Abstract
Dysregulation of the Wnt/β-catenin signaling pathway is critically involved in gastric cancer (GC) progression. However, current Wnt pathway inhibitors being studied in preclinical or clinical settings for other cancers such as colorectal and pancreatic cancers are either too cytotoxic or insufficiently efficacious for GC. Thus, we screened new potent targets from β-catenin destruction complex associated with GC progression from clinical samples, and found that scaffolding protein RACK1 deficiency plays a significant role in GC progression, but not APC, AXIN, and GSK3β. Then, we identified its upstream regulator UBE2T which promotes GC progression via hyperactivating the Wnt/β-catenin signaling pathway through the ubiquitination and degradation of RACK1 at the lysine K172, K225, and K257 residues independent of an E3 ligase. Indeed, UBE2T protein level is negatively associated with prognosis in GC patients, suggesting that UBE2T is a promising target for GC therapy. Furthermore, we identified a novel UBE2T inhibitor, M435-1279, and suggested that M435-1279 acts inhibit the Wnt/β-catenin signaling pathway hyperactivation through blocking UBE2T-mediated degradation of RACK1, resulting in suppression of GC progression with lower cytotoxicity in the meantime. Overall, we found that increased UBE2T levels promote GC progression via the ubiquitination of RACK1 and identified a novel potent inhibitor providing a balance between growth inhibition and cytotoxicity as well, which offer a new opportunity for the specific GC patients with aberrant Wnt/β-catenin signaling.
Highlights
As one of the most globally prevalent cancers, gastric cancer (GC) has an incidence in the world ranking fifth and mortality ranking third in all kinds of cancers according to “National Cancer Report 2019” published by the National Cancer Center [1]
GC appears to be heterogeneous since both genomic alterations and environmental factors were universally involved in gastric carcinogenesis, which impedes the development of targeted drugs [25, 26]
Previous studies showed that Wnt/ β-catenin signaling hyperactivation could be triggered by virulence factor CagA and VacA of Helicobacter pylori infection in gastric carcinogenesis [29,30,31,32]
Summary
As one of the most globally prevalent cancers, gastric cancer (GC) has an incidence in the world ranking fifth and mortality ranking third in all kinds of cancers according to “National Cancer Report 2019” published by the National Cancer Center [1]. Despite significant progress that has been achieved during the past decade, the improvement of long-term survival for advanced GC patients remains unsatisfactory. The 5-year survival rate of GC patients varies from 30 to 50% after radical gastrectomy combined with chemotherapy [2, 3]. For unresectable GC patients treated with chemotherapy plus trastuzumab, the media survival time could be prolonged from 11.1 to 13.8 months compared with chemotherapy alone [4]. The positive rate of erbB2 is only about 20% in GC patients [5, 6]. It is urgent to identify new therapeutic targets and more effective drugs to further improve the long-term survival of GC patients
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