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Oxaliplatin
Synonyms: L-OHP,NSC 266046
Oxaliplatin is a DNA alkylating agent that activates autophagy. Oxaliplatin inhibits DNA synthesis by conforming DNA adducts in RT4, TCCSUP, A2780, HT-29, U-373MG, U-87MG, SK-MEL-2, and HT-144 cells.Solutions are unstable and should be fresh-prepared.DMSO is not recommended to dissolve platinum-based drugs, which can easily lead to drug inactivation.
Oxaliplatin Chemical Structure
CAS No. 61825-94-3
Purity & Quality Control
Batch:
Purity:
99.78%
99.78
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Signaling Pathway
Cell Data
| Cell Lines | Assay Type | Concentration | Incubation Time | Formulation | Activity Description | PMID |
|---|---|---|---|---|---|---|
| Caco2 | Function Assay | 30/100 μM | 16 h | DMSO | activates Nrf2 | 24556415 |
| Caco2 | Function Assay | 3/10/30 μM | 16 h | DMSO | increases the mRNA levels of AKR1C1, NQO1, HO-1, MRP2, andMRP3 dose-dependently | 24556415 |
| Caco2 | Function Assay | 30 μM | 24 h | DMSO | induces the expression of HO-1, AKR1C, and NQO1 | 24556415 |
| SW620 | Growth Inhibition Assay | 10-70 mg/L | 24/48/72 h | inhibits cell growth in both time and dose dependent manner | 24646305 | |
| SW480 | Growth Inhibition Assay | 48 h | IC50=20.8 ug/mL | 24720675 | ||
| HCT116 | Function Assay | 2/5 µM | 24/48 h | suppresses survivin mRNA expression | 24761411 | |
| HT-29 | Growth Inhibition Assay | 1 μM | 0-72 h | inhibits cell growth in a time dependent manner | 24997451 | |
| SW480 | Growth Inhibition Assay | 1 μM | 0-72 h | inhibits cell growth in a time dependent manner | 24997451 | |
| HUVEC | Growth Inhibition Assay | IC50=11.30 ± 1.02 μM | 25307448 | |||
| HEK293 | Growth Inhibition Assay | IC50=8.82 ± 5.59 μM | 25307448 | |||
| HT-29 | Growth Inhibition Assay | IC50>50 μM | 25307448 | |||
| HCT-116 | Growth Inhibition Assay | IC50=6.24 ± 2.97 μM | 25307448 | |||
| MCF-7 | Growth Inhibition Assay | IC50=14.24 ± 1.82 μM | 25307448 | |||
| HepG2 | Growth Inhibition Assay | IC50=14.24 ± 1.82 μM | 25307448 | |||
| A549 | Growth Inhibition Assay | IC50=51.08 ± 10.96 μM | 25307448 | |||
| SGC7901 | Growth Inhibition Assay | IC50=21.73 ± 3.08 μM | 25307448 | |||
| COC1 | Growth Inhibition Assay | IC50=46.20 ± 3.14 μM | 25307448 | |||
| HCT116 | Growth Inhibition Assay | 72 h | IC50=6.23±0.75 µg/mL | 25360631 | ||
| SW480 | Growth Inhibition Assay | 72 h | IC50=10.7±2.26 µg/mL | 25360631 | ||
| MIAPaCa-2 | Function Assay | 25 µM | 24/48 h | induces cleavage of PARP, caspase-9, caspase-8 and caspase-3 | 25444914 | |
| Panc-1 | Function Assay | 25 µM | 24/48 h | induces cleavage of PARP, caspase-9, caspase-8 and caspase-3 | 25444914 | |
| MIAPaCa-2 | Apoptosis Assay | 25 µM | 24 h | induces apoptosis in a synergistic manner combined with WA | 25444914 | |
| Panc-1 | Apoptosis Assay | 25 µM | 24 h | induces apoptosis in a synergistic manner combined with WA | 25444914 | |
| HPDE | Cell Viability Assay | 25/50 μM | 24/48 h | inhibits proliferation of PC cells in a synergistic manner combined with WA | 25444914 | |
| SW1990 | Cell Viability Assay | 25/50 μM | 24/48 h | inhibits proliferation of PC cells in a synergistic manner combined with WA | 25444914 | |
| MIAPaCa-2 | Cell Viability Assay | 25/50 μM | 24/48 h | inhibits proliferation of PC cells in a synergistic manner combined with WA | 25444914 | |
| Panc-1 | Cell Viability Assay | 25/50 μM | 24/48 h | inhibits proliferation of PC cells in a synergistic manner combined with WA | 25444914 | |
| A549/CDDP | Growth Inhibition Assay | IC50=18.6 ± 1.2 μM | 25625243 | |||
| A549 | Growth Inhibition Assay | IC50=5.8 ± 0.6 μM | 25625243 | |||
| SW480 | Function Assay | 10 µg/ml | 24 h | enhances cellular autophagic flux | 25749420 | |
