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RSS FeedsA thiazole-derived oridonin analogue exhibits antitumor activity by directly and allosterically inhibiting STAT3 [Gene Regulation] (Journal of Biological Chemistry)

 
 

15 november 2019 11:02:53

 
A thiazole-derived oridonin analogue exhibits antitumor activity by directly and allosterically inhibiting STAT3 [Gene Regulation] (Journal of Biological Chemistry)
 


Constitutive activation of signal transducer and activator of transcription 3 (STAT3) occurs in ~70% of human cancers, and STAT3 is regarded as one of the most promising targets for cancer therapy. However, specific direct STAT3 inhibitors remain to be developed. Oridonin is an ent-kaurane plant-derived diterpenoid with anti-cancer and anti-inflammatory activities. Here, using an array of cell-based and biochemical approaches, including cell proliferation and apoptosis assays, pulldown and reporter gene assays, site-directed mutagenesis, and molecular dynamics analyses, we report that a thiazole-derived oridonin analogue, CYD0618, potently and directly inhibits STAT3. We found that CYD0618 covalently binds to Cys-542 in STAT3 and suppresses its activity through an allosteric effect, effectively reducing STAT3 dimerization and nuclear translocation, as well as decreasing expression of STAT3-targeted oncogenes. Remarkably, CYD0618 not only strongly inhibited growth of multiple cancer cell lines that harbor constitutive STAT3 activation, but it also suppressed in vivo tumor growth via STAT3 inhibition. Taken together, our findings suggest Cys-542 as a druggable site for selectively inhibiting STAT3 and indicate that CYD0618 represents a promising lead compound for developing therapeutic agents against STAT3-driven diseases.


 
183 viewsCategory: Biochemistry
 
Kinetic and structural evidence that Asp-678 plays multiple roles in catalysis by the quinoprotein glycine oxidase [Bioenergetics] (Journal of Biological Chemistry)
The transcription factor PU.1 mediates enhancer-promoter looping that is required for IL-1{beta} eRNA and mRNA transcription in mouse melanoma and macrophage cell lines [Immunology] (Journal of Biological Chemistry)
 
 
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