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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
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GPCR & G Protein
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Endocrinology & Hormones
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Transmembrane Transporters
- CD markers
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- SGLT
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Metabolism
- PPAR
- P450 (e.g. CYP17)
- HSP (HSP90)
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- Hydroxylase
- Factor Xa
- DHFR
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- Dehydrogenase
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- DPP
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- FAAH
- Acyltransferase
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- phosphatase
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- HMG-CoA Reductase
- Vitamin
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- Lipase
- FOX
- Fatty Acid Synthase
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- ACE
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- Mannosidase
- PGC-1α
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- Aldose Reductase
- CPSase
- Leukotriene
- Adenosine Deaminase
- OXPHOS
- Glutathione
- Acetyl-CoA carboxylase
- Adenosine Kinase
- Peroxidases
- SHIP
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- Mitochondrial Metabolism
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- PREP
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- Neprilysin
Proteases
- HDAC
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- Aminopeptidase
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- DPP
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- MMP
- Thrombin
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- Cysteine Protease
- MALT
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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
- 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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Binding of the anticancer drug BI-2536 to human serum albumin. A spectroscopic and theoretical study

by Selleckchem | Mar 01 2019

BI-2536 is a potent Polo-like kinase inhibitor which induces apoptosis in diverse human cancer cell lines. The binding affinity of BI-2536 for human serum albumin (HSA) protein may define its pharmacokinetic and pharmacodynamic profile. We have studied the binding of BI-2536 to HSA by means of different spectroscopic techniques and docking calculations. We have experimentally observed that the affinity of BI-2536 for HSA is higher than that of other common HSA binding drugs. Therefore, it can be postulated that the drug dose should be increased to achieve a certain concentration of free drug in plasma, although BI-2536could also reach tumour tissues by uptaking HSA/BI-2536 complex. Only a single binding site on HSA has been observed for BI-2536 which seems to correspond to the subdomain IIA pocket. The formation of the HSA/BI-2536 complex is a spontaneous and entropy-driven process that does not cause a significant change of the secondary structure of the protein. Its endothermic character could be related to proton release. Thermodynamic analysis showed that the main protein-drug interactions are of the van der Waals type although the presence of amide and ether groups in BI-2536 could also allow H-bonding with some residues in the subdomain IIA pocket.

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Cat.No.	Product Name	Information
S1109	BI 2536	BI-2536 is a potent Plk1 inhibitor with IC50 of 0.83 nM in a cell-free assay. BI-2536 inhibits Bromodomain 4 (BRD4) with Kd of 37 nM and potently suppresses c-Myc expression. BI-2536 induces apoptosis and attenuates autophagy. Phase 2.

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