AI Article Synopsis
- Pseudokinase TRIB2 plays a significant role in cell regulation and is linked to cancer progression and therapy resistance, making it a potential target for treatment.
- Researchers developed several TRIB2 degraders, notably compound 5k, which showed strong effectiveness in reducing TRIB2 levels in prostate cancer cells.
- Compound 5k not only outperformed traditional TRIB2 binders in inhibiting cancer cell growth but also provides a valuable resource for studying the function of TRIB2 in cancer biology.
Article Abstract
Pseudokinase TRIB2, a member of the CAMK Ser/Thr protein kinase family, regulates various cellular processes through phosphorylation-independent mechanisms. Dysregulation of TRIB2 has been implicated in promoting tumor growth, metastasis, and therapy resistance, making it a promising target for cancer treatment. In this study, we designed and synthesized a series of TRIB2 PROTAC degraders by conjugating a TRIB2 binder 1 with VHL or CRBN ligands via linkers of varying lengths and compositions. Among these compounds, 5k demonstrated potent TRIB2 degradation with a DC value of 16.84 nM (95 % CI: 13.66-20.64 nM) in prostate cancer PC3 cells. Mechanistic studies revealed that 5k directly interacted with TRIB2, selectively inducing its degradation through a CRBN-dependent ubiquitin-proteasomal pathway. Moreover, 5k outperformed the TRIB2 binder alone in inhibiting cell proliferation and inducing apoptosis, confirming that TRIB2 protein degradation could be a promising therapeutic strategy for TRIB2-associated cancers. Additionally, compound 5k also serves as an effective tool for probing TRIB2 biology.
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| http://dx.doi.org/10.1016/j.ejmech.2024.117016 | DOI Listing |
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