Registration Dossier
Registration Dossier
Please be aware that this old REACH registration data factsheet is no longer maintained; it remains frozen as of 19th May 2023.
The new ECHA CHEM database has been released by ECHA, and it now contains all REACH registration data. There are more details on the transition of ECHA's published data to ECHA CHEM here.
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EC number: 200-664-3 | CAS number: 67-68-5
Specific investigations: other studies
Administrative data
Link to relevant study record(s)
- Endpoint:
- biochemical or cellular interactions
- Type of information:
- experimental study
- Adequacy of study:
- key study
- Reliability:
- 2 (reliable with restrictions)
- Rationale for reliability incl. deficiencies:
- other: data from iCSS CompTox Dashboard. Data Quality 100%. Data manually curated with highest confidence
- Principles of method if other than guideline:
- Using a high-throughput robotic screening system, DMDO was assessed for its potential to disrupt biological pathways (DNA binding, growth factor, nuclear receptor (non-steroidal and steroidal), cell cycle, cytochrome P450, hydrolase and cell morphology) that may result in toxicity.
- Type of method:
- in vitro
- Specific details on test material used for the study:
- DSSTOX GSID: 21735
- Remarks:
- 0.001 to 200µM
- Details on study design:
- See enclosed excel file
- Details on results:
- 316 assays were performed, DMSO induced a positive response in 2 assays (ATG_Ahr_CIS_up and NVS_ADME_hCYP19A1). In the NVS_ADME_hCYP19A1 assay, the biochemical assay was < 50% efficacy and both assays were flagged as borderline activity. Therefore, there is no evidence that DMSO could interfere with the expression of the screened genes.
- Executive summary:
Using a high-throughput robotic screening system, DMSO was assessed for its potential to disrupt biological pathways (DNA binding, growth factor, nuclear receptor (non-steroidal and steroidal), cell cycle, cytochrome P450, hydrolase and cell morphology) that may result in toxicity. 316 assays were performed, DMSO induced a positive response in 2 assays (ATG_Ahr_CIS_up and NVS_ADME_hCYP19A1). In the NVS_ADME_hCYP19A1 assay, the biochemical assay was < 50% efficacy and both assays were flagged as borderline activity. Therefore, there is no evidence that DMSO could interfere with the expression of the screened genes.
- Endpoint:
- biochemical or cellular interactions
- Type of information:
- experimental study
- Adequacy of study:
- key study
- Reliability:
- 2 (reliable with restrictions)
- Principles of method if other than guideline:
- The PubChem BioAssay database was searched for chemogenomic, medicinal chemistry and functional genomics biological activities
- Type of method:
- in vivo
- Specific details on test material used for the study:
- PubChem CID: 679
PubChem SID: 67640, 48414927, 26757375, 103172948, 144211274, 316919445 - Details on results:
- 429 bioassays with 440 bioactivity outcomes were retrieved from the PubChem BioAssay data base. DMSO was reported as inactive in 195 assays, inconclusive in 25 assays and active in 5 bioassays. Activity was unspecified for 215 assays. None of the reported positive assays was demonstrative of a toxicological activity.
- Executive summary:
The PubChem BioAssay database was searched for chemogenomic, medicinal chemistry and functional genomics biological activities. 429 bioassays with 440 bioactivity outcomes were retrieved. DMSO was reported as inactive in 195 assays, inconclusive in 25 assays and active in 5 bioassays. Activity was unspecified for 215 assays. DMSO had no activity in cell viability assays, no agonist and/or antagonist activities on the peroxisome proliferator-activated receptor alpha (PPARa), delta (PPARd) and gamma (PPARg), antioxidant response element (ARE), androgen receptor (AR), estrogen receptor alpha (ER-alpha), thyroid receptor (TR) and glucocorticoid receptor (GR), p53, vitamin D receptor, retinoid X receptor alpha, farnesoid-X-receptor (FXR), hypoxia (HIF-1), NFkB, RXR, retinoid-related orphan receptor gamma (ROR-gamma) and aryl hydrocarbon receptor (AhR) signaling pathways. None of the reported positive assays was demonstrative of a toxicological activity.
