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LEE011 (Ribociclib) CDK4/6-Inhibitor
Kat.-Nr.S7440
Chemische Struktur
Molekulargewicht: 434.54
Qualitätskontrolle
Zellkultur, Behandlung & Arbeitskonzentration
| Zelllinien | Assay-Typ | Konzentration | Inkubationszeit | Formulierung | Aktivitätsbeschreibung | PMID |
|---|---|---|---|---|---|---|
| DFSP105 | Growth Inhibition Assay | 24 h | GI50=276 nM | 25852058 | ||
| Myoblast | Growth Inhibition Assay | 72 h | IC50=1035 nM | 25810375 | ||
| IMRS | Growth Inhibition Assay | 72 h | IC50=873 nM | 25810375 | ||
| SKNAS | Growth Inhibition Assay | 72 h | IC50>10000 nM | 25810375 | ||
| Rh28 | Growth Inhibition Assay | 72 h | IC50=845 nM | 25810375 | ||
| Rh41 | Growth Inhibition Assay | 72 h | IC50=7187 nM | 25810375 | ||
| CW9019 | Growth Inhibition Assay | 72 h | IC50=9912 nM | 25810375 | ||
| Rh5 | Growth Inhibition Assay | 72 h | IC50>10000 nM | 25810375 | ||
| Rh30 | Growth Inhibition Assay | 72 h | IC50>10000 nM | 25810375 | ||
| 778 | Growth Inhibition Assay | 72 h | inhibits cell growth dose dependently | 25028469 | ||
| 449 | Growth Inhibition Assay | 72 h | inhibits cell growth dose dependently | 25028469 | ||
| LP3 | Growth Inhibition Assay | 72 h | inhibits cell growth dose dependently | 25028469 | ||
| LP6 | Growth Inhibition Assay | 72 h | inhibits cell growth dose dependently | 25028469 | ||
| LP8 | Growth Inhibition Assay | 72 h | inhibits cell growth dose dependently | 25028469 | ||
| LPS141 | Growth Inhibition Assay | 72 h | inhibits cell growth dose dependently | 25028469 | ||
| 778 | Growth Inhibition Assay | 3.33 μM | 24 h | decreases the proportion of cells in S phase | 25028469 | |
| 449 | Growth Inhibition Assay | 3.33 μM | 24 h | decreases the proportion of cells in S phase | 25028469 | |
| LP3 | Growth Inhibition Assay | 3.33 μM | 24 h | decreases the proportion of cells in S phase | 25028469 | |
| LP6 | Growth Inhibition Assay | 3.33 μM | 24 h | decreases the proportion of cells in S phase | 25028469 | |
| LP8 | Growth Inhibition Assay | 3.33 μM | 24 h | decreases the proportion of cells in S phase | 25028469 | |
| LPS141 | Growth Inhibition Assay | 3.33 μM | 24 h | decreases the proportion of cells in S phase | 25028469 | |
| IMR5 | Growth Inhibition Assay | 24 h | DMSO | IC50=126 nM | 24045179 | |
| BE2C | Growth Inhibition Assay | 24 h | DMSO | IC50=134 nM | 24045179 | |
| 1643 | Growth Inhibition Assay | 24 h | DMSO | IC50=147 nM | 24045179 | |
| SKNSH | Growth Inhibition Assay | 24 h | DMSO | IC50=148 nM | 24045179 | |
| SY5Y | Growth Inhibition Assay | 24 h | DMSO | IC50=154 nM | 24045179 | |
| NGP | Growth Inhibition Assay | 24 h | DMSO | IC50=175 nM | 24045179 | |
| KELLY | Growth Inhibition Assay | 24 h | DMSO | IC50=220 nM | 24045179 | |
| CHP134 | Growth Inhibition Assay | 24 h | DMSO | IC50=273 nM | 24045179 | |
| NLF | Growth Inhibition Assay | 24 h | DMSO | IC50=328 nM | 24045179 | |
| LAN5 | Growth Inhibition Assay | 24 h | DMSO | IC50=429 nM | 24045179 | |
| NB69 | Growth Inhibition Assay | 24 h | DMSO | IC50=738 nM | 24045179 | |
| SKNDZ | Growth Inhibition Assay | 24 h | DMSO | IC50=801 nM | 24045179 | |
| NBSD | Growth Inhibition Assay | 24 h | DMSO | IC50=1900 nM | 24045179 | |
| SKNF1 | Growth Inhibition Assay | 24 h | DMSO | IC50=3500 nM | 24045179 | |
| EBC1 | Growth Inhibition Assay | 24 h | DMSO | IC50=6400 nM | 24045179 | |
| SKNAS | Growth Inhibition Assay | 24 h | DMSO | IC50>10000 nM | 24045179 | |
| NB16 | Growth Inhibition Assay | 24 h | DMSO | IC50>10000 nM | 24045179 | |
| RPE1 | Growth Inhibition Assay | 24 h | DMSO | IC50>10000 nM | 24045179 | |
| Sf21 | Function assay | 10 mins | Inhibition of recombinant human full length N-terminal GST-tagged CDK4/Cyclin-D3 co-expressed in baculovirus infected sf21 cells using Rb substrate in presence of [gamma33P]ATP after 10 mins by scintillation counting method, IC50 = 0.013 μM. | 29518312 | ||
| Sf21 | Function assay | 10 mins | Inhibition of recombinant human full length C-terminal 6His-tagged CDK9/Cyclin-T1 co-expressed in baculovirus infected sf21 cells using PDKtide substrate in presence of [gamma33P]ATP after 10 mins by scintillation counting method, IC50 = 0.197 μM. | 29518312 | ||
