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Featured researches published by Wansong Pan.


Diabetes | 1996

Regulation of Rat Liver Glucose-6-Phosphatase Gene Expression in Different Nutritional and Hormonal States: Gene Structure and 5′-Flanking Sequence

Doriane Argaud; Qing Zhang; Wansong Pan; Subir Maitra; Simon J. Pilkis; Alex J. Lange

The mRNA level of the catalytic subunit of rat liver glucose-6-phosphatase (Glu-6-Pase) was regulated by hormones commensurate with activity changes in vivo. Insulin exerts a dominant negative effect on the mRNA levels of Glu-6-Pase. Both mRNA levels and activities of the enzyme are low in the fed and refed state where insulin levels are elevated. Insulin administration to diabetic rats also decreases levels of mRNA and Glu-6-Pase activity. Insulin at a concentration of 1 nmol/l completely overcomes the stimulatory effect of glucocorticoids on Glu-6-Pase message levels in FAO hepatoma cells. The stimulatory response to glucocorticoid in FAO cells is biphasic, with maxima seen at 3 and 18 h after hormone addition (respectively 1.6- and 3.3-fold). 8-(4-chlorophenylthio)-cAMP (CPT-cAMP) causes a fourfold increase in Glu-6-Pase mRNA at 3 h in FAO cells. The gene of rat liver Glu-6-Pase is 13 kilobases in length and comprised of 5 exons. The exon-intron structure is completely conserved when compared with the mouse and human genes. A 0.5-kb 3′-untranslated region, which is present in rat and mouse liver Glu-6-Pase cDNA, is absent in the Glu-6-Pase gene reported here, indicating the possible duplication of either the terminal fifth exon or the entire gene. The promoter region contains a consensus core CCAAT element at position –207 and a TATAAA at position –31. Several possible response elements have been identified in the 5′-flanking region (from a HindIII site at position –1641). A consensus glucocorticoid response element is located at base pair –1552, a 9/10 match of the insulin response sequence is located at position –1449, and a 7/8 match of the cAMP response element is located at position –164.


Academic Emergency Medicine | 1996

Renal gluconeogenesis and blood flow during endotoxic shock.

Subir R. Maitra; Clark S. Homan; Wansong Pan; Evan R. Geller; Mark C. Henry; Henry C. Thode


Journal of Surgical Research | 1993

Effect of diltiazem on altered glucose regulation during endotoxic shock

Subir R. Maitra; Wansong Pan; Evan R. Geller


Shock | 1997

GLUCOSE-6-PHOSPHATASE GENE EXPRESSION FOLLOWING HEMORRHAGIC SHOCK AND RESUSCITATION: 234

Subir R. Maitra; Mark L. Gestring; Wansong Pan; M. R. El-Maghrabi


Shock | 1996

GENE EXPRESSION OF HEPATIC GLUCONEOGENIC ENZYMES FOLLOWING HEMORRHAGIC SHOCK.: 171

Subir R. Maitra; Wansong Pan; M. Raafat El-Maghrabi; Evan R. Geller


Shock | 1996

GLUCOSE-6-PHOSPHATASE GENE EXPRESSION FOLLOWING CRYSTALLOID RESUSCITATION IN HEMORRHAGIC SHOCK.: 170

Mark L. Gestring; Evan R. Geller; Wansong Pan; Subir R. Maitra


Shock | 1996

EFFECT OF ENDOTOXIC SHOCK ON GLUCOSE-6-PHOSPHATASE AND PHOSPHOENOL PYRUVATE CARBOXYKINASE GENE EXPRESSION.: 172

Wansong Pan; Mark L. Gestring; Evan R. Geller; Subir R. Maitra


Shock | 1995

DILTIAZEM INCREASES LEVELS OF HEPATIC GLUCOSE-6-PHOSPHATE WHEN ADDED TO STANDARD RESUSCITATION REGIMEN FOLLOWING HEMORRHAGIC SHOCK.: 107

Mark L. Gestring; Evan R. Geller; Wansong Pan; Subir R. Maitra


Shock | 1995

ISOLATION OF GLUCOSE-6-PHOSPHATASE ACTIVATOR IN HEMORRHAGIC SHOCK.: 116

Wansong Pan; Raafat M. El-Maghrabi; Naji N. Abumrad; Subir R. Maitra


Shock | 1995

ALTERATIONS IN HEPATIC HEXOSE MONOPHOSPHATE LEVELS DURING EARLY ENDOTOXIC SHOCK.: 175

Evan R. Geller; Mark L. Gestring; Wansong Pan; Brian Bowers; Subir R. Maitra

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Subir R. Maitra

Harper University Hospital

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Evan R. Geller

Harper University Hospital

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M. Raafat El-Maghrabi

State University of New York System

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Naji N. Abumrad

Vanderbilt University Medical Center

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Clark S. Homan

State University of New York System

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