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PI3K/Akt/mTOR
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Epigenetics
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Methylation
- DNA Methyltransferase
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- WDR5
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Immunology & Inflammation
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Angiogenesis
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Apoptosis
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Autophagy
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ER stress & UPR
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MAPK
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Cytoskeletal Signaling
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Cell Cycle
- CDK
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- PD-1/PD-L1
- Ras
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- HSP (HSP90)
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TGF-beta/Smad
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DNA Damage/DNA Repair
- HDAC
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- Nucleoside Analog/Antimetabolite
- LIM kinase
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- FENs
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Stem Cells & Wnt
- GSK-3
- JAK
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- TGF-beta/Smad
- Wnt/beta-catenin
- ROCK
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- PKA
- Stemness kinase
- KLF
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Hippo
- LATS
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Ubiquitin
- Proteasome
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Neuronal Signaling
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- P-gp
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- MT Receptor
- MAO
- FAAH
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- Trk receptor
- GlyT
- NMDAR
- CaMK
- Notch
- Imidazoline Receptor
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- NPY receptor
- Serotonin Transporter
- CCK receptor
- Neurotensin Receptor
- COMT
- Melanocortin Receptor
- Adenosine Deaminase
- TRP Channel
- Adenosine Kinase
- BChE
- EAAT
- Neurokinin Receptor
NF-κB
- HDAC
- NF-κB
- IκB/IKK
- MALT
- Nrf2
- ROS
- NOD
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- AP-1
GPCR & G Protein
- Ras
- 5-HT Receptor
- CCR
- GluR
- Adrenergic Receptor
- AChR
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- Dopamine Receptor
- Opioid Receptor
- GPR
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- Endothelin Receptor
- S1P Receptor
- Hedgehog/Smoothened
- SGLT
- LPA Receptor
- OX Receptor
- CGRP Receptor
- MT Receptor
- PAFR
- PKA
- Adenosine Receptor
- Vasopressin Receptor
- cAMP
- CXCR
- TAAR
- CaSR
- Glucagon Receptor
- LTR
- Parathyroid Hormone Receptor
- NPY receptor
- DOCK
- AdipoR
- GPCR19
- Guanylate Cyclase
- GHSR
- CCK receptor
- FPR
- GRK
- Leukotriene
- Prostaglandin Receptor
- PKD
- TSH Receptor
- Neurokinin Receptor
- GNRH Receptor
- CRFR
- PKG
- Bradykinin Receptor
- Angiotensin Receptor
- Bombesin Receptor
- Imidazoline Receptor
- Neurotensin Receptor
- RGS
- Melanocortin Receptor
- Sigma Receptor
- Taste Receptor
- PAR
Endocrinology & Hormones
- Adrenergic Receptor
- 5-alpha Reductase
- Estrogen/progestogen Receptor
- Androgen Receptor
- RAAS
- Opioid Receptor
- Aromatase
- GPR
- Glucocorticoid Receptor
- THR
- ACE
- SSTR
- GHSR
- CCK receptor
- PGES
- TSH Receptor
- GNRH Receptor
- PGDS
- Mineralocorticoid Receptor
Transmembrane Transporters
- CD markers
- Calcium Channel
- Sodium Channel
- ATPase
- Chloride Channel
- Potassium Channel
- GluR
- AChR
- GABA Receptor
- P-gp
- Proton Pump
- CFTR
- P2 Receptor
- SGLT
- GLUT
- GlyT
- NMDAR
- OCT
- CRM1
- MCT
- Amino acid transporter
- OAT
- Mechanosensitive Channel
- BCRP
- NKCC
- NCX
- TRP Channel
- OATP
- VRAC
- Aquaporin
- EAAT
- VDAC
- MTP
- VMAT
- GlyR
Metabolism
- PPAR
- P450 (e.g. CYP17)
- HSP (HSP90)
- PDE
- Hydroxylase
- Factor Xa
- DHFR
- Aminopeptidase
- Dehydrogenase
- Procollagen C Proteinase
- Phospholipase (e.g. PLA)
- DPP
- Carbonic Anhydrase
- Phosphorylase
- Liver X Receptor
- FAAH
- Acyltransferase
- Serine/threonin kinase
- CETP
- IDO/TDO
- phosphatase
- GLUT
- HMG-CoA Reductase
- Vitamin
- PKM
- Lipoxygenase
- FOX
- Lipase
- Fatty Acid Synthase
- LDL
- NAMPT
- Decarboxylase
- Casein Kinase
- Thioredoxin
- Retinoid Receptor
- Transferase
- FXR
- Neprilysin
- PP2A
- FTO
- RUNX
- SREBP
- AdipoR
- PAD
- CPT
- SCD
- CAR
- AP-1
- LDH
- Carbohydrate Metabolism
- γGCS
- SSTR
- PAI-1
- FTase
- SOD
- ATP-citrate lyase
- FAO
- SGK
- GOT
- 3-MST
- GTPCH
- glucocerebrosidase
- FABP
- Serine hydrolase
- Epoxide Hydrolase
- ACSS2
- ROR
- Catalase
- THR
- PDHK
- Glucosylceramide Synthase
- ACE
- Thioredoxin Reductase
- PGC-1α
- PARG
- Xanthine Oxidase
- Mannosidase
- Leukotriene
- Adenosine Deaminase
- Aldose Reductase
- CPSase
- Acetyl-CoA carboxylase
- Adenosine Kinase
- OXPHOS
- Glutathione
- PCSK9
- Mitochondrial Metabolism
- Peroxidases
- SHIP
- PGDS
- Mitochondrial pyruvate carrier
- PREP
Proteases
- HDAC
- Proteasome
- Caspase
- Aminopeptidase
- HCV Protease
- DPP
- HIV Protease
- MMP
- Thrombin
- Acyltransferase
- MALT
- Glutaminase
- Tyrosinase
- Serine Protease
- Cysteine Protease
- PAD
- PCSK9
- Secretase
- Cathepsin B
- PGDS
- Neprilysin
- SGK
- PREP
- GOT
- 3C-Like Protease
Microbiology
- HCV Protease
- Integrase
- Reverse Transcriptase
- HIV Protease
- Anti-infection
- Fungal
- CMV
- Neuraminidase
- Parasite
- Antiviral
- Thioredoxin Reductase
- Bacterial
- β-lactamase
- Antibiotics
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- Enterovirus
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- SARS-CoV
- RSV
- HPV
- HSV
- HCV
- HBV
- HIV
Others
- ADC Cytotoxin
- ADC Linker
- Drug-Linker Conjugates for ADC
- Antineoplastic and Immunosuppressive Antibiotics
- Selection Antibiotics for Transfected Cell
- Antibiotics for Mammalian Cell Culture
- Antibiotics for Plant Cell Culture
- Hydrotropic Agents
- Dyes
- PROTAC
- PROTAC Linker
- E3 ligase Ligand
- Target Protein Ligand
- Others
- Antibody-Drug Conjugate