Referenceopen allclose all
316 assays were performed, all results are displayed in the enclosed excel file.
Dimethyl sulphoxide induce a positive respons in 2 assay (see attached figure and table).
Intended Target Family |
Assay Component Endpoint Name |
AC50 (µM) |
LogAC50 |
Result |
cell cycle |
ACEA_T47D_80hr_Negative |
>100 |
Inactive |
|
nuclear receptor |
ACEA_T47D_80hr_Positive |
>100 |
Inactive |
|
dna binding |
ATG_AP_1_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_AP_1_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_AP_2_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_AP_2_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_AR_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_AR_TRANS_up |
>100 |
Inactive |
|
dna binding |
ATG_Ahr_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_Ahr_CIS_up |
1.76642438 |
1.23330695 |
Active |
dna binding |
ATG_BRE_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_BRE_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_CAR_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_CAR_TRANS_up |
>100 |
Inactive |
|
background measurement |
ATG_CMV_CIS_dn |
>100 |
Inactive |
|
background measurement |
ATG_CMV_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_CRE_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_CRE_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_C_EBP_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_C_EBP_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_DR5_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_E2F_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_E2F_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_EGR_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_EGR_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_ERE_CIS_dn |
1.86335 |
0.70526483 |
Inactive |
nuclear receptor |
ATG_ERE_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_ERRa_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_ERRa_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_ERRg_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_ERRg_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_ERa_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_ERa_TRANS_up |
>100 |
Inactive |
|
dna binding |
ATG_E_Box_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_E_Box_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_Ets_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_Ets_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_FXR_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_FXR_TRANS_up |
>100 |
Inactive |
|
dna binding |
ATG_FoxA2_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_FoxA2_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_FoxO_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_FoxO_CIS_up |
>100 |
Inactive |
|
background measurement |
ATG_GAL4_TRANS_dn |
>100 |
Inactive |
|
background measurement |
ATG_GAL4_TRANS_up |
>100 |
Inactive |
|
dna binding |
ATG_GATA_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_GATA_CIS_up |
1.36529001 |
0.47689725 |
Inactive |
dna binding |
ATG_GLI_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_GLI_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_GR_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_GR_TRANS_up |
>100 |
Inactive |
|
dna binding |
ATG_HIF1a_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_HIF1a_CIS_up |
-2.60376115 |
0.71408501 |
Inactive |
nuclear receptor |
ATG_HNF4a_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_HNF4a_TRANS_up |
>100 |
Inactive |
|
dna binding |
ATG_HNF6_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_HNF6_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_HSE_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_HSE_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_IR1_CIS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_IR1_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_ISRE_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_ISRE_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_LXRa_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_LXRb_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_LXRb_TRANS_up |
