T0070907

Catalog No.S2871 Batch:S287105

Print

Technical Data

Formula

C12H8ClN3O3
Molecular Weight 277.66 CAS No. 313516-66-4
Solubility (25°C)* In vitro DMSO 55 mg/mL (198.08 mM)
Water Insoluble
Ethanol Insoluble
In vivo (Add solvents to the product individually and in order)
Homogeneous suspension
CMC-NA
≥5mg/ml Taking the 1 mL working solution as an example, add 5 mg of this product to 1 ml of CMC-Na solution, mix evenly to obtain a homogeneous suspension with a final concentration of 5 mg/ml.
* <1 mg/ml means slightly soluble or insoluble.
* Please note that Selleck tests the solubility of all compounds in-house, and the actual solubility may differ slightly from published values. This is normal and is due to slight batch-to-batch variations.
* Room temperature shipping (Stability testing shows this product can be shipped without any cooling measures.)

Preparing Stock Solutions

Biological Activity

Description T0070907 is a potent inhibitor of PPARγ (peroxisome proliferator activator receptor γ ) that induces G2/M arrest and enhances the effect of radiation in human cervical cancer cells through mitotic catastrophe. It also acts as an antagonist of PPARγ that suppresses breast cancer cell proliferation and motility via both PPARgamma-dependent and -independent mechanisms.
Targets
PPARγ [1]
In vitro

T0070907 is a potent and selective PPARγ antagonist. With an apparent binding affinity of 1 nM, this compound covalently modifies PPARγ on cysteine 313 in helix 3 of human PPARγ2. It blocks PPARγ function in both cell-based reporter gene and adipocyte differentiation assays. Consistent with its role as an antagonist of PPARγ, this chemical blocks agonist-induced recruitment of coactivator-derived peptides to PPARγ in a homogeneous time-resolved fluorescence-based assay and promotes recruitment of the transcriptional corepressor NCoR to PPARγ in both glutathione S-transferase pull-down assays and a PPARγ/retinoid X receptor (RXR) α-dependent gel shift assay. Studies with mutant receptors suggest that it modulates the interaction of PPARγ with these cofactor proteins by affecting the conformation of helix 12 of the PPARγ ligand-binding domain. Interestingly, whereas the T0070907-induced NCoR recruitment to PPARγ/RXRα heterodimer can be almost completely reversed by the simultaneous treatment with RXRα agonist LGD1069, this compound treatment has only modest effects on LGD1069-induced coactivator recruitment to the PPARγ/RXRα heterodimer. [1] This chemical treatment inhibits proliferation, invasion and migration but does not significantly affect apoptosis. Molecular inhibition using a dominant negative (Δ462) receptor yields similar results. It also mediates a dose-dependent decrease in phosphorylation of PPARγ, and its ability to bind to DNA, and may directly affect mitogen-activated protein kinase signaling. [2]
In vivo

Lipopolysaccharide preconditioning significantly attenuates the development of renal dysfunction, hepatocellular injury, and circulatory failure as well as the increase in the plasma levels of interleukin-1 [beta] caused by severe endotoxemia. This compound can attenuate all of these beneficial effects afforded by preconditioning with lipopolysaccharide [3]

Protocol (from reference)

Kinase Assay:

[1]
  • Ligand Binding Assay

    To determine the binding affinity of T0070907 to the PPARs, scintillation proximity assay (SPA) is performed with the following modifications. A 90-μl reaction contains SPA buffer (10 mm KH2PO4, 10 mm KH2PO4, 2 mm EDTA, 50 mm NaCl, 1 mm dithiothreitol, 2 mmCHAPS, 10% (v/v) glycerol, pH 7.1), 50 ng of GST-PPARγ (or 150 ng of GST-PPARα, GST-PPARδ), 5 nm 3H-labeled radioligands, and 5 μl of this compound in Me2SO. After incubation for 1 h at room temperature, 10 μl of polylysine-coated SPA beads (at 20 mg/ml in SPA buffer) are added, and the mixtureis incubated for 1 h before reading in Packard Topcount.
Cell Assay:

[2]
  • Cell lines

    MCF-7 cells

  • Concentrations

    20 μM and higher concentrations

  • Incubation Time

    48 h

  • Method

    MTS assay
Animal Study:

[3]
  • Animal Models

    Preconditioning is performed by administering a low dose (1 mg/kg) of Escherichia coli LPS (serotype 0.127:B8) intraperitoneally 24 hr before the induction of severe endotoxemia.

