The xanthone derivate 5',6'-dimethylxanthenone-4-acetic acid (DMXAA, also known as ASA404 or vadimezan) is a potent agonist of murine STING (stimulator of interferon genes), but cannot activate human STING. Herein we report that α-mangostin, which bears the xanthone skeleton, is an agonist of human STING, but activates murine STING to a lesser extent. Biochemical and cell-based assays indicate that α-mangostin binds to and activates human STING, leading to activation of the downstream interferon regulatory factor (IRF) pathway and production of type I interferons. Furthermore, our studies show that α-mangostin has the potential to repolarize human monocyte-derived M2 macrophages to the M1 phenotype. The agonist effect of α-mangostin in the STING pathway might account for its antitumor and antiviral activities.
The
development of bifunction al molecules, which can
enable targeted
RNA degradation, targeted protein acetylation, or targeted protein
degradation, remains a time-consuming process that requires tedious
optimization. We propose a split-and-mix nanoplatform that serves
as a self-adjustable platform capable of facile screening, programmable
ligand ratios, self-optimized biomolecule spatial recognition, and
multifunctional applications. Herein, we demonstrate the potential
of our proposed nanoplatform by showcasing proteolysis-targeting chimeras
(PROTACs), namely, split-and-mix PROTAC (SM-PROTAC). We highlight
the scope of our platform through the targeted disruption of intracellular
therapeutic targets involving ERα, CDK4/6, AR, MEK1/2, BRD2/4,
BCR-ABL, etc. These studies confirm the effectiveness and universality
of the SM-PROTAC platform for proximity-induced applications. This
platform is programmable, with significant potential applications
to biomolecule regulation, including the fields of epigenetics, gene
editing, and biomolecule modification regulation.
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