>100 |
Inactive |
|
dna binding |
ATG_MRE_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_MRE_CIS_up |
>100 |
Inactive |
|
background measurement |
ATG_M_06_CIS_dn |
>100 |
Inactive |
|
background measurement |
ATG_M_06_CIS_up |
>100 |
Inactive |
|
background measurement |
ATG_M_06_TRANS_dn |
>100 |
Inactive |
|
background measurement |
ATG_M_06_TRANS_up |
>100 |
Inactive |
|
background measurement |
ATG_M_19_CIS_dn |
>100 |
Inactive |
|
background measurement |
ATG_M_19_CIS_up |
>100 |
Inactive |
|
background measurement |
ATG_M_19_TRANS_dn |
>100 |
Inactive |
|
background measurement |
ATG_M_19_TRANS_up |
>100 |
Inactive |
|
background measurement |
ATG_M_32_CIS_dn |
>100 |
Inactive |
|
background measurement |
ATG_M_32_CIS_up |
>100 |
Inactive |
|
background measurement |
ATG_M_32_TRANS_dn |
>100 |
Inactive |
|
background measurement |
ATG_M_32_TRANS_up |
>100 |
Inactive |
|
background measurement |
ATG_M_61_CIS_dn |
>100 |
Inactive |
|
background measurement |
ATG_M_61_CIS_up |
>100 |
Inactive |
|
background measurement |
ATG_M_61_TRANS_dn |
>100 |
Inactive |
|
background measurement |
ATG_M_61_TRANS_up |
>100 |
Inactive |
|
dna binding |
ATG_Myb_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_Myb_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_Myc_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_Myc_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_NFI_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_NFI_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_NF_kB_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_NF_kB_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_NRF1_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_NRF1_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_NRF2_ARE_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_NRF2_ARE_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_NURR1_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_NURR1_TRANS_up |
>100 |
Inactive |
|
dna binding |
ATG_Oct_MLP_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_Oct_MLP_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_PBREM_CIS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_PBREM_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_PPARa_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_PPARa_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_PPARd_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_PPARd_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_PPARg_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_PPARg_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_PPRE_CIS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_PPRE_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_PXRE_CIS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_PXRE_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_PXR_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_PXR_TRANS_up |
>100 |
Inactive |
|
dna binding |
ATG_Pax6_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_Pax6_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_RARa_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_RARa_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_RARb_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_RARb_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_RARg_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_RARg_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_RORE_CIS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_RORE_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_RORb_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_RORb_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_RORg_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_RORg_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_RXRa_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_RXRa_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_RXRb_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_RXRb_TRANS_up |
