Development of an MDM2 Degrader for Treatment of Acute Leukemias

Marcellino, Bridget; Yang, Xiaobao; Chen, He; Chen, Karie; Brady, Claudia; Clementelli, Cara; Li, Zhijun; Hoffman, Ronald; Liu, Jing; Kanıskan, H. Ümit; Xiong, Yujie; Jin, Jian; Shih, Alan H.

doi:10.1182/blood-2021-147522

Cited by 3 publications

(2 citation statements)

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“…9 ). The three co-opted E3 ligases, VHL , XIAP , and AHR , have been explored against cancer targets in PROTAC 12 , 22 , 44 – 46 , and their expression patterns in tumor and normal tissues suggest extensive future usage, such as XIAP in breast cancer (Fig. 4c , Supplementary Fig.…”

Section: Resultsmentioning

confidence: 99%

Expanding PROTACtable genome universe of E3 ligases

Liu,

Yang,

Wang

et al. 2023

Nat Commun

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Proteolysis-targeting chimera (PROTAC) and other targeted protein degradation (TPD) molecules that induce degradation by the ubiquitin-proteasome system (UPS) offer new opportunities to engage targets that remain challenging to be inhibited by conventional small molecules. One fundamental element in the degradation process is the E3 ligase. However, less than 2% amongst hundreds of E3 ligases in the human genome have been engaged in current studies in the TPD field, calling for the recruiting of additional ones to further enhance the therapeutic potential of TPD. To accelerate the development of PROTACs utilizing under-explored E3 ligases, we systematically characterize E3 ligases from seven different aspects, including chemical ligandability, expression patterns, protein-protein interactions (PPI), structure availability, functional essentiality, cellular location, and PPI interface by analyzing 30 large-scale data sets. Our analysis uncovers several E3 ligases as promising extant PROTACs. In total, combining confidence score, ligandability, expression pattern, and PPI, we identified 76 E3 ligases as PROTAC-interacting candidates. We develop a user-friendly and flexible web portal (https://hanlaboratory.com/E3Atlas/) aimed at assisting researchers to rapidly identify E3 ligases with promising TPD activities against specifically desired targets, facilitating the development of these therapies in cancer and beyond.

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Section: Resultsmentioning

confidence: 99%

Expanding PROTACtable genome universe of E3 ligases

Liu,

Yang,

Wang

et al. 2023

Nat Commun

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“…Two other PROTAC–MDM2 degrader molecules have been reported, but their structures have not been disclosed. Marcellino et al reported the development of the PROTAC–MDM2 degrader XY-27 using an undisclosed MDM2 inhibitor tethered to a ligand of the VHL E3 ubiquitin ligase [ 86 ]. VHL was selected due to its higher expression in acute myelogenous leukemia (AML) compared to other cancers, and its use can potentially improve the potency and specificity in AML.…”

Section: Targeting the Protein–protein Interaction Between Mdm2 And P53mentioning

confidence: 99%

Therapeutic Strategies to Activate p53

Aguilar

Wang

2022

Pharmaceuticals

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The p53 protein has appropriately been named the “guardian of the genome”. In almost all human cancers, the powerful tumor suppressor function of p53 is compromised by a variety of mechanisms, including mutations with either loss of function or gain of function and inhibition by its negative regulators MDM2 and/or MDMX. We review herein the progress made on different therapeutic strategies for targeting p53.

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