Identification of NVP-BKM120 as a Potent, Selective, Orally Bioavailable Class I PI3 Kinase Inhibitor for Treating Cancer

Burger, Matthew T.; Pecchi, Sabina; Wagman, Allan S.; Ni, Zhi‐Jie; Knapp, Mark; Hendrickson, Thomas F.; Atallah, Gordana; Pfister, Keith; Zhang, Yanchen; Bartulis, Sarah; Frazier, Kelly; Ng, Simon; Smith, Aaron; Verhagen, Joelle; Haznedar, Joshua; Huh, Kay; Iwanowicz, Ed; Xin, Xiaohua; Menezes, Daniel L.; Merritt, Hanne; Lee, Isabelle; Wiesmann, Marion; Kaufman, Susan; Crawford, Kenneth R.; Chin, Michael T.; Bussiere, Dirksen E.; Shoemaker, Kevin R.; Zaror, Isabel; Maira, Sauveur‐Michel; Voliva, Charles F.

doi:10.1021/ml200156t

Cited by 217 publications

(188 citation statements)

References 17 publications

Supporting

Mentioning

176

Contrasting

Unclassified

Order By: Relevance

“…This effort led to the discovery of NVP-BKM120, identified from the pan-PI3K inhibitor lead series 2-morpholino-4-amino-6-pyrimidinyl pyrimidines (MAPP) through a combination of structure-based drug design and optimization of in vivo properties (37). NVP-BKM120 inhibits PI3K in an ATP competitive manner, but this is the result of a mixed effect on K m and V max .…”

Section: Discussionmentioning

confidence: 99%

Identification and Characterization of NVP-BKM120, an Orally Available Pan-Class I PI3-Kinase Inhibitor

Maira

Pecchi

Huang

et al. 2012

Molecular Cancer Therapeutics

Self Cite

468

382

View full text Add to dashboard Cite

Following the discovery of NVP-BEZ235, our first dual pan-PI3K/mTOR clinical compound, we sought to identify additional phosphoinositide 3-kinase (PI3K) inhibitors from different chemical classes with a different selectivity profile. The key to achieve these objectives was to couple a structure-based design approach with intensive pharmacologic evaluation of selected compounds during the medicinal chemistry optimization process. Here, we report on the biologic characterization of the 2-morpholino pyrimidine derivative pan-PI3K inhibitor NVP-BKM120. This compound inhibits all four class I PI3K isoforms in biochemical assays with at least 50-fold selectivity against other protein kinases. The compound is also active against the most common somatic PI3Ka mutations but does not significantly inhibit the related class III (Vps34) and class IV (mTOR, DNA-PK) PI3K kinases. Consistent with its mechanism of action, NVP-BKM120 decreases the cellular levels of p-Akt in mechanistic models and relevant tumor cell lines, as well as downstream effectors in a concentrationdependent and pathway-specific manner. Tested in a panel of 353 cell lines, NVP-BKM120 exhibited preferential inhibition of tumor cells bearing PIK3CA mutations, in contrast to either KRAS or PTEN mutant models. NVP-BKM120 shows dose-dependent in vivo pharmacodynamic activity as measured by significant inhibition of p-Akt and tumor growth inhibition in mechanistic xenograft models. NVP-BKM120 behaves synergistically when combined with either targeted agents such as MEK or HER2 inhibitors or with cytotoxic agents such as docetaxel or temozolomide. The pharmacological, biologic, and preclinical safety profile of NVP-BKM120 supports its clinical development and the compound is undergoing phase II clinical trials in patients with cancer. Mol Cancer Ther; 11(2); 317-28. Ó2011 AACR.

show abstract

Section: Discussionmentioning

confidence: 99%

Identification and Characterization of NVP-BKM120, an Orally Available Pan-Class I PI3-Kinase Inhibitor

Maira

Pecchi

Huang

et al. 2012

Molecular Cancer Therapeutics

Self Cite

468

382

View full text Add to dashboard Cite

show abstract

“…The biochemical activity of NVP-BKM120 was observed for the inhibition of VPS34, mTOR, DNAPK, and PI4K. The drug exerts antitumor activity against two models of PI3K/Akt pathway driven cancers: the A2780 ovarian carcinoma model and the U87MG glioma model, which carry a PTEN deletion [80] . It has also been observed that the inhibition of glioma cells by NVP-BKM120 depends upon the mutational status of p53.…”