| HepG2 | Antiproliferative assay | 72 hrs | Antiproliferative activity against human HepG2 cells after 72 hrs by CelTiter-Glo assay, EC50 = 0.2862 μM. | 29407975 | ||
| SEM | Antiproliferative assay | 72 hrs | Antiproliferative activity against human SEM cells after 72 hrs by CelTiter-Glo assay, EC50 = 0.4605 μM. | 29407975 | ||
| KOPN8 | Antiproliferative assay | 72 hrs | Antiproliferative activity against human KOPN8 cells after 72 hrs by CelTiter-Glo assay, EC50 = 0.5008 μM. | 29407975 | ||
| NCI-H1299 | Cytotoxicity assay | 72 hrs | Cytotoxicity against human NCI-H1299 cells assessed as reduction in cell viability after 72 hrs by CCK8 assay, IC50 = 5.46 μM. | 29518312 | ||
| T47D | Growth inhibition assay | 72 hrs | Growth inhibition of human T47D cells incubated for 72 hrs by CCK8 assay, IC50 = 6.227 μM. | 28651979 | ||
| T47D | Cytotoxicity assay | 72 hrs | Cytotoxicity against human T47D cells assessed as reduction in cell viability after 72 hrs by CCK8 assay, IC50 = 6.23 μM. | 29518312 | ||
| H1299 | Growth inhibition assay | 72 hrs | Growth inhibition of human H1299 cells incubated for 72 hrs by CCK8 assay, IC50 = 7.637 μM. | 28651979 | ||
| KOPN8 | Apoptosis assay | 0.5 uM | 3 hrs | Induction of apoptosis in human KOPN8 cells assessed as upregulation of cleaved PARP level at 0.5 uM after 3 hrs by Western blot analysis | 29407975 | |
| KOPN8 | Apoptosis assay | 0.5 uM | 24 hrs | Induction of apoptosis in human KOPN8 cells assessed as upregulation of cleaved PARP level at 0.5 uM pre-treated with NAC for 1 hr and measured after 24 hrs by Western blot analysis | 29407975 | |
| Hep3B | Cell cycle assay | 24 hrs | Cell cycle arrest in human Hep3B cells assessed as accumulation at G0/G1 phase after 24 hrs by propidium iodide staining based flow cytometry | 29518312 | ||
| HepG2 | Cell cycle assay | 24 hrs | Cell cycle arrest in human HepG2 cells assessed as accumulation at G0/G1 phase after 24 hrs by propidium iodide staining based flow cytometry | 29518312 | ||
| A549 | Cell cycle assay | 24 hrs | Cell cycle arrest in human A549 cells assessed as accumulation at G0/G1 phase after 24 hrs by propidium iodide staining based flow cytometry | 29518312 | ||
| NCI-H460 | Cell cycle assay | 24 hrs | Cell cycle arrest in human NCI-H460 cells assessed as accumulation at G0/G1 phase after 24 hrs by propidium iodide staining based flow cytometry | 29518312 | ||
| T47D | Cell cycle assay | 24 hrs | Cell cycle arrest in human T47D cells assessed as accumulation at G0/G1 phase after 24 hrs by propidium iodide staining based flow cytometry | 29518312 | ||
| MDA-MB-231 | Cell cycle assay | 24 hrs | Cell cycle arrest in human MDA-MB-231 cells assessed as accumulation at G0/G1 phase after 24 hrs by propidium iodide staining based flow cytometry | 29518312 | ||
| Fluc-labeled 4T1 | Antitumor assay | 130 mg/kg | 18 days | Antitumor activity against mouse Fluc-labeled 4T1 cells implanted in Balb/c mouse assessed as reduction in tumor weight at 130 mg/kg, ip administered daily for 18 days measured after 8 to 25 days | 29518312 | |
| T47D | Cell cycle assay | 24 hrs | Induction of cell cycle arrest in human T47D cells assessed as increase in G0/G1 phase accumulation incubated for 24 hrs by flow cytometry | 28651979 | ||
| Klicken Sie hier, um weitere experimentelle Daten zu Zelllinien anzuzeigen | ||||||
Chemische Informationen, Lagerung & Stabilität
| Molekulargewicht | 434.54 | Formel | C23H30N8O |
Lagerung (Ab dem Eingangsdatum) | |
|---|---|---|---|---|---|
| CAS-Nr. | 1211441-98-3 | SDF herunterladen | Lagerung von Stammlösungen |
|
|
| Synonyme | LEE011 | Smiles | CN(C)C(=O)C1=CC2=CN=C(N=C2N1C3CCCC3)NC4=NC=C(C=C4)N5CCNCC5 | ||
Löslichkeit
|
In vitro |
DMSO
: 8 mg/mL
(18.41 mM)
Water : Insoluble Ethanol : Insoluble |
Molaritätsrechner
|
In vivo |
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In-vivo-Formulierungsrechner (Klare Lösung)
Schritt 1: Geben Sie die untenstehenden Informationen ein (Empfohlen: Ein zusätzliches Tier zur Berücksichtigung von Verlusten während des Experiments)
Schritt 2: Geben Sie die In-vivo-Formulierung ein (Dies ist nur der Rechner, keine Formulierung. Bitte kontaktieren Sie uns zuerst, wenn es im Abschnitt "Löslichkeit" keine In-vivo-Formulierung gibt.)
