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DRUG:

MI-773

i
Other names: MI-773, SAR405838
Associations
Trials
Company:
Ascenta, Sanofi
Drug class:
MDM2 inhibitor, p53-MDM2-interaction inhibitor
Associations
Trials
9ms
Comparison of three-dimensional cell culture techniques of dedifferentiated liposarcoma and their integration with future research. (PubMed, Front Cell Dev Biol)
All samples were processed for histopathological analysis (HE, IHC and DNAscope™), Western blot, and qPCR; moreover, 3D collagen-based models were treated with different doses of SAR405838, a well-known inhibitor of MDM2, and cell viability was assessed in comparison to 2D model drug response...3D collagen samples showed higher cell viability after SAR40538 treatment than 2D models, while cells sensitive to the drug died by apoptosis or necrosis. Our results prompt us to extend our investigation by applying our 3D models to further oncological relevant applications, which may help address unresolved questions about dedifferentiated liposarcoma biology.
Preclinical • Journal
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MDM2 (E3 ubiquitin protein ligase)
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MI-773
over1year
Three dimensional models of dedifferentiated liposarcoma cell lines: scaffold-based and scaffold-free approaches. (PubMed, Hum Cell)
After treatment with MDM2 inhibitor SAR405838, DDLPS spheroids demonstrated different sensitivity patterns from 2D models. Taken together, we believed that 3D models would have a possibility to provide us a new predictability of efficacy and toxicity, and considered as one important process in in vitro pre-clinical phase prior to moving forward to clinical trials.
Preclinical • Journal
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MDM2 (E3 ubiquitin protein ligase)
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MDM2 amplification
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MI-773
2years
Targeting the MDM2-p53 pathway in dedifferentiated liposarcoma. (PubMed, Front Oncol)
Multiple agents have been developed, including Nutlins such as RG7112 and small molecular inhibitors including SAR405838 and HDM201. Mechanisms of resistance are being elucidated, and novel inhibitors and combination therapies are currently under investigation. This review provides an overview of these strategies for targeting MDM2 in DDLPS.
Review • Journal • Tumor Mutational Burden
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TMB (Tumor Mutational Burden) • MDM2 (E3 ubiquitin protein ligase)
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TMB-L • MDM2 amplification • MDM2 overexpression
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siremadlin (HDM201) • MI-773 • RG7112
3years
Pharmacogenomics characterization of the MDM2 inhibitor MI-773 reveals candidate tumours and predictive biomarkers. (PubMed, NPJ Precis Oncol)
A COMPARE analysis showed that the profile of MI-773 was similar to that of Nutlin-3a, the first potent inhibitor of p53-MDM2 interactions, and, in addition, had a superior potency. In silico biomarker investigations revealed that the TP53 mutation status plus the aggregated expression levels of 11 genes involved in the p53 signalling pathway predicted sensitivity or resistance of CLs to inhibitors of p53-MDM2 interactions reliably. The results obtained for MI-773 could help to refine the selection of cancer patients for therapy.
Journal
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MDM2 (E3 ubiquitin protein ligase)
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TP53 mutation
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Nutlin-3 • MI-773
3years
MI-773, a breaker of the MDM2/p53 axis, exhibits anticancer effects in neuroblastoma via downregulation of INSM1. (PubMed, Oncol Lett)
Meanwhile, knockdown of insulinoma-associated 1 decreased proliferation and increased apoptosis of NB cells. In conclusion, the present study demonstrated that MI-773 exhibited high selectivity and blockade affinity for the interaction between MDM2 and TP53 and may serve as a novel strategy for the treatment of NB.
Journal
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MDM2 (E3 ubiquitin protein ligase)
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MI-773
4years
[VIRTUAL] Integration of Deep Multi-Omics Profiling Veals New Insights into the Biology of Poor-Risk Acute Myeloid Leukemia (ASH 2020)
Collectively, t(6;9) primary samples also showed a selective drug sensitivity to XPO1 (selinexor and eltanexor) and JAK inhibitors (ruxolitinib, tofacitinib and momelotinib) compared to other cytogenetic risk groups. On the other hand, a comparison of in vitro drug sensitivity data with genomic data of our entire cohort of patients demonstrated that TP53 wt AMLs (n=37) were more sensitive to all four MDM2 inhibitors (AMG-232, idasanutlin, SAR405838 and NVP-CGM097) compared to TP53 mutated cases (n=13). Comparisons of transcriptomics with the in vitro sensitivity to drugs included in early/late phase AML clinical trials, identified signatures of response associated with MDM2 and Aurora B kinase (AZD1152-HQPA) inhibitors...Functionally, group A presented with elevated HOXA10 protein expression and enhanced in vitro response to genotoxic drugs and cell cycle inhibitors when compared to group B leukemia. Conclusions : Our study demonstrates the feasibility of simultaneously generating omics data from several different platforms and highlights that a combination of genetic and proteomic profiles may help to inform the choice of therapies based on the underlying biology of a patient’s AML.
IO biomarker
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TP53 (Tumor protein P53) • FLT3 (Fms-related tyrosine kinase 3) • KIT (KIT proto-oncogene, receptor tyrosine kinase) • CD34 (CD34 molecule) • NUP214 (Nucleoporin 214) • GATA2 (GATA Binding Protein 2) • FOXO3 (Forkhead box O3)
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TP53 mutation • FLT3-ITD mutation • MLL rearrangement
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Jakafi (ruxolitinib) • Xpovio (selinexor) • navtemadlin (KRT-232) • idasanutlin (RG7388) • eltanexor (KPT-8602) • CGM097 • barasertib-HQPA (AZD2811) • Ojjaara (momelotinib) • barasertib (AZD1152) • tofacitinib • MI-773
5years
BCR-ABL1 p190 in CML: A Minor Breakpoint with a Major Impact (ASH 2019)
CML patients with p190 had a median age of 72.5 years at the diagnosis (range: 50-80) and all received imatinib as a frontline treatment. Only one patient achieved a fluctuating major molecular response (MMR) by 12 months while the rest of the patients showed primary resistance to treatment and were shifted to a 2nd line TKI, nilotinib (n=2) or proceeded to HSCT (n=1)...DSRT results also revealed increased sensitivity of primary Ph+ ALL-p190 cells to Src-inhibitors (dasatinib and saracatinib), glucocorticoids and MDM2 inhibitors/TP53 activators (SAR405838 and idasanutlin)... In CML, p190 isoform of BCR-ABL1 is associated with distinct features and should be considered as a high-risk group. Combining clinical, genomic, phosphorylation and drug sensitivity data, we demonstrated that p190 activates specific cancer pathways, notably Src signaling and interferon pathways. Data also suggests that CML patients with p190 could benefit from broad spectrum TKI with Src inhibiting activity or combination of TKI with MDM2- or IAP-inhibitors.
IO biomarker
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TP53 (Tumor protein P53) • ABL1 (ABL proto-oncogene 1) • DNMT3A (DNA methyltransferase 1)
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dasatinib • imatinib • Tasigna (nilotinib) • idasanutlin (RG7388) • saracatinib (AZD0530) • MI-773