>100 |
Inactive |
|
dna binding |
ATG_SREBP_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_SREBP_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_STAT3_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_STAT3_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_Sox_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_Sox_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_Sp1_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_Sp1_CIS_up |
>100 |
Inactive |
|
background measurement |
ATG_TAL_CIS_dn |
>100 |
Inactive |
|
background measurement |
ATG_TAL_CIS_up |
>100 |
Inactive |
|
background measurement |
ATG_TA_CIS_dn |
>100 |
Inactive |
|
background measurement |
ATG_TA_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_TCF_b_cat_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_TCF_b_cat_CIS_up |
>100 |
Inactive |
|
growth factor |
ATG_TGFb_CIS_dn |
>100 |
Inactive |
|
growth factor |
ATG_TGFb_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_THRa1_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_THRa1_TRANS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_VDRE_CIS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_VDRE_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_VDR_TRANS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_VDR_TRANS_up |
>100 |
Inactive |
|
cell cycle |
ATG_XTT_Cytotoxicity_up |
>100 |
Inactive |
|
dna binding |
ATG_Xbp1_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_Xbp1_CIS_up |
>100 |
Inactive |
|
dna binding |
ATG_p53_CIS_dn |
>100 |
Inactive |
|
dna binding |
ATG_p53_CIS_up |
>100 |
Inactive |
|
cyp |
NVS_ADME_hCYP19A1 |
0.93735446 |
1.22870888 |
Active |
cyp |
NVS_ADME_hCYP19A1_Activator |
>100 |
Inactive |
|
nuclear receptor |
NVS_NR_bER |
>100 |
Inactive |
|
nuclear receptor |
NVS_NR_hER |
>100 |
Inactive |
|
nuclear receptor |
NVS_NR_mERa |
-1.08010089 |
0.85999974 |
Inactive |
nuclear receptor |
OT_AR_ARELUC_AG_1440 |
>100 |
Inactive |
|
nuclear receptor |
OT_AR_ARSRC1_0480 |
>100 |
Inactive |
|
nuclear receptor |
OT_AR_ARSRC1_0960 |
>100 |
Inactive |
|
nuclear receptor |
OT_ER_ERaERa_0480 |
>100 |
Inactive |
|
nuclear receptor |
OT_ER_ERaERa_1440 |
>100 |
Inactive |
|
nuclear receptor |
OT_ER_ERaERb_0480 |
>100 |
Inactive |
|
nuclear receptor |
OT_ER_ERaERb_1440 |
>100 |
Inactive |
|
nuclear receptor |
OT_ER_ERbERb_0480 |
>100 |
Inactive |
|
nuclear receptor |
OT_ER_ERbERb_1440 |
>100 |
Inactive |
|
nuclear receptor |
OT_ERa_EREGFP_0120 |
>100 |
Inactive |
|
nuclear receptor |
OT_ERa_EREGFP_0480 |
>100 |
Inactive |
|
nuclear receptor |
OT_FXR_FXRSRC1_0480 |
>100 |
Inactive |
|
nuclear receptor |
OT_FXR_FXRSRC1_1440 |
>100 |
Inactive |
|
nuclear receptor |
OT_NURR1_NURR1RXRa_0480 |
>100 |
Inactive |
|
nuclear receptor |
OT_NURR1_NURR1RXRa_1440 |
>100 |
Inactive |
|
nuclear receptor |
OT_PPARg_PPARgSRC1_0480 |
>100 |
Inactive |
|
nuclear receptor |
OT_PPARg_PPARgSRC1_1440 |
>100 |
Inactive |
|
background measurement |
TOX21_ARE_BLA_Agonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_ARE_BLA_Agonist_ch2 |
1.78565278 |
1.11859869 |
Inactive |
dna binding |
TOX21_ARE_BLA_agonist_ratio |
1.83795837 |
1.44565386 |
Inactive |
cell cycle |
TOX21_ARE_BLA_agonist_viability |
>100 |
Inactive |
|
background measurement |
TOX21_AR_BLA_Agonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_AR_BLA_Agonist_ch2 |
>100 |
Inactive |
|
nuclear receptor |
TOX21_AR_BLA_Agonist_ratio |
>100 |
Inactive |
|
background measurement |
TOX21_AR_BLA_Antagonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_AR_BLA_Antagonist_ch2 |
-3.02166522 |
