Details of Xenobiotics-DME Interaction (XEOTIC)

General Information of Drug-Metabolizing Enzyme (DME ID: DME0132)
DME Name	Alcohol dehydrogenase class-III (ADH5), Homo sapiens	DME Info
UniProt ID	ADHX_HUMAN
EC Number	EC: 1.1.1.1 (Click to Show/Hide the Complete EC Tree) Oxidoreductase CH-OH donor oxidoreductase NAD/NADP oxidoreductase EC: 1.1.1.1
Lineage	Species: Homo sapiens (Click to Show/Hide the Complete Species Lineage) Kingdom: Metazoa Phylum: Chordata Class: Mammalia Order: Primates Family: Hominidae Genus: Homo Species: Homo sapiens
Interactome

Interactions between Xenobiotics and DME (XEOTIC)
Fungicide(s), Herbicide(s) or Insecticide(s)
Herbicide		Click to Show/Hide the Full List of Xenobiotics: 1 Xenobiotics
Atrazine		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00969 XEOTIC Info		Gene Form	mRNA
Classification	Herbicide
DME Modulation	Atrazine inhibits the expression of DME ADH5				[1]
Pesticide/Insecticide		Click to Show/Hide the Full List of Xenobiotics: 1 Xenobiotics
Dicrotophos		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO01050 XEOTIC Info		Gene Form	mRNA
Classification	Pesticide/Insecticide
DME Modulation	Dicrotophos inhibits the expression of DME ADH5				[2]
Health or Environmental Toxicant(s)
Acute Toxic Substance		Click to Show/Hide the Full List of Xenobiotics: 1 Xenobiotics
Cadmium		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO01503 XEOTIC Info		Gene Form	mRNA
Classification	Acute Toxic Substance
DME Modulation	Cadmium inhibits the expression of DME ADH5				[3]
Carcinogen		Click to Show/Hide the Full List of Xenobiotics: 1 Xenobiotics
Benzo(a)pyrene		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00898 XEOTIC Info		Gene Form	mRNA
Classification	Carcinogen
DME Modulation	Benzo(a)pyrene inhibits the expression of DME ADH5				[4]
Natural Product(s), Extract(s) or Medicine(s)
Natural Product		Click to Show/Hide the Full List of Xenobiotics: 1 Xenobiotics
Apocarotenal		Click to Show/Hide the Detail			Induction
XEOTIC ID	XEO01523 XEOTIC Info		Gene Form	mRNA
Classification	Natural Product
DME Modulation	Apocarotenal up-regulates the expression of DME ADH5				[5]
Pharmaceutical Agent(s)
Approved/Marketed Drug		Click to Show/Hide the Full List of Xenobiotics: 5 Xenobiotics
Acetaminophen		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00217 XEOTIC Info		Gene Form	mRNA
Classification	Drug Approved by US FDA
DME Modulation	Acetaminophen inhibits the expression of DME ADH5				[6]
Beta carotene		Click to Show/Hide the Detail			Induction
XEOTIC ID	XEO00401 XEOTIC Info		Gene Form	mRNA
Classification	Drug Approved by US FDA
DME Modulation	Beta carotene up-regulates the expression of DME ADH5				[5]
Copper sulfate		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00117 XEOTIC Info		Gene Form	mRNA
Classification	Drug Approved by US FDA
DME Modulation	Copper sulfate inhibits the expression of DME ADH5				[7]
Cyclosporine		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00241 XEOTIC Info		Gene Form	mRNA
Classification	Drug Approved by US FDA
DME Modulation	Cyclosporine inhibits the expression of DME ADH5				[8]
Urethane		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00435 XEOTIC Info		Gene Form	mRNA
Classification	Drug Approved by US FDA
DME Modulation	Urethane inhibits the expression of DME ADH5				[9]
Drug in Phase 2 Clinical Trial		Click to Show/Hide the Full List of Xenobiotics: 1 Xenobiotics
Ethanol		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00539 XEOTIC Info		Gene Form	Protein
Classification	Highest Clinical Status: Phase 2
DME Modulation	Ethanol inhibits the drug-metabolizing activity of DME ADH5				[10]
Drug in Phase 1 Clinical Trial		Click to Show/Hide the Full List of Xenobiotics: 1 Xenobiotics
Quercetin		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00538 XEOTIC Info		Gene Form	mRNA
Classification	Highest Clinical Status: Phase 1
DME Modulation	Quercetin inhibits the expression of DME ADH5				[11]
Preclinical/Patented Drug		Click to Show/Hide the Full List of Xenobiotics: 1 Xenobiotics
K-7174		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO01348 XEOTIC Info		Gene Form	mRNA
Classification	Patented Pharmaceutical Agent
DME Modulation	K-7174 inhibits the expression of DME ADH5				[12]
Other Chemical Compound(s) or Element(s)
Chemical Compound		Click to Show/Hide the Full List of Xenobiotics: 1 Xenobiotics
Gold		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO01504 XEOTIC Info		Gene Form	mRNA
Classification	Chemical Compound
DME Modulation	Gold inhibits the expression of DME ADH5				[13]

References
1	Endoplasmic reticulum stress impairs insulin signaling through mitochondrial damage in SH-SY5Y cells. Neurosignals. 2012;20(4):265-80.
2	Molecular mechanisms of discrotophos-induced toxicity in HepG2 cells: The role of CSA in oxidative stress. Food Chem Toxicol. 2017 May;103:253-260.
3	Short and long term gene expression variation and networking in human proximal tubule cells when exposed to cadmium. BMC Med Genomics. 2013;6 Suppl 1:S2.
4	Transcriptional signature of human macrophages exposed to the environmental contaminant benzo(a)pyrene. Toxicol Sci. 2010 Apr;114(2):247-59.
5	Beta-carotene and apocarotenals promote retinoid signaling in BEAS-2B human bronchioepithelial cells. Arch Biochem Biophys. 2006 Nov 1;455(1):48-60.
6	Multiple microRNAs function as self-protective modules in acetaminophen-induced hepatotoxicity in humans. Arch Toxicol. 2018 Feb;92(2):845-858.
7	Physiological and toxicological transcriptome changes in HepG2 cells exposed to copper. Physiol Genomics. 2009 Aug 7;38(3):386-401.
8	Integrating multiple omics to unravel mechanisms of Cyclosporin A induced hepatotoxicity in vitro. Toxicol In Vitro. 2015 Apr;29(3):489-501.
9	Toxicogenomics of the flame retardant tris (2-butoxyethyl) phosphate in HepG2 cells using RNA-seq. Toxicol In Vitro. 2018 Feb;46:178-188.
10	Interactive effects of in vitro binge-like alcohol and ATP on umbilical endothelial nitric oxide synthase post-translational modifications and redox modulation. Reprod Toxicol. 2014 Jan;43:94-101.
11	Disturbance of gene expression in primary human hepatocytes by hepatotoxic pyrrolizidine alkaloids: A whole genome transcriptome analysis. Toxicol In Vitro. 2015 Oct;29(7):1669-82.
12	A low-molecular-weight compound K7174 represses hepcidin: possible therapeutic strategy against anemia of chronic disease. PLoS One. 2013 Sep 27;8(9):e75568.
13	Changes in Caco-2 cells transcriptome profiles upon exposure to gold nanoparticles. Toxicol Lett. 2015 Mar 4;233(2):187-99.

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