| SW620 | Function Assay | 10 µg/ml | 24 h | enhances cellular autophagic flux | 25749420 | |
| SW480 | Function Assay | 10 µg/ml | 24 h | increases LC3-II accumulation and decreases P62 expression | 25749420 | |
| SW620 | Function Assay | 10 µg/ml | 24 h | increases LC3-II accumulation and decreases P62 expression | 25749420 | |
| HT-29 | Growth Inhibition Assay | IC50=5.22 μM | 25761479 | |||
| SNU-175 | Growth Inhibition Assay | IC50=1.51 μM | 25761479 | |||
| COLO-320DM | Growth Inhibition Assay | IC50=5.38 μM | 25761479 | |||
| DLD-1 | Growth Inhibition Assay | IC50=8.65 μM | 25761479 | |||
| DiFi | Growth Inhibition Assay | IC50=10.95 μM | 25761479 | |||
| HCT-15 | Growth Inhibition Assay | IC50=8.64 μM | 25761479 | |||
| SCM-1 | Growth Inhibition Assay | IC50=17.5 μM | 25789057 | |||
| TMK-1 | Growth Inhibition Assay | IC50=22.6 μM | 25789057 | |||
| MKN-45 | Growth Inhibition Assay | IC50=14.0 μM | 25789057 | |||
| AGS | Growth Inhibition Assay | IC50=10.6 μM | 25789057 | |||
| S3 | Growth Inhibition Assay | IC50=53.5 ± 1.5 μM | 25801007 | |||
| SiHa | Growth Inhibition Assay | IC50=0.8 ± 0.1 μM | 25801007 | |||
| HT-29 | Growth Inhibition Assay | IC50=35.6 μM | 26003085 | |||
| DLD-1 | Growth Inhibition Assay | IC50=32.2 μM | 26003085 | |||
| HT29 | Growth Inhibition Assay | IC50=63 μM ± 18 | 26004084 | |||
| MC38 | Growth Inhibition Assay | IC50=23 μM ± 2 | 26004084 | |||
| SW620 | Growth Inhibition Assay | IC50=3.68 μM | 26023085 | |||
| SW480 | Growth Inhibition Assay | IC50=2.86 μM | 26023085 | |||
| RKO | Growth Inhibition Assay | IC50=1.23 μM | 26023085 | |||
| LoVo | Growth Inhibition Assay | IC50=1.2 μM | 26023085 | |||
| KM12 | Growth Inhibition Assay | IC50=4.37 μM | 26023085 | |||
| HCT116p53- | Growth Inhibition Assay | IC50=1.08 μM | 26023085 | |||
| HCT116 | Growth Inhibition Assay | IC50=1.04 μM | 26023085 | |||
| HCT15 | Growth Inhibition Assay | IC50=1.43 μM | 26023085 | |||
| HT29 | Growth Inhibition Assay | IC50=2.69 μM | 26023085 | |||
| DLD1 | Growth Inhibition Assay | IC50=2.01 μM | 26023085 | |||
| Colo205 | Growth Inhibition Assay | IC50=3.33 μM | 26023085 | |||
| BE | Growth Inhibition Assay | IC50=3.33 μM | 26023085 | |||
| CT26 | Cell Viability Assay | 4 mM | 48 h | decreases cell viability to 53.2% | 26137012 | |
| CT26 | Function Assay | 4 mM | 48 h | increases the expression levels of autophagy-related proteins, such as LC3-II, Beclin1 and ATG5 | 26137012 | |
| CT26 | Function Assay | 4 mM | 48 h | induces autophagy | 26137012 | |
| SK-OV-3 | Function Assay | 50 μM | 48 h | promotes sensitivity of ovarian carcinoma to NK cell-mediated cytolysis | 26138671 | |
| OVCAR-5 | Function Assay | 20 μM | 24h | promotes sensitivity of ovarian carcinoma to NK cell-mediated cytolysis | 26138671 | |
| PA-1 | Function Assay | 10 μM | 24h | promotes sensitivity of ovarian carcinoma to NK cell-mediated cytolysis | 26138671 | |
| SK-OV-3 | Function Assay | 50 μM | 96 h | up-regulates the stress ligands for NK cell-activating receptors and TRAIL receptors | 26138671 | |
| OVCAR-5 | Function Assay | 30 μM | 48h | up-regulates the stress ligands for NK cell-activating receptors and TRAIL receptors | 26138671 | |
| PA-1 | Function Assay | 10 μM | 48h | up-regulates the stress ligands for NK cell-activating receptors and TRAIL receptors | 26138671 | |
| SK-OV-3 | Function Assay | 50 μM | 96 h | triggeres the production of type I IFNs and chemokines | 26138671 | |
| OVCAR-5 | Function Assay | 30 μM | 48h | triggeres the production of type I IFNs and chemokines | 26138671 | |
| PA-1 | Function Assay | 10 μM | 24h | triggeres the production of type I IFNs and chemokines | 26138671 | |
| SK-OV-3 | Cell Viability Assay | 0-100 μM | 24/48/72 h | inhibits cell viability in both time and dose dependent manner | 26138671 | |