Berechnungsergebnisse:
Arbeitskonzentration: mg/ml;
Methode zur Herstellung der DMSO-Stammlösung: mg Wirkstoff vorgelöst in μL DMSO ( Konzentration der Stammlösung mg/mL, Bitte kontaktieren Sie uns zuerst, wenn die Konzentration die DMSO-Löslichkeit der Wirkstoffcharge überschreitet. )
Methode zur Herstellung der In-vivo-Formulierung: Nehmen Sie μL DMSO Stammlösung, dann hinzufügenμL PEG300, mischen und klären, dann hinzufügenμL Tween 80, mischen und klären, dann hinzufügen μL ddH2O, mischen und klären.
Methode zur Herstellung der In-vivo-Formulierung: Nehmen Sie μL DMSO Stammlösung, dann hinzufügen μL Maisöl, mischen und klären.
Hinweis: 1. Bitte stellen Sie sicher, dass die Flüssigkeit klar ist, bevor Sie das nächste Lösungsmittel hinzufügen.
2. Achten Sie darauf, das/die Lösungsmittel der Reihe nach hinzuzufügen. Sie müssen sicherstellen, dass die bei der vorherigen Zugabe erhaltene Lösung eine klare Lösung ist, bevor Sie mit der Zugabe des nächsten Lösungsmittels fortfahren. Physikalische Methoden wie Vortex, Ultraschall oder ein heißes Wasserbad können zur Unterstützung des Lösens verwendet werden.
Wirkmechanismus
| Merkmale |
Orally bioavailable CDK4/6-selective inhibitor that has been tested in Phase III clinical trials for treatment of advanced breast cancer.
|
|---|---|
| Targets/IC50/Ki |
CDK4
(Cell-free assay) 10 nM
CDK6
(Cell-free assay) 39 nM
|
| In vitro |
LEE011 hemmt als dualer CDK4/CDK6-Inhibitor signifikant das Wachstum von 12 von 17 Neuroblastom-Zelllinien mit einer mittleren IC50 von 307 nM. Die Wachstumshemmung von Neuroblastom-Zelllinien ist primär zytostatisch und wird durch einen G1-Cell Cycle-Arrest und zelluläre Seneszenz vermittelt. |
| In vivo |
LEE011 (200 mg/kg täglich, p.o.) bewirkt eine signifikante Verzögerung des Tumorwachstums bei Mäusen, die BE2C- oder 1643-Xenografts tragen, ohne Gewichtsverlust oder andere Anzeichen von Toxizität. |
Literatur |
|
Anwendungen
| Methoden | Biomarker | Bilder | PMID |
|---|---|---|---|
| Western blot | pRb(S807) / Rb / p53 / Cyclin E / Cyclin D1 / CDK4 / CDK6 / p27 / p21 / PARP |
|
29789630 |
| Growth inhibition assay | Cell viability |
|
26390342 |
Klinische Studieninformationen
(Daten von https://clinicaltrials.gov, aktualisiert am 2024-05-22)
| NCT-Nummer | Rekrutierung | Erkrankungen | Sponsor/Kooperationspartner | Startdatum | Phasen |
|---|---|---|---|---|---|
| NCT05843253 | Not yet recruiting | High Grade Glioma|Diffuse Intrinsic Pontine Glioma|Anaplastic Astrocytoma|Glioblastoma|Glioblastoma Multiforme|Diffuse Midline Glioma H3 K27M-Mutant|Metastatic Brain Tumor|WHO Grade III Glioma|WHO Grade IV Glioma |
Nationwide Children''s Hospital|Novartis |
May 30 2024 | Phase 2 |
| NCT06075758 | Recruiting | Breast Cancer |
Novartis Pharmaceuticals|Novartis |
March 7 2024 | -- |
| NCT05996107 | Recruiting | Breast Cancer |
University of Michigan Rogel Cancer Center |
February 27 2024 | Phase 1 |
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