Akt inhibitors in cancer treatment: The long journey from drug discovery to clinical use (Review)

Nițulescu, George Mihai; Margină, Denisa; Juzenas, Petras; Peng, Qian; Olaru, Octavian Tudorel; Saloustros, Emmanouil; Fenga, Concettina; Spandidos, Demetrios Α.; Libra, Massimo; Tsatsakis, Aristidis

doi:10.3892/ijo.2015.3306

Cited by 302 publications

(263 citation statements)

References 146 publications

Supporting

Mentioning

261

Contrasting

Unclassified

Order By: Relevance

“…These highly homologous isoforms phosphorylate a plethora of substrates that are involved in the regulation of key cellular processes including cell proliferation, apoptosis, and migration (94). It is well established that constitutive activation of Akt, through PI3K amplification or PTEN mutation, contributes to the oncogenic process and is associated with a poor prognosis and resistance to chemo-and radio-therapy (94). Indeed, Akt activation is one of the most frequent molecular alterations in cancers, including melanoma, gastric, pancreatic, breast, sarcoma and prostate cancer (95)(96)(97)(98).…”

Section: Phosphatidylinositol 3-kinase/protein Kinase B (Pi3k/akt) Simentioning

confidence: 99%

The T-Box transcription factor 3 in development and cancer

Willmer

Cooper

Peres

et al. 2017

BST

View full text Add to dashboard Cite

Section: Phosphatidylinositol 3-kinase/protein Kinase B (Pi3k/akt) Simentioning

confidence: 99%

The T-Box transcription factor 3 in development and cancer

Willmer

Cooper

Peres

et al. 2017

BST

View full text Add to dashboard Cite

“…Most AKT inhibitors, including ARQ 092, are being developed as anti-cancer drugs. 25 Given the fact that some cancer patients are at high risk of thrombogenesis, 37 our results also provide indirect evidence that ARQ 092 may be an effective drug in cancer patients with thrombotic complications.…”

Section: Discussionmentioning

confidence: 67%

“…24,25 ARQ 092 has been reported to be an orallyavailable, highly-selective AKT inhibitor. 26,27 Recent studies show that ARQ 092 blocks the activity of AKT1, AKT2, and AKT3 with IC 50 values of 5.0, 4.5, and 16 nM, respectively, and has excellent selectivity (>1,000-fold) over other kinases.…”

Section: Introductionmentioning

confidence: 99%

ARQ 092, an orally-available, selective AKT inhibitor, attenuates neutrophil-platelet interactions in sickle cell disease

Barazia

Tseng

et al. 2016

Haematologica

View full text Add to dashboard Cite

“…This need is reflected in clinical trials which show that non-specific Akt inhibition in cancer therapy, due to inadvertent off-targeting of closely related kinases or multiple Akt isozymes, can result in detrimental side-effects including liver damage and metabolic disorders [37][38][39][40]. Accordingly, the development of small molecule inhibitors for Akt has reflected this sentiment towards engineering greater target specificity [28]. From the earliest ATP-competitive inhibitors that unintentionally inhibited related AGC kinases, to more recent allosteric inhibitors that preferentially target Akt or even a subset of Akt isozymes, the continued pursuit for Akt1 inhibitor specificity requires an expanded understanding of the molecular basis of Akt1 activation and inhibition.…”

Section: Discussionmentioning

confidence: 99%

“…Several classes of chemical inhibitors were developed to repress aberrant Akt1 activity in cancer cells [28]. Early Akt1 inhibitors focused on ATP competitive compounds [29], yet these molecules suffered from significant cross reactivity with other AGC family kinases [30].…”

Section: Chemical Inhibition Of Phosphorylated Akt1 Variantsmentioning

confidence: 99%

Phosphorylation-Dependent Inhibition of Akt1

Balasuriya¹,

McKenna²,

Liu³

et al. 2018

Preprint

View full text Add to dashboard Cite

Akt1 is a proto-oncogene that is over active in most cancers. Akt1 activation requires phosphorylation at Thr308; phosphorylation at Ser473 further enhances catalytic activity. Akt1 activity is also regulated via interactions between the kinase domain and the N-terminal autoinhibitory pleckstrin homology (PH) domain. As it was previously difficult to produce Akt1 in sitespecifically phosphorylated forms, the contribution of each activating phosphorylation site to autoinhibition was unknown. Using a combination of genetic code expansion and in vivo enzymatic phosphorylation, we produced Akt1 variants containing programmed phosphorylation to probe the interplay between Akt1 phosphorylation status and the auto-inhibitory function of the PH domain. Deletion of the PH domain increased the enzyme activity for all three phosphorylated Akt1 variants. For the doubly phosphorylated enzyme, deletion of the PH domain relieved auto-inhibition by 295-fold. We next found that phosphorylation at Ser473 provided resistance to chemical inhibition by Akti-1/2 inhibitor VIII. The Akti-1/2 inhibitor was most effective against pAkt1 T308 and showed 4-fold decreased potency with Akt1 variants phosphorylated at Ser473. The data highlight the need to design more potent Akt1 inhibitors that are effective against the doubly phosphorylated and most pathogenic form of Akt1.

show abstract

Akt inhibitors in cancer treatment: The long journey from drug discovery to clinical use (Review)

Cited by 302 publications

References 146 publications

The T-Box transcription factor 3 in development and cancer

The T-Box transcription factor 3 in development and cancer

ARQ 092, an orally-available, selective AKT inhibitor, attenuates neutrophil-platelet interactions in sickle cell disease

Phosphorylation-Dependent Inhibition of Akt1

Contact Info

Product

Resources

About