| OVCAR-5 | Cell Viability Assay | 0-60 μM | 24/48/72 h | inhibits cell viability in both time and dose dependent manner | 26138671 | |
| PA-1 | Cell Viability Assay | 0-20 μM | 24/48 h | inhibits cell viability in both time and dose dependent manner | 26138671 | |
| HCT116 | Growth Inhibition Assay | IC50=0.41 ± 0.02 μM | 26148596 | |||
| HT29 | Growth Inhibition Assay | IC50=0.88 ± 0.2 μM | 26148596 | |||
| SNU-387 | Growth Inhibition Assay | IC50=25 ± 2.7 μM | 26160429 | |||
| SNU-475 | Growth Inhibition Assay | IC50>30 μM | 26160429 | |||
| Hep-G2 | Growth Inhibition Assay | IC50=13.1 ± 1.6 μM | 26160429 | |||
| SNU-398 | Growth Inhibition Assay | IC50=6.5 ± 1.1 μM | 26160429 | |||
| LoVo | Function Assay | 1/5 μM | 24/48 h | induces transcriptional repression of DUT-N | 26208523 | |
| HCT116 p53+/+ | Function Assay | 1/5 μM | 24/48 h | induces transcriptional repression of DUT-N | 26208523 | |
| MDA-MB-231 | Growth Inhibition Assay | IC50=23.1 ± 0.1 μM | 26211591 | |||
| MCF-7 | Growth Inhibition Assay | IC50=15.4 ± 0.3 μM | 26211591 | |||
| SK-BR-3 | Growth Inhibition Assay | IC50=31.0 ± 0.1 μM | 26211591 | |||
| LoVo | Growth Inhibition Assay | 48 h | IC50=94.83 μM | 26269759 | ||
| HCT116 | Growth Inhibition Assay | 48 h | IC50=11.86 μM | 26269759 | ||
| SW480 | Growth Inhibition Assay | 48 h | IC50=1.87 μM | 26269759 | ||
| CaES-17 | Cytotoxicity Assay | 0–160 μM | 48 h | IC50=5.5 ± 0.2 μM | 26474693 | |
| HKESC-2 | Cytotoxicity Assay | 0–160 μM | 48 h | IC50=5.8 ± 0.5 μM | 26474693 | |
| Click to View More Cell Line Experimental Data | ||||||
Biological Activity
| Description | Oxaliplatin is a DNA alkylating agent that activates autophagy. Oxaliplatin inhibits DNA synthesis by conforming DNA adducts in RT4, TCCSUP, A2780, HT-29, U-373MG, U-87MG, SK-MEL-2, and HT-144 cells.Solutions are unstable and should be fresh-prepared.DMSO is not recommended to dissolve platinum-based drugs, which can easily lead to drug inactivation. | |
|---|---|---|
| Features | This product is not recommended to be dissolved in dimethylsulfoxide (DMSO).[9] | |
| Targets |
|
| In vitro | ||||
| In vitro | The main mechanism of action of Oxaliplatin is mediated through the formation of DNA–adducts. Oxaliplatin induces primary and secondary DNA lesions that lead to cell apoptosis. [1] Oxaliplatin is active against human melanoma cell lines C32 and G361 with IC50 of 0.98 mM and 0.14 mM, respectively. [2] Oxaliplatin effectively inhibits bladder carcinoma cell lines RT4 and TCCSUP, ovarian carcinoma cell line A2780, colon carcinoma cell line HT-29, glioblastoma cell lines U-373MG and U-87MG, and melanoma cell lines SK-MEL-2 and HT-144 with IC50 of 11 μM, 15 μM, 0.17 μM, 0.97 μM, 2.95 μM, 17.6 μM, 30.9 μM and 7.85 μM, respectively. [4] |
|||
|---|---|---|---|---|
| Cell Research | Cell lines | RT4, TCCSUP, A2780, HT-29, U-373MG, U-87MG, SK-MEL-2 and HT-144 cell lines | ||
| Concentrations | ~100 μM | |||
| Incubation Time | 48 hours | |||
| Method | The cytotoxicity studies are carried out with the sulforhodamine-B microculture colorimetrie assay. Typically, cells are plated into 96-well plates on day 0 and exposed to Oxaliplatin on day 1; the sulforhodamine-B assay is carried out 48 h after Oxaliplatin exposure. The plates are incubated at 37 °C in 5% CO2 and 100% relative humidity at all times except when adding Oxaliplatin and during the final assay period. The initial number of cells plated for the assay ranged from 2-20 × 103 cells/50 /nL/well. The numbers of cells for plating and the drug exposure time are based on pilot studies using the criteria that (a) the cells in control wells are still in the log phase of growth on the day of the assay; (b) the maximum absorbance for the untreated controls on the day of the assay is in the range of 1.0 to 1.5; and (c) cells go through >2 doublings during the drug exposure. Eight wells are used per concentration. The plates are read at 570 and/or 540 nm using a Biotek Instruments model EL309 microplate reader interfaced with an IBM PC-compatible computer. The data are transferred and transformed into a LOTUS 1-2-3 format by the computer program DATALOG, and survival fractions are calculated by comparing the drug treated with control |