0.1559117 |
Inactive |
nuclear receptor |
TOX21_AR_BLA_Antagonist_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_AR_BLA_Antagonist_viability |
>100 |
Inactive |
|
nuclear receptor |
TOX21_AR_LUC_MDAKB2_Agonist |
>100 |
Inactive |
|
nuclear receptor |
TOX21_AR_LUC_MDAKB2_Antagonist |
>100 |
Inactive |
|
dna binding |
TOX21_AhR_LUC_Agonist |
>100 |
Inactive |
|
cyp |
TOX21_Aromatase_Inhibition |
1.27111531 |
0.40139802 |
Inactive |
background measurement |
TOX21_AutoFluor_HEK293_Cell_blue |
0.61089687 |
0.02833535 |
Inactive |
background measurement |
TOX21_AutoFluor_HEK293_Cell_green |
>100 |
Inactive |
|
background measurement |
TOX21_AutoFluor_HEK293_Cell_red |
0.79073689 |
0.05699185 |
Inactive |
background measurement |
TOX21_AutoFluor_HEK293_Media_blue |
>100 |
Inactive |
|
background measurement |
TOX21_AutoFluor_HEK293_Media_green |
0.45262469 |
0.007909 |
Inactive |
background measurement |
TOX21_AutoFluor_HEK293_Media_red |
>100 |
Inactive |
|
background measurement |
TOX21_AutoFluor_HEPG2_Cell_blue |
>100 |
Inactive |
|
background measurement |
TOX21_AutoFluor_HEPG2_Cell_green |
>100 |
Inactive |
|
background measurement |
TOX21_AutoFluor_HEPG2_Cell_red |
>100 |
Inactive |
|
background measurement |
TOX21_AutoFluor_HEPG2_Media_blue |
>100 |
Inactive |
|
background measurement |
TOX21_AutoFluor_HEPG2_Media_green |
>100 |
Inactive |
|
background measurement |
TOX21_AutoFluor_HEPG2_Media_red |
>100 |
Inactive |
|
hydrolase |
TOX21_ELG1_LUC_Agonist |
>100 |
Inactive |
|
background measurement |
TOX21_ERa_BLA_Agonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_ERa_BLA_Agonist_ch2 |
>100 |
Inactive |
|
nuclear receptor |
TOX21_ERa_BLA_Agonist_ratio |
>100 |
Inactive |
|
background measurement |
TOX21_ERa_BLA_Antagonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_ERa_BLA_Antagonist_ch2 |
>100 |
Inactive |
|
nuclear receptor |
TOX21_ERa_BLA_Antagonist_ratio |
1.60457702 |
0.34364255 |
Inactive |
cell cycle |
TOX21_ERa_BLA_Antagonist_viability |
>100 |
Inactive |
|
nuclear receptor |
TOX21_ERa_LUC_BG1_Agonist |
>100 |
Inactive |
|
nuclear receptor |
TOX21_ERa_LUC_BG1_Antagonist |
>100 |
Inactive |
|
background measurement |
TOX21_ESRE_BLA_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_ESRE_BLA_ch2 |
>100 |
Inactive |
|
dna binding |
TOX21_ESRE_BLA_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_ESRE_BLA_viability |
>100 |
Inactive |
|
background measurement |
TOX21_FXR_BLA_Antagonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_FXR_BLA_Antagonist_ch2 |
>100 |
Inactive |
|
background measurement |
TOX21_FXR_BLA_agonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_FXR_BLA_agonist_ch2 |
>100 |
Inactive |
|
nuclear receptor |
TOX21_FXR_BLA_agonist_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_FXR_BLA_agonist_viability |
>100 |
Inactive |
|
nuclear receptor |
TOX21_FXR_BLA_antagonist_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_FXR_BLA_antagonist_viability |
>100 |
Inactive |
|
background measurement |
TOX21_GR_BLA_Agonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_GR_BLA_Agonist_ch2 |
>100 |
Inactive |
|
nuclear receptor |
TOX21_GR_BLA_Agonist_ratio |
>100 |
Inactive |
|
background measurement |
TOX21_GR_BLA_Antagonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_GR_BLA_Antagonist_ch2 |
>100 |
Inactive |
|
nuclear receptor |
TOX21_GR_BLA_Antagonist_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_GR_BLA_Antagonist_viability |
>100 |
Inactive |
|
background measurement |
TOX21_HSE_BLA_agonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_HSE_BLA_agonist_ch2 |
>100 |
Inactive |
|
dna binding |
TOX21_HSE_BLA_agonist_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_HSE_BLA_agonist_viability |
>100 |
Inactive |
|
cell morphology |
TOX21_MMP_ratio_down |
>100 |
Inactive |
|
cell morphology |
TOX21_MMP_ratio_up |
0.74481946 |
0.34222594 |
Inactive |
cell cycle |
