Details of Xenobiotics-DME Interaction (XEOTIC)

General Information of Drug-Metabolizing Enzyme (DME ID: DME0073)
DME Name	Alcohol dehydrogenase class-V (ADH6), Homo sapiens	DME Info
UniProt ID	ADH6_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)
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 ADH6				[1]
Carcinogen		Click to Show/Hide the Full List of Xenobiotics: 3 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 ADH6				[2]
Dimethyl nitrosamine		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO01006 XEOTIC Info		Gene Form	mRNA
Classification	Carcinogen
DME Modulation	Dimethyl nitrosamine inhibits the expression of DME ADH6				[1]
Aflatoxin B1		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00806 XEOTIC Info		Gene Form	mRNA
Classification	Carcinogen-mycotoxin
DME Modulation	Aflatoxin B1 inhibits the expression of DME ADH6				[3]
Environmental Pollutant		Click to Show/Hide the Full List of Xenobiotics: 1 Xenobiotics
Zinc		Click to Show/Hide the Detail			Induction
XEOTIC ID	XEO01512 XEOTIC Info		Gene Form	mRNA
Classification	Environmental Pollutant
DME Modulation	Zinc up-regulates the expression of DME ADH6				[4]
Health Hazard/Toxicant		Click to Show/Hide the Full List of Xenobiotics: 2 Xenobiotics
Butyraldehyde		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00999 XEOTIC Info		Gene Form	mRNA
Classification	Health Hazard
DME Modulation	Butyraldehyde inhibits the expression of DME ADH6				[5]
Tris(1,3-dichloro-2-propyl)phosphate		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO01031 XEOTIC Info		Gene Form	mRNA
Classification	Health Hazard
DME Modulation	Tris(1,3-dichloro-2-propyl)phosphate inhibits the expression of DME ADH6				[6]
Natural Product(s), Extract(s) or Medicine(s)
Natural Product		Click to Show/Hide the Full List of Xenobiotics: 1 Xenobiotics
Walrycin A		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO01498 XEOTIC Info		Gene Form	mRNA
Classification	Natural Product
DME Modulation	Walrycin A inhibits the expression of DME ADH6				[7]
Pharmaceutical Agent(s)
Approved/Marketed Drug		Click to Show/Hide the Full List of Xenobiotics: 7 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 ADH6				[8]
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 ADH6				[9]
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 ADH6				[10]
Estradiol		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00090 XEOTIC Info		Gene Form	mRNA
Classification	Drug Approved by US FDA
DME Modulation	Estradiol inhibits the expression of DME ADH6				[11]
Leflunomide		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00053 XEOTIC Info		Gene Form	mRNA
Classification	Drug Approved by US FDA
DME Modulation	Leflunomide inhibits the expression of DME ADH6				[12]
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 ADH6				[13]
Valproic acid		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00029 XEOTIC Info		Gene Form	mRNA
Classification	Drug Approved by US FDA
DME Modulation	Valproic acid inhibits the expression of DME ADH6				[14]
Drug in Phase 1 Clinical Trial		Click to Show/Hide the Full List of Xenobiotics: 2 Xenobiotics
Quercetin		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00538 XEOTIC Info		Gene Form	Protein
Classification	Highest Clinical Status: Phase 1
DME Modulation	Quercetin inhibits the drug-metabolizing activity of DME ADH6				[15]
Sodium arsenite		Click to Show/Hide the Detail			Inhibition
XEOTIC ID	XEO00632 XEOTIC Info		Gene Form	Protein
Classification	Highest Clinical Status: Phase 1
DME Modulation	Sodium arsenite inhibits the drug-metabolizing activity of DME ADH6				[16]

References
1	Classification of heavy-metal toxicity by human DNA microarray analysis. Environ Sci Technol. 2007 May 15;41(10):3769-74.
2	New insights into BaP-induced toxicity: role of major metabolites in transcriptomics and contribution to hepatocarcinogenesis. Arch Toxicol. 2016 Jun;90(6):1449-58.
3	Aflatoxin B1 induces persistent epigenomic effects in primary human hepatocytes associated with hepatocellular carcinoma. Toxicology. 2016 Mar 28;350-352:31-9.
4	Vitamin D protects against particles-caused lung injury through induction of autophagy in an Nrf2-dependent manner. Environ Toxicol. 2019 May;34(5):594-609.
5	Integrated analysis of microRNA and mRNA expression profiles highlights aldehyde-induced inflammatory responses in cells relevant for lung toxicity. Toxicology. 2015 Aug 6;334:111-21.
6	Motexafin gadolinium and zinc induce oxidative stress responses and apoptosis in B-cell lymphoma lines. Cancer Res. 2005 Dec 15;65(24):11676-88.
7	Gene expression changes in human lung cells exposed to arsenic, chromium, nickel or vanadium indicate the first steps in cancer. Metallomics. 2012 Aug;4(8):784-93.
8	Multiple microRNAs function as self-protective modules in acetaminophen-induced hepatotoxicity in humans. Arch Toxicol. 2018 Feb;92(2):845-858.
9	Physiological and toxicological transcriptome changes in HepG2 cells exposed to copper. Physiol Genomics. 2009 Aug 7;38(3):386-401.
10	Integrative "-Omics" analysis in primary human hepatocytes unravels persistent mechanisms of cyclosporine A-induced cholestasis. Chem Res Toxicol. 2016 Dec 19;29(12):2164-2174.
11	Comparison of HepG2 and HepaRG by whole-genome gene expression analysis for the purpose of chemical hazard identification. Toxicol Sci. 2010 May;115(1):66-79.
12	Endoplasmic reticulum stress and MAPK signaling pathway activation underlie leflunomide-induced toxicity in HepG2 Cells. Toxicology. 2017 Dec 1;392:11-21.
13	Defensive and adverse energy-related molecular responses precede tris (1, 3-dichloro-2-propyl) phosphate cytotoxicity. J Appl Toxicol. 2016 May;36(5):649-58.
14	Endoplasmic reticulum stress impairs insulin signaling through mitochondrial damage in SH-SY5Y cells. Neurosignals. 2012;20(4):265-80.
15	Essential requirements for substrate binding affinity and selectivity toward human CYP2 family enzymes. Arch Biochem Biophys. 2003 Jan 1;409(1):32-44.
16	Combination therapy of 5-fluorouracil with rapamycin for hormone receptor-negative human breast cancer. Anticancer Res. 2010 Jul;30(7):2625-30.

If you find any error in data or bug in web service, please kindly report it to Dr. Yin and Dr. Li.