AI Article Synopsis

  • Compound VBT-5445 is an inhibitor that blocks the interaction of Pim and EDC3, which helps regulate mRNA decay, and it also targets the Pim and mTORC protein kinases.
  • Structural modifications led to a series of VBT analogs that effectively reduce the growth of various cancers, such as pancreatic, prostate, breast, lung, and leukemia.
  • Notably, the GRG-1-34 derivative showed low toxicity in mice and has a suitable pharmacokinetic profile, suggesting it could be a promising candidate for future cancer treatment development.

Article Abstract

Compound VBT-5445 was identified as an inhibitor to block the association of Pim and the protein Enhancer of Decapping 3 (EDC3), a Pim substrate, which normally functions to enhance the decapping of messenger RNA (mRNA). It was also shown to inhibit both the Pim and mTORC protein kinases. The activity of this compound class can be fine-tuned by structural modification. A series of VBT analogs were designed, synthesized, and evaluated. These compounds decrease the growth of multiple cancer types, including pancreas, prostate, breast, lung, and leukemia. Notably, 6-methyl (GRG-1-31, ), 4-Bromo (GRG-1-34, ), 4-Chloro (GRG-1-35, ), and phenylthio substituted (GRG-1-104, ) derivatives are highly potent at inhibiting tumor growth. The ability of these compounds to block cancer growth is highly correlated with their activity as mTORC inhibitors. The toxicity of GRG 1-34 is low in mice treated with twice-daily gavage for 30 days and did not induce weight loss. Pharmacokinetics of a single oral dose demonstrated a peak concentration at 0.5 hours after gavage. In summary, further development of this compound class has the potential to inhibit important signaling pathways and impact cancer treatment.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9648566PMC
http://dx.doi.org/10.1007/s00044-022-02904-zDOI Listing

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