A PROTAC peptide induces durable β-catenin degradation and suppresses Wnt-dependent intestinal cancer

Aberrant activation of Wnt/β-catenin signaling has been associated with the onset and progression of many types of tumors and thus β-catenin represents one attractive intracellular target for Cancer therapy. Based on the Axin-derived peptide that binds to β-catenin, two stapled Peptides SAHPA1 and xStAx were reported to enhance or impair Wnt/β-catenin signaling, respectively. In this study, we designed PROTACs (proteolysis targeting chimeras) by coupling SAHPA1 or xStAx with the VHL ligand to achieve efficient β-catenin degradation. The obtained xStAx-VHLL sustained β-catenin degradation and manifested strong inhibition of Wnt signaling in Cancer cells and in APC^-/- organoids. Furthermore, xStAx-VHLL could effectively restrain tumor formation in BALB/C nude mice, and diminish the existing tumors in APC^min/+ mice. More importantly, xStAx-VHLL could potently inhibit the survival of colorectal Cancer patient-derived organoids. These findings suggest that xStAx-VHLL exhibits the ability of Cancer prevention and cure, highlighting the potential of β-catenin degrader PROTACs as a new class of promising Anticancer agent.