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PI3K/Akt/mTOR
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Cell Cycle
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Stem Cells & Wnt
- GSK-3
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NF-κB
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GPCR & G Protein
- Ras
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Endocrinology & Hormones
- Adrenergic Receptor
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Transmembrane Transporters
- CD markers
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Metabolism
- PPAR
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- Hydroxylase
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- FAAH
- Acyltransferase
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- phosphatase
- GLUT
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- Vitamin
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- Lipoxygenase
- FOX
- Lipase
- Fatty Acid Synthase
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- OXPHOS
- Glutathione
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- ATP-citrate lyase
- FAO
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- SOD
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- GTPCH
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- GOT
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- glucocerebrosidase
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- Catalase
- THR
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- ROR
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- ACE
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- PDHK
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- Xanthine Oxidase
- Mannosidase
- PGC-1α
Proteases
- HDAC
- Proteasome
- Caspase
- Aminopeptidase
- HCV Protease
- DPP
- HIV Protease
- MMP
- Thrombin
- Acyltransferase
- MALT
- Glutaminase
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- PGDS
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Microbiology
- HCV Protease
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- Anti-infection
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Others
- ADC Cytotoxin
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- Antineoplastic and Immunosuppressive Antibiotics
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- Hydrotropic Agents
- Dyes
- PROTAC
- PROTAC Linker
- E3 ligase Ligand
- Target Protein Ligand
- Others
- Antibody-Drug Conjugate

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MST2 phosphorylation at serine 385 in mitosis inhibits its tumor suppressing activity

by Selleckchem | Mar 20 2018

Mammalian sterile 20-like kinase 1/2 (MST1/2) are core tumor suppressors in the Hippo signaling pathway. MST1/2 have been shown to regulate mitotic progression. Here, we report a novel mechanism for phospho-regulation of MST2 in mitosis and its biological significance in cancer. We found that the mitotic kinase cyclin-dependent kinase 1 (CDK1) phosphorylates MST2 in vitro and in vivo at serine 385 during antimitotic drug-induced G2/M phase arrest. This phosphorylation occurs transiently during unperturbed mitosis. Mitotic phosphorylation of MST2 does not affect its kinase activity or Hippo-YAP signaling. We further showed that mitotic phosphorylation-deficient mutant MST2-S385A possesses higher activity in suppressing cell proliferation and anchorage-independent growth in vitro and tumorigenesis in vivo. Together, our findings reveal a novel layer of regulation for MST2 in mitosis and its role in tumorigenesis.

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