  • Dosages

    1 mg/kg

  • Administration

    intraperitoneally

References

  • https://pubmed.ncbi.nlm.nih.gov/11877444/
  • https://pubmed.ncbi.nlm.nih.gov/21498701/
  • https://pubmed.ncbi.nlm.nih.gov/16484917/
  • https://pubmed.ncbi.nlm.nih.gov/24642720/

Customer Product Validation

Knocking down LKB1 reversed the PPARc antagonist T0070907-induced changes in the protein expression of the M1 markers (iNOS, green) and the M2 markers (CD206, red) by immunofluorescence staining. Scale bar = 20 μm.

Data from [ , , Aging Cell, 2018, doi: 10.1111/acel.12774 ]

PPARγ mRNA expression and activated PPARγ in nuclear extraction in monocytes after treatment with 10 μM atorvastatin for 24 h in the presence or absence of T0070907 (10 nM) or rosiglitazone (100 nM).§P<0.05 for atorvastatin versus vehicle. *P<0.05 for atorvastatin plus the indicated chemicals versus atorvastatin.

Data from [ , , Int Immunopharmacol, 2015, 26(1): 58-64 ]

Selleck's T0070907 Has Been Cited by 99 Publications

PPARG-centric transcriptional re-wiring during differentiation of human trophoblast stem cells into extravillous trophoblasts [ Nucleic Acids Res, 2025, 53(14)gkaf669] PubMed: 40705926
Gut symbiont-derived ursodeoxycholic acid promotes fatty acid oxidation to protect against renal ischemia-reperfusion injury [ Cell Rep Med, 2025, 6(10):102373] PubMed: 41015035
Nutrient deficiency-induced downregulation of SNX1 inhibits ferroptosis through PPARs-ACSL1/4 axis in colorectal cancer [ Apoptosis, 2025, 30(5-6):1391-1409] PubMed: 40095264
Stromal vascular fraction inhibits renal fibrosis by regulating metabolism and inflammation in obstructive nephropathy [ Front Pharmacol, 2025, 16:1559446] PubMed: 40432888
Diverse Lenabasum pathway activation in dermatomyositis patients' blood [ Sci Rep, 2025, 15(1):17232] PubMed: 40383862
Dysregulation of adipocytokines via the hsa-miR-548ay-3p/PPARγ signaling pathway leads to cardiac fibrosis [ Sci Rep, 2025, 15(1):27779] PubMed: 40739110
Interleukin-34-orchestrated tumor-associated macrophage reprogramming is required for tumor immune escape driven by p53 inactivation [ Immunity, 2024, 57(10):2344-2361.e7] PubMed: 39321806
Pro-ferroptotic signaling promotes arterial aging via vascular smooth muscle cell senescence [ Nat Commun, 2024, 15(1):1429] PubMed: 38365899
Targeted knockdown of PGAM5 in synovial macrophages efficiently alleviates osteoarthritis [ Bone Res, 2024, 12(1):15] PubMed: 38433252
Effect of genistein supplementation on microenvironment regulation of breast tumors in obese mice [ Breast Cancer Res, 2024, 26(1):147] PubMed: 39456028

RETURN POLICY
Selleck Chemical’s Unconditional Return Policy ensures a smooth online shopping experience for our customers. If you are in any way unsatisfied with your purchase, you may return any item(s) within 7 days of receiving it. In the event of product quality issues, either protocol related or product related problems, you may return any item(s) within 365 days from the original purchase date. Please follow the instructions below when returning products.

SHIPPING AND STORAGE
Selleck products are transported at room temperature. If you receive the product at room temperature, please rest assured, the Selleck Quality Inspection Department has conducted experiments to verify that the normal temperature placement of one month will not affect the biological activity of powder products. After collecting, please store the product according to the requirements described in the datasheet. Most Selleck products are stable under the recommended conditions.

NOT FOR HUMAN, VETERINARY DIAGNOSTIC OR THERAPEUTIC USE.