Litcius/Paper detail

Akt Inhibitor Advancements: From Capivasertib Approval to Covalent-Allosteric Promises

Kosmas Alexandros Pervanidis, G D'Angelo, Jörn Weisner, Sven Brandherm, Daniel Rauh

2024Journal of Medicinal Chemistry36 citationsDOIOpen Access PDF

Abstract

Akt kinase is vital in cell growth, survival, metabolism, and migration. Dysregulation of Akt signaling is implicated in cancer and metabolic disorders. In the context of cancer, overactive Akt promotes cell survival and proliferation. This has spurred extensive research into developing Akt inhibitors as potential therapeutic agents to disrupt aberrant Akt signaling. Akt inhibitors are classified into three main types: ATP-competitive, allosteric, and covalent-allosteric inhibitors (CAAIs). ATP-competitive inhibitors compete with ATP for binding to Akt, allosteric inhibitors interact with the Pleckstrin homology (PH) domain, and covalent-allosteric inhibitors form covalent bonds, making them more potent and selective. Notably, capivasertib (AZD5363), a potent ATP-competitive Akt inhibitor, received FDA approval in November 2023 for use in combination with the estrogen receptor degrader fulvestrant to treat breast cancer. Challenges remain, including improving selectivity, identifying biomarkers to tailor treatments, and enhancing therapeutic efficacy while minimizing adverse effects. Particularly covalent-allosteric inhibitors hold promise for future more effective and personalized treatments.

Topics & Concepts

Allosteric regulationProtein kinase BPleckstrin homology domainChemistryPharmacologyPI3K/AKT/mTOR pathwayFulvestrantBiochemistryCancer researchSignal transductionCancerEstrogen receptorBiologyReceptorInternal medicineMedicineBreast cancerPI3K/AKT/mTOR signaling in cancerCancer Mechanisms and TherapySynthesis and biological activity