TOX21_MMP_viability |
>100 |
Inactive |
|
background measurement |
TOX21_NFkB_BLA_agonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_NFkB_BLA_agonist_ch2 |
>100 |
Inactive |
|
dna binding |
TOX21_NFkB_BLA_agonist_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_NFkB_BLA_agonist_viability |
>100 |
Inactive |
|
cell cycle |
TOX21_PPARd_BLA_Agonist_viability |
>100 |
Inactive |
|
background measurement |
TOX21_PPARd_BLA_Antagonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_PPARd_BLA_Antagonist_ch2 |
>100 |
Inactive |
|
background measurement |
TOX21_PPARd_BLA_agonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_PPARd_BLA_agonist_ch2 |
>100 |
Inactive |
|
nuclear receptor |
TOX21_PPARd_BLA_agonist_ratio |
>100 |
Inactive |
|
nuclear receptor |
TOX21_PPARd_BLA_antagonist_ratio |
1.58391519 |
0.75071519 |
Inactive |
cell cycle |
TOX21_PPARd_BLA_antagonist_viability |
>100 |
Inactive |
|
background measurement |
TOX21_PPARg_BLA_Agonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_PPARg_BLA_Agonist_ch2 |
>100 |
Inactive |
|
nuclear receptor |
TOX21_PPARg_BLA_Agonist_ratio |
-0.16499306 |
0.14944656 |
Inactive |
background measurement |
TOX21_PPARg_BLA_Antagonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_PPARg_BLA_Antagonist_ch2 |
>100 |
Inactive |
|
nuclear receptor |
TOX21_PPARg_BLA_antagonist_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_PPARg_BLA_antagonist_viability |
>100 |
Inactive |
|
nuclear receptor |
TOX21_TR_LUC_GH3_Agonist |
>100 |
Inactive |
|
nuclear receptor |
TOX21_TR_LUC_GH3_Antagonist |
>100 |
Inactive |
|
cell cycle |
TOX21_VDR_BLA_Agonist_viability |
>100 |
Inactive |
|
background measurement |
TOX21_VDR_BLA_Antagonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_VDR_BLA_Antagonist_ch2 |
>100 |
Inactive |
|
background measurement |
TOX21_VDR_BLA_agonist_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_VDR_BLA_agonist_ch2 |
>100 |
Inactive |
|
cyp |
TOX21_VDR_BLA_agonist_ratio |
>100 |
Inactive |
|
cyp |
TOX21_VDR_BLA_antagonist_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_VDR_BLA_antagonist_viability |
>100 |
Inactive |
|
background measurement |
TOX21_p53_BLA_p1_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_p53_BLA_p1_ch2 |
>100 |
Inactive |
|
dna binding |
TOX21_p53_BLA_p1_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_p53_BLA_p1_viability |
>100 |
Inactive |
|
background measurement |
TOX21_p53_BLA_p2_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_p53_BLA_p2_ch2 |
>100 |
Inactive |
|
dna binding |
TOX21_p53_BLA_p2_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_p53_BLA_p2_viability |
>100 |
Inactive |
|
background measurement |
TOX21_p53_BLA_p3_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_p53_BLA_p3_ch2 |
>100 |
Inactive |
|
dna binding |
TOX21_p53_BLA_p3_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_p53_BLA_p3_viability |
>100 |
Inactive |
|
background measurement |
TOX21_p53_BLA_p4_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_p53_BLA_p4_ch2 |
>100 |
Inactive |
|
dna binding |
TOX21_p53_BLA_p4_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_p53_BLA_p4_viability |
>100 |
Inactive |
|
background measurement |
TOX21_p53_BLA_p5_ch1 |
>100 |
Inactive |
|
background measurement |
TOX21_p53_BLA_p5_ch2 |
>100 |
Inactive |
|
dna binding |
TOX21_p53_BLA_p5_ratio |
>100 |
Inactive |
|
cell cycle |
TOX21_p53_BLA_p5_viability |
>100 |
Inactive |
|
null |
undefined |
>100 |
Inactive |
|
nuclear receptor |
ATG_DR4_LXR_CIS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_DR4_LXR_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_DR5_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_GRE_CIS_dn |
>100 |
Inactive |
|
nuclear receptor |
ATG_GRE_CIS_up |
>100 |
Inactive |
|
nuclear receptor |
ATG_LXRa_TRANS_dn |
>100 |
Inactive |
The list of all the assays performed is displayed in the enclosed excel file.