|||
| Experimental Result Images | Methods | Biomarkers | Images | PMID |
| Western blot | VEGFR-1 / NRP-1 p-AKT(Ser473) / AKT / PTEN / p-Src(Tyr416) p-Src(Y418) / p-FAK(Y861) |
|
18790786 | |
| Immunofluorescence | E-cadherin / Vimentin ATXN2L / G3BP1 |
|
30787271 | |
| Growth inhibition assay | Cell viability |
|
28339092 | |
| In Vivo | ||
| In vivo | A weekly i.p. injection of Oxaliplatin at 10 mg/kg to nude mice bearing hepatocellular HCCLM3 tumors significantly reduces tumor volume and apoptotic index. [6] Oxaliplatin (5mg/kg, i.v. on days 1, 5 and 9) is active on T-leukemia-lymphoma L40 AKR with T/C of 1.77. Oxaliplatin is also efficient on intracerebrally grafted L1210 leukemia, MA 16-C xenografts, B16 melanoma xenografts, Lewis lung xenografts and C26 colon carcinoma xenografts. [7] Oxaliplatin induces impairment of retrograde neuronal transport in mice. [8] |
|
|---|---|---|
| Animal Research | Animal Models | Human hepatocellular carcinoma xenografts HCCLM3 |
| Dosages | 10 mg/kg | |
| Administration | A weekly i.p. injection | |
| NCT Number | Recruitment | Conditions | Sponsor/Collaborators | Start Date | Phases |
|---|---|---|---|---|---|
| NCT06320301 | Recruiting | Biliary Tract Cancer|Gemox Chemotherapy |
Sun Yat-Sen Memorial Hospital of Sun Yat-Sen University|Suzhou Suncadia Biopharmaceuticals Co. Ltd. |
April 1 2024 | Phase 2 |
| NCT05922358 | Not yet recruiting | Gastrointestinal Tumors |
Fujian Cancer Hospital |
September 1 2023 | Phase 2 |
| NCT05780684 | Recruiting | Colorectal Cancer|Esophagus Cancer|Appendix Cancer|Small Bowel Cancer|Ampullary Cancer |
Dartmouth-Hitchcock Medical Center |
July 14 2023 | Not Applicable |
| NCT05322590 | Recruiting | Metastatic Colorectal Carcinoma|Neuropathy |
Bexion Pharmaceuticals Inc.|ICON plc|CTI Clinical Trial and Consulting Services |
January 9 2023 | Phase 1|Phase 2 |
Chemical Information & Solubility
| Molecular Weight | 397.29 | Formula | C8H14N2O4Pt |
| CAS No. | 61825-94-3 | SDF | Download Oxaliplatin SDF |
| Smiles | C1CCC(C(C1)[NH-])[NH-].C(=O)(C(=O)O)O.[Pt+2] | ||
| Storage (From the date of receipt) | 2 years 4°C(in the dark) powder | Solutions are unstable. Prepare fresh or purchase small, pre-packaged sizes. Repackage upon receipt. | |
|
In vitro |
Water : 2 mg/mL Ethanol : Insoluble |
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In vivo Add solvents to the product individually and in order. |
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Answers to questions you may have can be found in the inhibitor handling instructions. Topics include how to prepare stock solutions, how to store inhibitors, and issues that need special attention for cell-based assays and animal experiments.
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Frequently Asked Questions
Question 1:
Is it ok to dissolve Oxaliplatin in saline?
Answer:
Oxaliplatin is partially converted to cisplatin and L-isomers when dissolved in saline. The L-isomer of oxaliplatin is inactive. DMF is a better choice.
Question 2:
Is it ok to dissolve Oxaliplatin in DMSO?
Answer:
Even though cis-platin is soluble in DMSO, the use of DMSO to dissolve cis– or trans-diamminedichloroplatinum (DDP) in biological studies is strongly discouraged. The DMSO inserts itself into the ligand and inactivates platin-containing compounds. DMF is a much better choice than DMSO.
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