Lipopolysaccharide

• Identification
• Experimental evidence
• Physicochemical properties
• ADMET properties
• Descriptors
• Chemical-gene interaction
• Chemical-phenotype interaction
• Chemical-disease association
• ToxCast endpoints
• Associated AOPs
• Presence in consumer products
• Presence in chemical regulation or guideline
• Presence in human biospecimen

Predicted ADME Properties
Type	Property	Tool	Interpretation	Probability/Value
Absorption	Caco-2 permeability	admetSAR	Low	0.82 %
		pkCSM	Low	-4.963 cm/s
	Human Intestinal Absorption	admetSAR	Low	12.85 %
		pkCSM	Low	0 %
		SwissADME	Low	-
	Human Oral Bioavailability	admetSAR	Low Bioavailability	8.93 %
	Log Kp (Skin permeation)	pkCSM	High	-2.735 logkp (cm/h)
		SwissADME	-	-39.73 logkp (cm/s)
Distribution	P-glycoprotein substrate	admetSAR	High	66.79 %
		pkCSM	No	-
		SwissADME	Yes	-
		vNN	No Prediction	-
	P-glycoprotein inhibitor	admetSAR	Low	31.59 %
		vNN	No Prediction	-
	P-glycoprotein inhibitor I	pkCSM	No	-
	P-glycoprotein inhibitor II	pkCSM	No	-
	Blood Brain Barrier	admetSAR	Low	12.98 %
		pkCSM	No	-17.684 logBB
		SwissADME	No	-
		vNN	No Prediction	-
	CNS permeability	pkCSM	No	-21.631 logPS
	Fraction unbound in human	pkCSM	-	0.381
	Plasma protein binding	admetSAR	79.75 %	Moderate
	Steady state volume of distribution (VDss)	pkCSM	Moderate	0.011 log(L/kg)
Metabolism	CYP1A2 inhibitor	admetSAR	Low	1.2 %
		pkCSM	No	-
		SwissADME	No	-
		vNN	No Prediction	-
	CYP2C19 inhibitor	admetSAR	Low	1.17 %
		pkCSM	No	-
		SwissADME	No	-
		vNN	No Prediction	-
	CYP2C9 inhibitor	admetSAR	Low	1.05 %
		pkCSM	No	-
		SwissADME	No	-
		vNN	No Prediction	-
	CYP2C9 substrate	admetSAR	Low	0.48 %
	CYP2D6 inhibitor	admetSAR	Low	6.77 %
		pkCSM	No	-
		SwissADME	No	-
		vNN	No Prediction	-
	CYP2D6 substrate	admetSAR	Low	0.48 %
		pkCSM	No	-
	CYP3A4 inhibitor	admetSAR	Low	1.39 %
		pkCSM	No	-
		SwissADME	No	-
		vNN	No Prediction	-
	CYP3A4 substrate	admetSAR	Low	5.24 %
		pkCSM	No	-
	Human Liver Microsomal (HLM) stability assay	vNN	No Prediction	-
	OATP2B1 inhibitor	admetSAR	Low	38.74 %
	OATP1B1 inhibitor	admetSAR	High	65.67 %
	OATP1B3 inhibitor	admetSAR	High	74.56 %
	MATE1 inhibitor	admetSAR	Low	8.21 %
	BSEP inhibitor	admetSAR	Low	47.2 %
	UGT catalysis	admetSAR	High	60.52 %
Excretion	Renal OCT2 inhibitor	admetSAR	Low	15.7 %
	Renal OCT2 substrate	pkCSM	No	-
	Total clearance	pkCSM	-	-1.06 ml/min/kg

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Predicted Toxicity properties
Property	Tool	Interpretation	Probability/Value
Acute oral toxicity	admetSAR	-	-3.15293836593628 log(mg/kg)
	ProTox	-	5000 mg/kg
Acute oral toxicity class	admetSAR	Low	8.6 %
	ProTox	5	-
Biodegradation	admetSAR	Low	22.83 %
	Toxtree	Class 2 (persistent chemical)	-
Carcinogens	admetSAR	Low	18.32 %
	Toxtree	No	-
Cramer's rule	Toxtree	High (Class III)	-
Cytotoxicity	vNN	NoPrediction	-
Genotoxic carcinogenity	Toxtree	No	-
Hepatotoxicity	admetSAR	Low	22.9 %
	pkCSM	No	-
	vNN	NoPrediction	-
Human Ether-a-go-go-Related Gene Inhibitor	admetSAR	High	65.8 %
	vNN	NoPrediction	-
Human Ether-a-go-go-Related Gene Inhibitor I	pkCSM	No	-
Human Ether-a-go-go-Related Gene Inhibitor II	pkCSM	No	-
Mitochondrial Membrane Potential (MMP)	vNN	NoPrediction	-
Maximum Recommended Tolerated Dose (MRTD)	pkCSM	Low	0.438 log(mg/kg/day)
	vNN	-	NoPrediction
Non-Genotoxic carcinogenicity	Toxtree	No	-
Oral rat acute toxicity	pkCSM	-	2.482 log(mg/kg_bw/day) (LD50)
	pkCSM	-	-3.518 log(mg/kg_bw/day) (LOAEL)
Micronucleus	admetSAR	Low	32.22 %
Skin sensitisation	pkCSM	No	-

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DISCLAIMER

We have built a comprehensive resource which compiles potential endocrine disrupting chemicals (EDCs) based on the observed adverse effects or endocrine-mediated endpoints in published experiments on humans or rodents to support basic research. We are not responsible for any errors or omissions in the published research articles or supporting literature on potential EDCs compiled in this resource. Users are advised to exercise their own judgement on the weight of evidence for potential EDCs compiled in this resource. Importantly, our sole goal to build this resource on potential EDCs is to enable future basic research towards better understanding of the systems-level perturbations upon chemical exposure rather than influencing regulatory advice on chemical use.