Co-targeting PIM and PI3K/mTOR using multikinase inhibitor AUM302 and a combination of AZD-1208 and BEZ235 in prostate cancer

Luszczak, Sabina; Simpson, Benjamin S.; Stopka‐Farooqui, Urszula; Sathyadevan, Vignesh Krishna; Echeverría, Lina María Carmona; Kumar, Christopher; Costa, Helena; Haider, Aiman; Freeman, Alex; Jameson, Charles; Ratynska, Marzena; Ben-Salha, Imen; Sridhar, Ashwin; Shaw, Greg; Kelly, John D.; Pye, Hayley; Gately, Kathy; Whitaker, Hayley C.; Heavey, Susan

doi:10.1038/s41598-020-71263-9

Cited by 9 publications

(6 citation statements)

References 40 publications

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“…Cen et al showed that inhibition of Akt led to transcriptional induction of PIM1 kinase which in turn regulated the expression of RTKs in prostate cancer [5]. We have shown that a co-targeted approach is more effective compared to single PIM kinase or PI3K-mTOR inhibition, as previously reported in prostate cancer [10].…”

Section: Introductionsupporting

confidence: 81%

Co-Targeting PIM Kinase and PI3K/mTOR in NSCLC

Moore

Lightner

Elbai

et al. 2021

Cancers

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PIM kinases are constitutively active proto-oncogenic serine/threonine kinases that play a role in cell cycle progression, metabolism, inflammation and drug resistance. PIM kinases interact with and stabilize p53, c-Myc and parallel signaling pathway PI3K/Akt. This study evaluated PIM kinase expression in NSCLC and in response to PI3K/mTOR inhibition. It investigated a novel preclinical PI3K/mTOR/PIM inhibitor (IBL-301) in vitro and in patient-derived NSCLC tumor tissues. Western blot analysis confirmed PIM1, PIM2 and PIM3 are expressed in NSCLC cell lines and PIM1 is a marker of poor prognosis in patients with NSCLC. IBL-301 decreased PIM1, c-Myc, pBAD and p4EBP1 (Thr37/46) and peIF4B (S406) protein levels in-vitro and MAP kinase, PI3K-Akt and JAK/STAT pathways in tumor tissue explants. IBL-301 significantly decreased secreted pro-inflammatory cytokine MCP-1. Altered mRNA expression, including activated PIM kinase and c-Myc, was identified in Apitolisib resistant cells (H1975GR) by an IL-6/STAT3 pathway array and validated by Western blot. H1975GR cells were more sensitive to IBL-301 than parent cells. A miRNA array identified a dysregulated miRNA signature of PI3K/mTOR drug resistance consisting of regulators of PIM kinase and c-Myc (miR17-5p, miR19b-3p, miR20a-5p, miR15b-5p, miR203a, miR-206). Our data provides a rationale for co-targeting PIM kinase and PI3K-mTOR to improve therapeutic response in NSCLC.

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Section: Introductionsupporting

confidence: 81%

Co-Targeting PIM Kinase and PI3K/mTOR in NSCLC

Moore

Lightner

Elbai

et al. 2021

Cancers

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“…BEZ235 inhibits multiple class I PI3K isoforms and mTORC1/2 kinase activity, exerts potent anticancer activity, and attenuates PI3K reactivation and mTORC2-mediated AKT reactivation (Chiarini et al, 2015). It has exhibited antitumor effects in various cancers, including pancreatic cancer, and its synergistic effects have been revealed in combination with numerous drugs, including cytotoxic drugs and target inhibitors https://doi.org/10.4062/biomolther.2021.145 (Murakami et al, 1987;Zhu et al, 2015;Chen et al, 2018;Luszczak et al, 2020;Ruan et al, 2020). However, PI3K inhibitors, including BEZ-235, have been reported to enhance MEK/ERK pathway activation through a negative feedback loop mediated by mTORC2 in pancreatic cancer cells, leading to drug resistance (Soares et al, 2015).…”

Section: Discussionmentioning

confidence: 99%

Combination Therapy of the Active KRAS-Targeting Antibody inRas37 and a PI3K Inhibitor in Pancreatic Cancer

Lee

Woo

Jung

et al. 2022

Biomol Ther (Seoul)

