cancer
IL-1R in inactive conformations.
- Which are highly ligand efficient, kinase selective and cellular active.
- Vogler M, Weber K, Dinsdale D, Schmitz I, Schulze-Osthoff K, Dyer MJS, Cohen GM. Different types of cell death induced by putative BCL2 inhibitors.
- Carrageenan is in widespread commercial use as a thickener in a variety of cosmetic and foods, which range from sexual lubricants to infant feeding formulas.
- Herein, we report structure-activity relationships of the class of cinnamides for selective lethality towards CSC-enriched populations.
- MicroRNAs are small non-coding RNAs regulating the expression of several target genes.
Akgul C. Mcl-1 is really a potential therapeutic target in multiple forms of cancer.
Significant advancements have already been made over the past couple of years towards the discovery of Mcl-1 inhibitors.
However, the Mcl-1 inhibitors described to date are still at an extremely early stage.
source and set the stage for exploring MtbAldR as a potential anti-tuberculosis target.
© 2016 by The American Society for Biochemistry and Molecular Biology, Inc.
Currently challenged in clinical trials as one of the most promising antiviral drug class, and possibly among the first anti-HCV agents to be approved for the treating HCV infection.
To counteract this development, we propose “pathway drug cocktails”, that’s, drug combinations aimed at parallel pathways.
Hydroxamic acid derivatives as potent peptide deformylase inhibitors and antibacterial agents.
CD4-specific designed ankyrin repeat proteins are novel potent HIV entry inhibitors with original characteristics.
STK33 kinase inhibitor BRD-8899 has no effect on KRAS-dependent cancer cell viability.
This could herald the initial success for a chemokine receptor antagonist as an anti-inflammatory therapeutic and confirms the importance of chemokine receptors as a target class for anti-inflammatory and autoimmune diseases.
Drug conjugated to an ADC, and could be useful in ensuring the product quality, efficacy and the safety of ADCs.
An enzymatic deconjugation way for the analysis of small molecule active drugs on antibody-drug conjugates.
Of most tested P-type ATPases from fungal (Pma1p; H+-ATPase), plant (AHA2; H+-ATPase) and animal (SERCA; Ca2+-ATPase) cells.
All three curcuminoids acted as non-competitive antagonist to ATP and hence may bind to a highly conserved allosteric site…
- Furthermore, Mcl-1 overexpression induces resistance contrary to the aforementioned Bcl-2-inhibitors, as well as a number of widely used anticancer therapies including paclitaxel (Wertz et al., 2011), vincristine (Wertz et al., 2011) and gemcitabine (Wei et al., 2008).
- The synthesis and the structure-activity relationships derived from in vitro studies are presented.
- DNA methylation is a major factor that regulates gene expression in cells, and an increase in DNA methylation can block the genes that regulate cell division and growth.
- harmane or other related beta-carbolines could be potential candidates as endogenous ligands of the benzodiazepine receptor.
harmane or other related beta-carbolines could be potential candidates as endogenous ligands of the benzodiazepine receptor.
Plasmin substrate binding site cooperativity guides the design of potent peptide aldehyde inhibitors .
These compounds serve as promising leads for the development of novel antimalarial agents.
Synthesis of gallinamide A analogues as potent falcipain inhibitors and antimalarials.
A little molecule inhibitor of ETV1, YK-4-279, prevents prostate cancer growth and metastasis in a mouse xenograft model.
Of the BH3-only proteins, Bim and Puma are the least selective, binding to all five anti-apoptotic proteins.
Bad binds strongly to Bcl-2, Bcl-XL and Bcl-w; whereas, Noxa binds exclusively to Mcl-1 and Bfl-1/A1.
Members of the Bcl-2 family proteins share conserved sequences in regions referred to as Bcl-2 homology domains (BH1–BH4) (Korsmeyer, 1999, Pang et al., 2012).
Members within the same family might have opposite effects.
The anti-apoptotic or pro-survival proteins, including Bcl-2, Bcl-XL, Bcl-w, Bfl-1/A1 and Mcl-1 (Adams & Cory, 2007), keep cells alive; whereas, the pro-apoptotic proteins (e.g., Bim, tBid, Bad, Puma, Noxa, Bak, and Bax) (Youle & Strasser, 2008) promote cell death.
The relative levels of the anti- and pro-apoptotic proteins govern whether a cell will live or die.
Reversed the inhibitory aftereffect of GKRP on GK activity and promoted GK translocation both in vitro and in vivo .
A co-crystal structure of full-length human GKRP in complex with AMG-1694 revealed a previously unknown binding pocket in GKRP distinct from and features which make it unique on the list of anti-apoptotic Bcl-2 members of the family.
Mcl-1 can be unique in that it includes a very short half-life of h, depending on cellular conditions (Yang-Yen, 2006), and multiple pathways tightly regulate Mcl-1 transcription, translation, and degradation (Thomas et al., 2010).
Structurally, Mcl-1’s N-terminus also differs from that of the other anti-apoptotic Bcl-2 proteins in that it contains two PEST (proline/glutamic acid/serine/threonine-containing) regions (Germain & Duronio, 2007).