Dibutyldichlorotin

Predicted ADME Properties
TypePropertyToolInterpretationProbability/Value
AbsorptionCaco-2 permeabilityadmetSARHigh95.57 %
pkCSMHigh1.413 cm/s
Human Intestinal AbsorptionadmetSARHigh96.46 %
pkCSMHigh90.98 %
SwissADMELow-
Human Oral BioavailabilityadmetSARLow Bioavailability45.8 %
Log Kp (Skin permeation)pkCSMLow-1.124 logkp (cm/h)
SwissADME--4.31 logkp (cm/s)
DistributionP-glycoprotein substrateadmetSARLow4.29 %
pkCSMNo-
SwissADMENo-
vNNNo Prediction-
P-glycoprotein inhibitoradmetSARLow4.06 %
vNNNo Prediction-
P-glycoprotein inhibitor IpkCSMNo-
P-glycoprotein inhibitor IIpkCSMNo-
Blood Brain BarrieradmetSARHigh97.72 %
pkCSMYes0.752 logBB
SwissADMENo-
vNNNo Prediction-
CNS permeabilitypkCSMModerate-2.064 logPS
Fraction unbound in humanpkCSM-0.34
Plasma protein bindingadmetSAR86.39 %Moderate
Steady state volume of distribution (VDss)pkCSMModerate0.32 log(L/kg)
MetabolismCYP1A2 inhibitoradmetSARHigh82.53 %
pkCSMNo-
SwissADMENo-
vNNNo Prediction-
CYP2C19 inhibitoradmetSARHigh81.14 %
pkCSMNo-
SwissADMENo-
vNNNo Prediction-
CYP2C9 inhibitoradmetSARLow47.07 %
pkCSMNo-
SwissADMENo-
vNNNo Prediction-
CYP2C9 substrateadmetSARLow43.1 %
CYP2D6 inhibitoradmetSARLow21.62 %
pkCSMNo-
SwissADMENo-
vNNNo Prediction-
CYP2D6 substrateadmetSARLow47.62 %
pkCSMNo-
CYP3A4 inhibitoradmetSARLow3.82 %
pkCSMNo-
SwissADMENo-
vNNNo Prediction-
CYP3A4 substrateadmetSARHigh63.56 %
pkCSMNo-
Human Liver Microsomal (HLM) stability assayvNNNo Prediction-
OATP2B1 inhibitoradmetSARLow13.33 %
OATP1B1 inhibitoradmetSARHigh97.59 %
OATP1B3 inhibitoradmetSARHigh98.13 %
MATE1 inhibitoradmetSARLow6.16 %
BSEP inhibitoradmetSARHigh57.52 %
UGT catalysisadmetSARLow1.56 %
ExcretionRenal OCT2 inhibitoradmetSARLow30.84 %
Renal OCT2 substratepkCSMNo-
Total clearancepkCSM-0.571 ml/min/kg
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Predicted Toxicity properties
PropertyToolInterpretationProbability/Value
Acute oral toxicityadmetSAR--2.83534908294678 log(mg/kg)
ProTox-50 mg/kg
Acute oral toxicity classadmetSARHigh82.25 %
ProTox2-
BiodegradationadmetSARLow8.54 %
ToxtreeClass 3 (unknown biodegradability)-
CarcinogensadmetSARLow47.46 %
ToxtreeNo-
Cramer's ruleToxtreeHigh (Class III)-
CytotoxicityvNNNoPrediction-
Genotoxic carcinogenityToxtreeNo-
HepatotoxicityadmetSARHigh80.72 %
pkCSMNo-
vNNNoPrediction-
Human Ether-a-go-go-Related Gene InhibitoradmetSARLow16.74 %
vNNNoPrediction-
Human Ether-a-go-go-Related Gene Inhibitor IpkCSMNo-
Human Ether-a-go-go-Related Gene Inhibitor IIpkCSMNo-
Mitochondrial Membrane Potential (MMP)vNNYes-
Maximum Recommended Tolerated Dose (MRTD)pkCSMLow0.463 log(mg/kg/day)
vNN-NoPrediction
Non-Genotoxic carcinogenicityToxtreeNo-
Oral rat acute toxicitypkCSM-2.667 log(mg/kg_bw/day) (LD50)
pkCSM-1.236 log(mg/kg_bw/day) (LOAEL)
MicronucleusadmetSARLow15.13 %
Skin sensitisationpkCSMYes-
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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.