Andrew G. Smith scite author profile

Andrew G. Smith

5Publications

40Citation Statements Received

79Citation Statements Given

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Affiliations

University of Utah, Georgia Institute of Technology, Castrol (United Kingdom)

Publications

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Intrinsic Hepatic Phenotype Associated with the Cyp1a2 Gene as Shown by cDNA Expression Microarray Analysis of the Knockout Mouse

Smith¹,

Davies²,

Dalton³

et al. 2002

Environ. Health Perspect.

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Several forms of cytochrome P450 (CYP) appear to metabolize principally pharmaceutical agents, as well as other dietary and plant chemicals. Other CYP forms have major roles in steroid, sterol, and bile acid metabolism. CYP1A2 expression is constitutively high in mouse liver and is well known for metabolizing several drugs and many procarcinogens to reactive intermediates that can cause toxicity or cancer. CYP1A2 is also known to carry out several endogenous functions such as uroporphyrinogen and melatonin oxidation and the 2-and 4-hydroxylations of estradiol. We have used cDNA microarray analysis of the untreated Cyp1a2(-/-) knockout mouse to search for changes in gene expression that might indicate important intrinsic roles for this enzyme. For 15 of the up-or downregulated genes, these increases or decreases were corroborated by reverse-transcription real-time polymerase chain reaction. Other than upregulation of the Hprt gene (used in the selection procedure for disrupting the Cyp1a2 gene), we found several genes upregulated that are associated with cell-cycle regulation and lipid metabolism. Besides Cyp1a2, the gene exhibiting the greatest downregulation was Igfbp1 (insulin-like growth factor binding protein-1), showing only 12% expression of that in the Cyp1a2(+/+) wild-type liver. Recurrent themes between both up-and downregulated genes include cell-cycle control, insulin action, lipogenesis, and fatty acid and cholesterol biosynthetic pathways. Histologically, the Cyp1a2(-/-) mouse exhibited an approximately 50% decrease in lipid stored in hepatocytes, and 50% increase in lipid present in interstitial fat-storing cells compared with that in the Cyp1a2(+/+) wild-type. These data suggest that the CYP1A2 enzyme might perform additional hepatic endogenous functions heretofore not appreciated. Toxicogenomics | Article Kimura et al. 1999;Shertzer et al. 2002). Cyp1a2(-/-) mice metabolize zoxazolamine, caffeine, and phenacetin less extensively than Cyp1a2(+/+) wild-type mice and are more susceptible to some aspects of toxicity of these drugs (Liang et al. 1996;Buters et al. 1996;Peters et al. 1999). On the contrary, Cyp1a2-null mice are unexpectedly protected from 4-aminobiphenyl-induced tumorigenesis ) and 4-aminobiphenyl-induced methemoglobinemia (Shertzer et al. 2002). Cyp1a2(-/-) mice also appear to be completely protected from hepatic uroporphyria caused by dioxin, hexachlorobenzene, and iron overload, although metabolism of these chemicals does not seem to be involved in the mechanism of their toxicity (Sinclair et al. 1998;Sinclair et al. 2000;Smith et al. 2001); in these cases, CYP1A2 appears to be functioning in a mode that does not involve production of a reactive metabolite. Other studies suggest that CYP1A2 might have a role in bilirubin metabolism (Zaccaro et al. 2001). It has been proposed that CYP1A1 metabolizes an endogenous substrate that modulates AH receptormediated gene expression and that, in the liver, CYP1A2 can take over this role (Nebert et al. 2000b). Since there is no constitutive exp...

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A computational model for the cooling phase of injection moulding

Smith

Wrobel

McCalla

et al. 2008

Journal of Materials Processing Technology

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This paper discusses the approaches and techniques used to build a realistic numerical model to analyse the cooling phase of the injection moulding process. The procedures employed to select an appropriate mesh and the boundary and initial conditions for the problem are discussed and justified. The final model is validated using direct comparisons with experimental results generated in an earlier study. The model is shown to be a useful tool for further studies aimed at optimising the cooling phase of the injection moulding process. Using the numerical model provides additional information relating to changes in conditions throughout the process, which otherwise could not be deduced or assessed experimentally. These results, and other benefits related to the use of the model, are also discussed in the paper.

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Gene expression profiles associated with inflammation, fibrosis and cholestasis in mouse liver after griseofulvin

Gant¹,

Baus²,

Clothier³

et al. 2002

Environ. Health Perspect. Toxicogenomics

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Erythropoietic protoporphyria patients can develop cholestasis, severe hepatic damage, fibrosis, and cirrhosis. We modeled this hepatic pathology in C57BL/6J and BALB/c mice using griseofulvin and analyzed 3,127 genes for alteration of expression in the liver before and during the onset of protoporphyria, cholestasis, inflammation, and hepatic fibrosis. The two mouse strains developed different levels of pathologic damage in response to the griseofulvin. Characteristic gene expression profiles could be associated with griseofulvin-induced gene expression, disruption of lipid metabolism, and the pathologic states of inflammation, early fibrosis, and cholestasis. Additionally, some genes individually indicated an alteration of homeostasis or pathologic state; for example, fibroblast proliferation was potentially indicated by increased calcyclin (SA100a6) expression. Changes in cytochrome P450 (Cyp) gene expression were particularly pronounced, with increased expression of the Cyp2a, Cyp2b, and Cyp3a families. Decreased Cyp4a10 and Cyp4a14 expression was observed that could be associated with early pathologic change. A potential decrease in bile acid and steroid biosynthesis was indicated by the decreased expression of Cyp7b1 and Hsd3b4, respectively. DNA damage was indicated by induction of GADD45. This study illustrates how transcriptional programs can be associated with different stimuli in the same experiment. The time course of change in the gene expression profile compared with changes in pathology and clinical chemistry shows the potential of this approach for modeling causative, predictive, and adaptive changes in gene expression during pathologic change.

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A Comparison of Full Scale Aft Cavity Drag Reduction Concepts With Equivalent Wind Tunnel Test Results

Kehs

Visser

Grossman³

et al. 2013

SAE Int. J. Commer. Veh.

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Accuracy, Reliability and Performance of Spray Combustion Models in LES

Srinivasan

Smith

Menon

2011

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Andrew G. Smith

Intrinsic Hepatic Phenotype Associated with the Cyp1a2 Gene as Shown by cDNA Expression Microarray Analysis of the Knockout Mouse

A computational model for the cooling phase of injection moulding

Gene expression profiles associated with inflammation, fibrosis and cholestasis in mouse liver after griseofulvin

A Comparison of Full Scale Aft Cavity Drag Reduction Concepts With Equivalent Wind Tunnel Test Results

Accuracy, Reliability and Performance of Spray Combustion Models in LES

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