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KRAS activating mutations, which are present in more than 90% of pancreatic cancers, drive tumor dependency on the RAS/ mitogen-activated protein kinase (MAPK) and phosphoinositide 3-kinase (PI3K)/AKT signaling pathways. Therefore, combined targeting of RAS/MAPK and PI3K/AKT signaling pathways may be required for optimal therapeutic effect in pancreatic cancer. However, the therapeutic efficacy of combined MAPK and PI3K/AKT signaling target inhibitors is unsatisfactory in pancreatic cancer treatment, because it is often accompanied by MAPK pathway reactivation by PI3K/AKT inhibitor. Therefore, we developed an inRas37 antibody, which directly targets the intra-cellularly activated GTP-bound form of oncogenic RAS mutation and investigated its synergistic effect in the presence of the PI3K inhibitor BEZ-235 in pancreatic cancer. In this study, inRas37 remarkably increased the drug response of BEZ-235 to pancreatic cancer cells by inhibiting MAPK reactivation. Moreover, the co-treatment synergistically inhibited cell proliferation, migration, and invasion and exhibited synergistic anticancer activity by inhibiting the MAPK and PI3K pathways. The combined administration of inRas37and BEZ-235 significantly inhibited tumor growth in mouse models. Our results demonstrated that inRas37 synergistically increased the antitumor activity of BEZ-235 by inhibiting MAPK reactivation, suggesting that inRas37 and BEZ-235 co-treatment could be a potential treatment approach for pancreatic cancer patients with KRAS mutations.

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“…The combination of the PIM inhibitor AZD1208 and the PI3K/mTOR inhibitor BEZ235 (dactolisib) has been investigated in clinical trials. 399 A novel and highly efficient triple PIM/PI3K/mTOR inhibitor AUM302 elicited a superior functional outcome compared to the effects of the combination of AZD1208 and BEZ235; these results may help reduce treatment toxicity in future trials. 399 Overall, the clinical application of PI3K/AKT/mTOR inhibitors is still limited in PCa, and further studies that can identify new biomarkers for patient selection or improve co-targeting strategies are still required to enhance their therapeutic effects.…”

Section: Targeting the Pi3k/akt/mtor Signaling Axismentioning

confidence: 98%

Targeting signaling pathways in prostate cancer: mechanisms and clinical trials

Xiao

et al. 2022

Sig Transduct Target Ther

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Prostate cancer (PCa) affects millions of men globally. Due to advances in understanding genomic landscapes and biological functions, the treatment of PCa continues to improve. Recently, various new classes of agents, which include next-generation androgen receptor (AR) signaling inhibitors (abiraterone, enzalutamide, apalutamide, and darolutamide), bone-targeting agents (radium-223 chloride, zoledronic acid), and poly(ADP-ribose) polymerase (PARP) inhibitors (olaparib, rucaparib, and talazoparib) have been developed to treat PCa. Agents targeting other signaling pathways, including cyclin-dependent kinase (CDK)4/6, Ak strain transforming (AKT), wingless-type protein (WNT), and epigenetic marks, have successively entered clinical trials. Furthermore, prostate-specific membrane antigen (PSMA) targeting agents such as 177Lu-PSMA-617 are promising theranostics that could improve both diagnostic accuracy and therapeutic efficacy. Advanced clinical studies with immune checkpoint inhibitors (ICIs) have shown limited benefits in PCa, whereas subgroups of PCa with mismatch repair (MMR) or CDK12 inactivation may benefit from ICIs treatment. In this review, we summarized the targeted agents of PCa in clinical trials and their underlying mechanisms, and further discussed their limitations and future directions.

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Co-targeting PIM and PI3K/mTOR using multikinase inhibitor AUM302 and a combination of AZD-1208 and BEZ235 in prostate cancer

Cited by 9 publications

References 40 publications

Co-Targeting PIM Kinase and PI3K/mTOR in NSCLC

Co-Targeting PIM Kinase and PI3K/mTOR in NSCLC

Combination Therapy of the Active KRAS-Targeting Antibody inRas37 and a PI3K Inhibitor in Pancreatic Cancer

Targeting signaling pathways in prostate cancer: mechanisms and clinical trials

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