Detailed data on the assays reported as positive:
Activity Value [µM] |
Substance SID |
BioAssay AID |
BioAssay Name |
Target |
67640 |
196 |
NCI In Vivo Anticancer Drug Screen. Data for tumor model B16 Melanoma (intracerebral) in B6D2F1 (BDF1) mice |
||
67640 |
212 |
NCI In Vivo Anticancer Drug Screen. Data for tumor model Colon Carcinoma 38 (subcutaneous) in B6D2F1 (BDF1) mice |
||
48414927 |
1188 |
DSSTox (EPAFHM) EPA Fathead Minnow Acute Toxicity |
||
61.1306 |
144211274 |
743219 |
qHTS assay for small molecule agonists of the antioxidant response element (ARE) signaling pathway: Summary |
NFE2L2 |
103172948 |
1159620 |
Summary of drug indications. |
Data for SID 67640 in AID 196
schedule |
Q01DX005 (ip) |
endpoint |
median survival time |
vehicle |
saline |
dose |
8000.0 mg/kg/injection |
tcprcnt |
487 |
toxicity |
Antitumor endpoint evaluated on day 60; 09/10 animals surviving on day 5 |
Data for SID 67640 in AID 212
schedule |
Q07DX003 (ip) |
endpoint |
median tumor weight (est.) |
vehicle |
saline |
dose |
12.0 grams/kg/injection |
tcprcnt |
171 |
toxicity |
Antitumor endpoint evaluated on day 20; 10/10 animals surviving on tox evaluation day (usually day 5) |
Data for SID 48414927 in AID 1188
LC50_mg [mg/l] |
34000 |
LC50_mmol [mmol/l] |
435 |
MOA |
Baseline narcosis |
MOA_Confidence |
Moderate |
Data for SID 144211274 in AID 743219
Activity Summary |
active agonist |
Ratio Activity |
active agonist |
Ratio Potency (uM) [uM]* |
61.1306 |
Ratio Efficacy (%) [%] |
29.2951 |
530 nm Activity |
inactive |
530 nm Potency (uM) [uM] |
|
530 nm Efficacy (%) [%] |
0 |
460 nm Activity |
inconclusive agonist |
460 nm Potency (uM) [uM] |
61.1306 |
460 nm Efficacy (%) [%] |
62.7706 |
Viability Activity |
inactive |
Viability Potency (uM) [uM] |
|
Viability Efficacy (%) [%] |
0 |
Blue (460 nm) auto fluorescence outcome |
inactive |
Sample Source |
SIGMA |
Data for SID 103172948 in AID 1159620
First Approval |
1982 |
MeSH ID |
D063806 |
MeSH Heading |
MYALGIA |
EFO ID |
HP:000332 |
EFO Term |
MYALGIA |
Max Phase for Indication |
4 |
References |
ATC; |
Description of key information
Using a high-throughput robotic screening system (US EPA, 2017), DMSO was assessed for its potential to disrupt biological pathways (DNA binding, growth factor, nuclear receptor (non-steroidal and steroidal), cell cycle, cytochrome P450, hydrolase and cell morphology) that may result in toxicity. 316 assays were performed, DMSO induced a positive response in 2 assays (ATG_Ahr_CIS_up and NVS_ADME_hCYP19A1). In the NVS_ADME_hCYP19A1 assay, the biochemical assay was < 50% efficacy and both assays were flagged as borderline activity. Therefore, there is no evidence that DMSO could interfere with the expression of the screened genes.
The PubChem BioAssay database was searched for chemogenomic, medicinal chemistry and functional genomics biological activities (NCBI, 2017). 429 bioassays with 440 bioactivity outcomes were retrieved. DMSO was reported as inactive in 195 assays, inconclusive in 25 assays and active in 5 bioassays. Activity was unspecified for 215 assays. DMSO had no activity in cell viability assays, no agonist and/or antagonist activities on the peroxisome proliferator-activated receptor alpha (PPARa), delta (PPARd) and gamma (PPARg), antioxidant response element (ARE), androgen receptor (AR), estrogen receptor alpha (ER-alpha), thyroid receptor (TR) and glucocorticoid receptor (GR), p53, vitamin D receptor, retinoid X receptor alpha, farnesoid-X-receptor (FXR), hypoxia (HIF-1), NFkB, RXR, retinoid-related orphan receptor gamma (ROR-gamma) and aryl hydrocarbon receptor (AhR) signaling pathways. None of the reported positive assays was demonstrative of a toxicological activity.
Additional information
Information on Registered Substances comes from registration dossiers which have been assigned a registration number. The assignment of a registration number does however not guarantee that the information in the dossier is correct or that the dossier is compliant with Regulation (EC) No 1907/2006 (the REACH Regulation). This information has not been reviewed or verified by the Agency or any other authority. The content is subject to change without prior notice.
Reproduction or further distribution of this information may be subject to copyright protection. Use of the information without obtaining the permission from the owner(s) of the respective information might violate the rights of the owner.
