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Alzheimer disease
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	Field	Term

General Information:

Id:	5,299 (click here to show other Interactions for entry)
Diseases:	Diabetes mellitus, type II - [OMIM] Insulin resistance
Organism:	Mus musculus
Publication type:	article
Reference:	Thom R et al.(2014) Hypoxic induction of vascular endothelial growth factor (VEGF) and angiogenesis in muscle by truncated peroxisome proliferator-activated receptor gamma coactivator (PGC)-1alpha J. Biol. Chem. 13: 8810-8817 [PMID: 24505137]

Interaction Information:

Comment	Primary myoblasts were made to differentiate in cell culture, and were then treated with 0.5% oxygen for 16 h, versus normoxic control. Activation of a hypoxic program was confirmed by measuring expression of VEGF, Glut1, and PDK1, genes well known to be induced by hypoxia. Hypoxia induced the expression of alternatively spliced PGC-1alpha 8-fold. The expression of full length PGC-1alpha, on the other hand, was unaltered by hypoxic treatment. Hypoxia thus preferentially induces alternatively spliced PGC-1alpha expression in skeletal muscle cells.
Formal Description Interaction-ID: 51799	process response to hypoxia increases_expression of gene/protein VEGFA in skeletal muscle
Drugbank entries	Show/Hide entries for VEGFA
Drugbank DB00112	Bevacizumab not specified VEGFA
Drugbank DB01017	Minocycline inhibitor VEGFA
Drugbank DB01120	Gliclazide other/unknown VEGFA
Drugbank DB01136	Carvedilol other VEGFA
Drugbank DB01270	Ranibizumab not specified VEGFA
Drugbank DB03088	Pyroglutamic Acid not specified VEGFA
Drugbank DB03754	Tris(Hydroxymethyl)Aminomethane not specified VEGFA
Drugbank DB06779	Dalteparin inhibitor VEGFA
Drugbank DB01270	Ranibizumab not specified VEGFA
Drugbank DB03088	Pyroglutamic Acid not specified VEGFA
Drugbank DB03754	Tris(Hydroxymethyl)Aminomethane not specified VEGFA

Comment	Primary myoblasts were made to differentiate in cell culture, and were then treated with 0.5% oxygen for 16 h, versus normoxic control. Activation of a hypoxic program was confirmed by measuring expression of VEGF, Glut1, and PDK1, genes well known to be induced by hypoxia. Hypoxia induced the expression of alternatively spliced PGC-1alpha 8-fold. The expression of full length PGC-1alpha, on the other hand, was unaltered by hypoxic treatment. Hypoxia thus preferentially induces alternatively spliced PGC-1alpha expression in skeletal muscle cells.
Formal Description Interaction-ID: 51864	process response to hypoxia increases_expression of gene/protein SLC2A1 in skeletal muscle

Comment	Primary myoblasts were made to differentiate in cell culture, and were then treated with 0.5% oxygen for 16 h, versus normoxic control. Activation of a hypoxic program was confirmed by measuring expression of VEGF, Glut1, and PDK1, genes well known to be induced by hypoxia. Hypoxia induced the expression of alternatively spliced PGC-1alpha 8-fold. The expression of full length PGC-1alpha, on the other hand, was unaltered by hypoxic treatment. Hypoxia thus preferentially induces alternatively spliced PGC-1alpha expression in skeletal muscle cells.
Formal Description Interaction-ID: 51865	process response to hypoxia increases_expression of gene/protein PDK1 in skeletal muscle
Drugbank entries	Show/Hide entries for PDK1
Drugbank DB07403	4-[(3-CHLORO-4-{[(2R)-3,3,3-TRIFLUORO-2- ... not specified PDK1
Drugbank DB08809	Dichloroacetic Acid inhibitor PDK1

Comment	Primary myoblasts were made to differentiate in cell culture, and were then treated with 0.5% oxygen for 16 h, versus normoxic control. Activation of a hypoxic program was confirmed by measuring expression of VEGF, Glut1, and PDK1, genes well known to be induced by hypoxia. Hypoxia induced the expression of alternatively spliced PGC-1alpha 8-fold. The expression of full length PGC-1alpha, on the other hand, was unaltered by hypoxic treatment. Hypoxia thus preferentially induces alternatively spliced PGC-1alpha expression in skeletal muscle cells.
Formal Description Interaction-ID: 51866	process response to hypoxia increases_expression of mRNA/protein variant NT-PPARGC1A-a in skeletal muscle

Comment	Primary myoblasts were made to differentiate in cell culture, and were then treated with 0.5% oxygen for 16 h, versus normoxic control. Activation of a hypoxic program was confirmed by measuring expression of VEGF, Glut1, and PDK1, genes well known to be induced by hypoxia. Hypoxia induced the expression of alternatively spliced PGC-1alpha 8-fold. The expression of full length PGC-1alpha, on the other hand, was unaltered by hypoxic treatment. Hypoxia thus preferentially induces alternatively spliced PGC-1alpha expression in skeletal muscle cells.
Formal Description Interaction-ID: 51867	process response to hypoxia increases_expression of mRNA/protein variant NT-PPARGC1A-b in skeletal muscle

Comment	Primary myoblasts were made to differentiate in cell culture, and were then treated with 0.5% oxygen for 16 h, versus normoxic control. Activation of a hypoxic program was confirmed by measuring expression of VEGF, Glut1, and PDK1, genes well known to be induced by hypoxia. Hypoxia induced the expression of alternatively spliced PGC-1alpha 8-fold. The expression of full length PGC-1alpha, on the other hand, was unaltered by hypoxic treatment. Hypoxia thus preferentially induces alternatively spliced PGC-1alpha expression in skeletal muscle cells.
Formal Description Interaction-ID: 51868	process response to hypoxia NOT affects_expression of gene/protein PPARGC1A in skeletal muscle

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