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PI3 Kinase Pathway and MET Inhibition is Efficacious in Malignant Pleural Mesothelioma

by Selleckchem | Jul 27 2017

Malignant pleural mesothelioma (MPM) is an aggressive cancer that is commonly associated with prior asbestos exposure. Receptor tyrosine kinases (RTKs) such as MET and its downstream target PI3K are overexpressed and activated in a majority of MPMs. Here, we studied the combinatorial therapeutic efficacy of the MET/ALK inhibitor crizotinib, with either a pan-class I PI3K inhibitor, BKM120, or with a PI3K/mTOR dual inhibitor, GDC-0980, in mesothelioma. Cell viability results showed that MPM cells were highly sensitive to crizotinib, BKM120 and GDC-0980 when used individually and their combination was more effective in suppressing growth. Treatment of MPM cells with these inhibitors also significantly decreased cell migration, and the combination of them was synergistic. Treatment with BKM120 alone or in combination with crizotinib induced G2-M arrest and apoptosis. Both crizotinib and BKM120 strongly inhibited the activity of MET and PI3K as evidenced by the decreased phosphorylation of MET, AKT and ribosomal S6 kinase. Using a PDX mouse model, we showed that a combination of crizotinib with BKM120 was highly synergetic in inhibiting MPM tumor growth. In conclusion our findings suggest that dual inhibition of PI3K and MET pathway is an effective strategy in treating MPM as compared to a single agent.

Related Products

Cat.No.	Product Name	Information
S1068	Crizotinib	Crizotinib is a potent inhibitor of c-Met and ALK with IC50 of 11 nM and 24 nM in cell-based assays, respectively. It is also a potent ROS1 inhibitor with Ki value less than 0.025 nM. Crizotinib induces autophagy through inhibition of the STAT3 pathway in multiple lung cancer cell lines.

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