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Stem Cells & Wnt
- GSK-3
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Hippo
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Ubiquitin
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NF-κB
- HDAC
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GPCR & G Protein
- Ras
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- PAFR
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- cAMP
- CXCR
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- CRFR
- PKG
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- Imidazoline Receptor
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- RGS
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- Sigma Receptor
- Melanocortin Receptor
- PAR
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- NPY receptor
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- DOCK
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- GPCR19
- Guanylate Cyclase
- GHSR
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- GRK
- Leukotriene
- FPR
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- TSH Receptor
- PKD
- GNRH Receptor
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Endocrinology & Hormones
- Adrenergic Receptor
- 5-alpha Reductase
- Estrogen/progestogen Receptor
- Androgen Receptor
- RAAS
- Opioid Receptor
- Aromatase
- GPR
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- GHSR
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- THR
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Transmembrane Transporters
- CD markers
- Calcium Channel
- Sodium Channel
- ATPase
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- Potassium Channel
- GluR
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- GABA Receptor
- P-gp
- Proton Pump
- CFTR
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- SGLT
- GLUT
- GlyT
- NMDAR
- OCT
- CRM1
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- NCX
- OATP
- TRP Channel
- VRAC
- Aquaporin
- EAAT
- VDAC
- MTP
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- MCT
- Amino acid transporter
- OAT
- Mechanosensitive Channel
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
- FXR
- Transferase
- CETP
- Serine/threonin kinase
- IDO/TDO
- phosphatase
- GLUT
- HMG-CoA Reductase
- Vitamin
- PKM
- Lipoxygenase
- FOX
- Lipase
- Fatty Acid Synthase
- LDL
- NAMPT
- Decarboxylase
- Casein Kinase
- Thioredoxin
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- Peroxidases
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- Neprilysin
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- CAR
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- LDH
- γGCS
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- FTase
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- FAO
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- GOT
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- GTPCH
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- Epoxide Hydrolase
- ACSS2
- ROR
- Catalase
- THR
- Thioredoxin Reductase
- PDHK
- Glucosylceramide Synthase
- ACE
- Mannosidase
- PGC-1α
- PARG
- Xanthine Oxidase
- CPSase
- Leukotriene
- Adenosine Deaminase
- Aldose Reductase
- Glutathione
- Acetyl-CoA carboxylase
- Adenosine Kinase
- OXPHOS
Proteases
- HDAC
- Proteasome
- Caspase
- Aminopeptidase
- HCV Protease
- DPP
- HIV Protease
- MMP
- Thrombin
- Acyltransferase
- Tyrosinase
- Serine Protease
- Cysteine Protease
- MALT
- Glutaminase
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- PGDS
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- PAD
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Microbiology
- HCV Protease
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- Anti-infection
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- SARS-CoV
Others
- ADC Cytotoxin
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- Antineoplastic and Immunosuppressive Antibiotics
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- 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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Exploiting Temporal Collateral Sensitivity in Tumor Clonal Evolution.

by Selleckchem | Jun 17 2017

The prevailing approach to addressing secondary drug resistance in cancer focuses on treating the resistance mechanisms at relapse. However, the dynamic nature of clonal evolution, along with potential fitness costs and cost compensations, may present exploitable vulnerabilities-a notion that we term "temporal collateral sensitivity." Using a combined pharmacological screen and drug resistance selection approach in a murine model of Ph(+) acute lymphoblastic leukemia, we indeed find that temporal and/or persistent collateral sensitivity to non-classical BCR-ABL1 drugs arises in emergent tumor subpopulations during the evolution of resistance toward initial treatment with BCR-ABL1-targeted inhibitors. We determined the sensitization mechanism via genotypic, phenotypic, signaling, and binding measurements in combination with computational models and demonstrated significant overall survival extension in mice. Additional stochastic mathematical models and small-molecule screens extended our insights, indicating the value of focusing on evolutionary trajectories and pharmacological profiles to identify new strategies to treat dynamic tumor vulnerabilities.

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