^
Contact us  to learn more about
our Premium Content:  News alerts, weekly reports and conference planners
DRUG:

ZM 447439

i
Other names: ZM 447439
Associations
Trials
Company:
Bio-Techne
Drug class:
Aurora kinase A inhibitor, Aurora kinase B inhibitor
Associations
Trials
1m
Construction of a novel lipid drop-mitochondria-associated genetic profile for predicting the survival and prognosis of lung adenocarcinoma. (PubMed, Discov Oncol)
Our results suggest that the LD-M risk score is an effective prognostic indicator for individualized treatment of LUAD.
Journal • IO biomarker
|
CAV2 (Caveolin 2)
|
BMS-754807 • ZM 447439
9ms
The cell death-related genes machine learning model for precise therapy and clinical drug selection in hepatocellular carcinoma. (PubMed, J Cell Mol Med)
Moreover, our investigation has shown that AZD2014, SB505124, LJI308 and OSI-207 show a greater efficacy in patients in the low-risk category. Conversely, for the high-risk group patients, PD173074, ZM447439 and CZC24832 exhibit a stronger response...This innovative model provides a novel approach for forecasting prognosis and assessing drug sensitivity in HCC patients, driving a more personalized and efficacious treatment paradigm, elevating clinical outcomes. Nonetheless, additional research endeavours are required to confirm the model's precision and assess its potential to inform clinical decision-making for HCC patients.
Journal • Tumor mutational burden • Machine learning
|
TMB (Tumor Mutational Burden)
|
TMB-L
|
vistusertib (AZD2014) • CZC24832 • ZM 447439
over1year
V-Src delocalizes Aurora B by suppressing Aurora B kinase activity during monopolar cytokinesis. (PubMed, Cell Signal)
Furthermore, like v-Src, treatment with the Aurora B inhibitor ZM447439 also caused Aurora B delocalization at concentrations that partially inhibited Aurora B autophosphorylation. Given that phosphorylation of Aurora B by v-Src was not observed, these results suggest that v-Src causes Aurora B delocalization by indirectly suppressing Aurora B kinase activity.
Journal
|
SRC (SRC Proto-Oncogene) • CDK1 (Cyclin-dependent kinase 1) • CSK (C-Terminal Src Kinase)
|
ZM 447439
over2years
Identifying the role of transient receptor potential channels (TRPs) in kidney renal clear cell carcinoma and their potential therapeutic significances using genomic and transcriptome analyses. (PubMed, BMC Med Genomics)
Besides, high-risk KIRC patients might benefit from ABT888, AZD6244, AZD7762, Bosutinib, Camptothecin, CI1040, JNK inhibitor VIII, KU55933, Lenalidomide, Nilotinib, PLX4720, RO3306, Vinblastine, and ZM.447439; however, low-risk populations might benefit from Bicalutamide, FH535, and OSI906. Finally, calibration curves were used to validate the nomogram with a satisfactory predictive survival probability. In conclusion, this research provides useful insight that can aid and guide clinical practice and scientific research.
Journal • Tumor Mutational Burden • PARP Biomarker
|
TMB (Tumor Mutational Burden)
|
lenalidomide • Koselugo (selumetinib) • Tasigna (nilotinib) • PLX4720 • Bosulif (bosutinib) • veliparib (ABT-888) • CI-1040 • bicalutamide • linsitinib (ASP7487) • vinblastine • KU-55933 • AZD-7762 • ZM 447439
3years
Biological and Clinical Significance of PIM1 Genetic Alterations in Diffuse Large B-Cell Lymphoma (ASH 2021)
We further found that compared to patients with low-risk score, patients with high-risk score had higher sensitivity to some drugs of targeting the immune microenvironment, including TGFβ receptor inhibitors SB525334 ( P <0.0001) and SB505124 ( P <0.0001) and immunomodulator Lenalidomide ( P =0.041), as well as NF-κB inhibitors Parthenolide ( P <0.0001) and TPCA-1 ( P <0.0001) and JAK inhibitors Ruxolitinib ( P =0.014) and TG101348 ( P =0.0053), accompanying with significantly lower IC50 values. In addition, another common chemotherapeutic drug Gemcitabine was also predicted to be more sensitive for patients with high-risk score ( P =0.047). Other targeted drugs such as Aurora kinase inhibitors VX-680 ( P <0.0001) and ZM-447439 ( P =0.014), Bcl-2 inhibitors Obatoclax Mesylate ( P =0.00036) and Navitoclax ( P <0.0001), and CDK inhibitors Roscovitine ( P =0.0012), AT-7519 ( P =0.0033), PHA-793887 ( P <0.0001) and THZ2-49 ( P =0.0053) also exhibited higher drug sensitivity for patients with high-risk score. Conclusions : PIM1 mutations play a vital role in patient risk stratification and provide novel insights into therapeutic decision making for DLBCL patients with high-risk score.
Clinical • IO biomarker
|
MYD88 (MYD88 Innate Immune Signal Transduction Adaptor) • CD79B (CD79b Molecule) • PIM1 (Pim-1 Proto-Oncogene) • TGFB1 (Transforming Growth Factor Beta 1) • IL17A (Interleukin 17A) • PRDM1 (PR/SET Domain 1)
|
MYD88 mutation • CD79B mutation • PIM1 mutation • SPEN mutation
|
gemcitabine • lenalidomide • Jakafi (ruxolitinib) • navitoclax (ABT 263) • Inrebic (fedratinib) • PHA 793887 • AT7519 • ZM 447439 • obatoclax (GX 15-070) • seliciclib (CYC202) • tozasertib (MK-0457)
over3years
Inhibition of Cdc20 suppresses the metastasis in triple negative breast cancer (TNBC). (PubMed, Breast Cancer)
These results suggest an essential role of Cdc20 in tumor formation and metastasis of TNBC, which might be a potential target therapy for TNBC treatment.
Journal
|
CDC20 (Cell Division Cycle 20)
|
BI2536 • ZM 447439 • tozasertib (MK-0457)