Section: Current Progress In Clinical Trialsmentioning

confidence: 99%

PI3K and Akt as molecular targets for cancer therapy: current clinical outcomes

2012

View full text Add to dashboard Cite

The PI3K-Akt pathway is a vital regulator of cell proliferation and survival. Alterations in the PIK3CA gene that lead to enhanced PI3K kinase activity have been reported in many human cancer types, including cancers of the colon, breast, brain, liver, stomach and lung. Deregulation of PI3K causes aberrant Akt activity. Therefore targeting this pathway could have implications for cancer treatment. The first generation PI3K-Akt inhibitors were proven to be highly effective with a low IC 50 , but later, they were shown to have toxic side effects and poor pharmacological properties and selectivity. Thus, these inhibitors were only effective in preclinical models. However, derivatives of these first generation inhibitors are much more selective and are quite effective in targeting the PI3K-Akt pathway, either alone or in combination. These second-generation inhibitors are essentially a specific chemical moiety that helps to form a strong hydrogen bond interaction with the PI3K/Akt molecule. The goal of this review is to delineate the current efforts that have been undertaken to inhibit the various components of the PI3K and Akt pathway in different types of cancer both in vitro and in vivo. Our focus here is on these novel therapies and their inhibitory effects that depend upon their chemical nature, as well as their development towards clinical trials.

show abstract

“…41,42 Buparlisib has potent, pan-class I PI3K inhibitory PROPERTIES against p110-α, -β, -δ, and -γ enzymes at IC 50 of 52, 166, 116, and 262 nM, respectively. 43 Other panclass I PI3K inhibitors in clinical development include XL147 (IC 50 of 39, 36, 23, and 383 nM against p110-α, -β, -δ, and -γ, respectively), GDC-0941 (pictilisib; IC 50 of 3 nM against p110-α and -δ enzymes), BAY80-6946 (copanlisib; IC 50 of 0.469 nM against p110-α and 3.72 nM against p110-β), PX-866 (sonolisib; IC 50 of 0.1-88 nM), and CH5132799 (IC 50 of 14 nM against p110-α). [44][45][46][47][48][49] …”

Section: Inhibitors Of the Pi3k/akt/mtor Signaling Pathwaymentioning

confidence: 99%

Pharmacodynamic Biomarker Development for PI3K Pathway Therapeutics

Josephs

Sarker

2015

Translational Oncogenomics

View full text Add to dashboard Cite

AbstrAct:The phosphatidylinositol 3-kinase (PI3K) signaling pathway is integral to many essential cell processes, including cell growth, differentiation, proliferation, motility, and metabolism. Somatic mutations and genetic amplifications that result in activation of the pathway are frequently detected in cancer. This has led to the development of rationally designed therapeutics targeting key members of the pathway. Critical to the successful development of these drugs are pharmacodynamic biomarkers that aim to define the degree of target and pathway inhibition. In this review, we discuss the pharmacodynamic biomarkers that have been utilized in early-phase clinical trials of PI3K pathway inhibitors. We focus on the challenges related to development and interpretation of these assays, their optimal integration with pharmacokinetic and predictive biomarkers, and future strategies to ensure successful development of PI3K pathway inhibitors within a personalized medicine paradigm for cancer.

show abstract

Identification of NVP-BKM120 as a Potent, Selective, Orally Bioavailable Class I PI3 Kinase Inhibitor for Treating Cancer

Cited by 217 publications

References 17 publications

Identification and Characterization of NVP-BKM120, an Orally Available Pan-Class I PI3-Kinase Inhibitor

Identification and Characterization of NVP-BKM120, an Orally Available Pan-Class I PI3-Kinase Inhibitor

PI3K and Akt as molecular targets for cancer therapy: current clinical outcomes

Pharmacodynamic Biomarker Development for PI3K Pathway Therapeutics

Contact Info

Product

Resources

About