHs through AhR-independent disruption of cardiovascular function and morphogenesis. These findings have multiple implications for the assessment of PAH impacts on coastal habitats.

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Section: Discussionmentioning

confidence: 99%

“…However, AhR-dependent developmental defects were CYP1A independent. A CYP1A morpholino did not alter dioxin toxicity in zebrafish embryos, implicating other AhR target genes in dioxin pathophysiology (Carney et al 2004). …”

mentioning

confidence: 99%

Aryl Hydrocarbon Receptor–Independent Toxicity of Weathered Crude Oil during Fish Development

Incardona

Carls

Teraoka

et al. 2005

Environ Health Perspect

354

269

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“…NM_001033161). The ASO lead 1a is the murine homolog (a G to A base change at position 5) of the human TRADD lead reported previously (28). Control oligonucleotides 5 (5′-GCCCAATCTCGTTAGCGA-3′) were designed with six mismatches to 4 , such that they contained ≥4 mismatches to all known mouse sequence.…”

Section: Methodsmentioning

confidence: 96%

Antisense oligonucleotides containing locked nucleic acid improve potency but cause significant hepatotoxicity in animals

Swayze

Siwkowski

Wancewicz

et al. 2006

Nucleic Acids Research

385

330

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A series of antisense oligonucleotides (ASOs) containing either 2′-O-methoxyethylribose (MOE) or locked nucleic acid (LNA) modifications were designed to investigate whether LNA antisense oligonucleotides (ASOs) have the potential to improve upon MOE based ASO therapeutics. Some, but not all, LNA containing oligonucleotides increased potency for reducing target mRNA in mouse liver up to 5-fold relative to the corresponding MOE containing ASOs. However, they also showed profound hepatotoxicity as measured by serum transaminases, organ weights and body weights. This toxicity was evident for multiple sequences targeting three different biological targets, as well as in mismatch control sequences having no known mRNA targets. Histopathological evaluation of tissues from LNA treated animals confirmed the hepatocellular involvement. Toxicity was observed as early as 4 days after a single administration. In contrast, the corresponding MOE ASOs showed no evidence for toxicity while maintaining the ability to reduce target mRNA. These studies suggest that while LNA ASOs have the potential to improve potency, they impose a significant risk of hepatotoxicity.

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“…From FADD, the path obtained by our present method coincides with the intrinsic and the extrinsic pathway and not the path obtained by extreme pathway analysis. The intrinsic path that leads from FADD to the target gene DFF45 through the intermediate path as obtained by the present method can be found in [47]–[49].…”

Section: Resultsmentioning

confidence: 95%

Gradient Descent Optimization in Gene Regulatory Pathways

Das

Mukhopadhyay

2010

PLoS ONE

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BackgroundGene Regulatory Networks (GRNs) have become a major focus of interest in recent years. Elucidating the architecture and dynamics of large scale gene regulatory networks is an important goal in systems biology. The knowledge of the gene regulatory networks further gives insights about gene regulatory pathways. This information leads to many potential applications in medicine and molecular biology, examples of which are identification of metabolic pathways, complex genetic diseases, drug discovery and toxicology analysis. High-throughput technologies allow studying various aspects of gene regulatory networks on a genome-wide scale and we will discuss recent advances as well as limitations and future challenges for gene network modeling. Novel approaches are needed to both infer the causal genes and generate hypothesis on the underlying regulatory mechanisms.MethodologyIn the present article, we introduce a new method for identifying a set of optimal gene regulatory pathways by using structural equations as a tool for modeling gene regulatory networks. The method, first of all, generates data on reaction flows in a pathway. A set of constraints is formulated incorporating weighting coefficients. Finally the gene regulatory pathways are obtained through optimization of an objective function with respect to these weighting coefficients. The effectiveness of the present method is successfully tested on ten gene regulatory networks existing in the literature. A comparative study with the existing extreme pathway analysis also forms a part of this investigation. The results compare favorably with earlier experimental results. The validated pathways point to a combination of previously documented and novel findings.ConclusionsWe show that our method can correctly identify the causal genes and effectively output experimentally verified pathways. The present method has been successful in deriving the optimal regulatory pathways for all the regulatory networks considered. The biological significance and applicability of the optimal pathways has also been discussed. Finally the usefulness of the present method on genetic engineering is depicted with an example.

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COX-2 Regulates the Insulin-Like Growth Factor I-Induced Potentiation of Zn2+-Toxicity in Primary Cortical Culture

Cited by 215 publications

References 48 publications

Aryl Hydrocarbon Receptor–Independent Toxicity of Weathered Crude Oil during Fish Development

Aryl Hydrocarbon Receptor–Independent Toxicity of Weathered Crude Oil during Fish Development

Antisense oligonucleotides containing locked nucleic acid improve potency but cause significant hepatotoxicity in animals

Gradient Descent Optimization in Gene Regulatory Pathways

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