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Last update 08 May 2025

Aurora A x N-Myc

Last update 08 May 2025

Basic Info

Related Targets

Aurora AN-Myc

Drugs associated with Aurora A x N-Myc

HLB-0532259

Target

Aurora A x N-Myc

Mechanism

Aurora A inhibitors [+1]

Active Org.

University of Minnesota

Originator Org.

University of Minnesota

Active Indication

Neuroblastoma

Inactive Indication-

Drug Highest PhasePreclinical

First Approval Ctry. / Loc.-

First Approval Date20 Jan 1800

100 Clinical Results associated with Aurora A x N-Myc

100 Translational Medicine associated with Aurora A x N-Myc

0 Patents (Medical) associated with Aurora A x N-Myc

Literatures (Medical) associated with Aurora A x N-Myc

01 Jun 2025·Bioorganic Chemistry

Identification of novel AURKA inhibitors against neuroblastoma using a virtual screening approach

Article

Author: Yin, Hongli ; Liu, Tianyi ; Dong, Xue

This study aims to screen and validate AURKA inhibitors to provide lead compounds and theoretical foundations for targeted therapy of neuroblastoma (NB). Through computer-aided drug screening, 11 compounds effectively binding to AURKA were selected from the YaTCM database, and their toxicity was predicted using admetSAR. Subsequently, molecular dynamics (MD) simulations were employed to evaluate the binding affinity and complex stability of the compounds with AURKA, leading to the identification of four preferred compounds (Erylatissin B, (+)-khellactone, Brazilin, and hematoxylin). Further steered molecular dynamics (SMD) and umbrella sampling (US) simulations were conducted to calculate the dissociation energy, confirming their binding strength with AURKA. In vitro experiments demonstrated that Brazilin significantly inhibited proliferation, migration, and induced apoptosis in SK-N-BE (2) cells, while also suppressing AURKA protein expression and its interaction with N-Myc. In vivo experiments showed that Brazilin markedly inhibited tumor growth in a mouse NB model. The findings indicate that Brazilin, by targeting AURKA, exhibits potential anti-NB activity, offering a new candidate compound and theoretical support for NB treatment.

24 Apr 2025·Biochemical Journal

Aurora A binds to the transactivation domain of c-Myc and recognizes the phosphorylated N-terminal degron motif

Article

Author: Levinson, Nicholas M. ; Thompson, Andrew R. ; Dunleavy, Katie M. ; Joshi, Nidhi ; Beel, Kaitlin M. ; John, Felix L. ; Engel, Tiffany A. ; Thomas, David D.

The oncoprotein c-Myc is overexpressed or mutated in a large fraction of human cancers. The stability of c-Myc is controlled by phosphorylation of T58 and S62 within a conserved degron motif in the N-terminal transactivation domain (TAD), which triggers recruitment of the SCF ubiquitin ligase. The kinase Aurora A (AurA) has been shown to bind to both c-Myc and its paralog N-Myc and to promote their stability by interfering with ubiquitination and degradation. Here we show, using NMR and Förster resonance energy transfer experiments, that AurA binds to c-Myc through several discrete interactions spanning 145 residues within its TAD. AurA binding to c-Myc is enhanced by phosphorylation of the T58/S62 degron, demonstrating that the kinase recognizes the pool of c-Myc that has been marked for degradation by the ubiquitin proteasome pathway. Although AurA binds to segments of c-Myc flanking the degron, it does not appear to form extensive interactions with the phosphorylated degron itself, potentially leaving it accessible on the AurA surface. These observations establish a foundation for understanding the role of AurA in regulating c-Myc ubiquitination and degradation.

07 Feb 2025·Investigative Ophthalmology & Visual Science

Aurora A Kinase Inhibition Is Synthetic Lethal With the Activation of MYCN in Retinoblastoma

Article

Author: Fan, Xianqun ; Fan, Jiayan ; Shi, Hanhan ; Wen, Xuyang ; Jia, Renbing ; Liao, Qili ; Yang, Jie ; Li, Yongyun ; Chai, Peiwei ; Mengjiang, Reyizha ; Ge, Shengfang ; Zhang, Qianqian

PurposeRB1 inactivation and MYCN activation have been documented as common oncogenic alterations in retinoblastoma (RB). Direct targeting of RB1 and MYCN has not yet been proven to be feasible. The current treatment options for RB mainly consist of conventional chemotherapy, which inevitably poses health-threatening side effects. Here, we aimed to screen an in-house compound library to identify potential drugs for the treatment of human RB.MethodsAurora A kinase (AURKA) inhibitors were identified by differential viability screening with a tool compound library, and the pharmacological safety and efficacy of candidate drugs were further validated in zebrafish and RB patient-derived xenograft (PDX) models in vivo. Further CUT & Tag assay, ChIP-qPCR and RNA seq performances showed that MYCN binds to the AURKA promoter and upregulates its transcription, suggesting that AURKA inhibition induces synthetic lethality in RB.ResultsIn this study, we revealed that AURKA inhibitors exhibited high therapeutic efficacy against RB both in vitro and in vivo. Mechanistically, we found that MYCN could bind to the AURKA promoter region to regulate its transcription, thereby promoting AURKA expression and consequently driving RB progression. Interestingly, AURKA inhibition exhibited synthetic lethality with RB1-deficient and MYCN-amplification in RB cells.ConclusionsCollectively, these findings demonstrate that AURKA is crucial for RB progression and further expanded the current understanding of synthetic lethal therapeutic strategies. Our study indicates that AURKA inhibitors may represent a new therapeutic strategy for selectively targeting patients with RB with RB1-deficient and MYCN-amplification to improve the prognosis of aggressive types of patients with RB.

News (Medical) associated with Aurora A x N-Myc

09 Apr 2024

·www.sciencedaily.com

Research could unlock more precise prognoses and targeted treatments for children with cancer

Researchers have identified new variations in neuroblastoma that could lead to a more accurate prognosis and better-targeted treatments for this devastating childhood cancer. A study reveals three new subgroups of the most common type of neuroblastoma, each with different genetic traits, expected outcomes, and distinguishing features that offer clues as to which treatments may be most effective. Researchers have identified new variations in neuroblastoma that could lead to a more accurate prognosis and better-targeted treatments for this devastating childhood cancer. A study published in the British Journal of Cancer reveals three new subgroups of the most common type of neuroblastoma, each with different genetic traits, expected outcomes, and distinguishing features that offer clues as to which treatments may be most effective. Dr Yihua Wang from the University of Southampton, a senior author on the paper said: "This research represents a pivotal advancement in our understanding of MYCN non-amplified neuroblastomas. The results are striking. These kinds of neuroblastomas can be classified into three distinct subgroups, each demonstrating unique prognostic implications and varying vulnerabilities to investigational therapies." Around 100 children are diagnosed with neuroblastoma each year in the UK, representing six to ten per cent of all childhood cancers. Neuroblastoma is a cancer that starts in a type of nerve cell called a neuroblast. It can present in the abdomen, chest neck or pelvis and can spread to other parts of the body. The overall prognosis of the disease is poor, with just 20 per cent of patients still alive at 5 years after diagnosis, but the likelihood of the cancer being cured varies widely, with some tumours spontaneously regressing and others proving resistant to therapy and progressing. One of the key indicators of risk is the amplification of a gene called MYCN, where tumours have too many of this type of gene. This occurs in around 20 per cent of cases and accounts for about 40 per cent of high-risk neuroblastomas. Researchers from the University of Southampton and China wanted to find out more about cases where the MYCN gene isn't amplified to better understand the diversity of outcomes within these cases. Using advanced analytical techniques, the research team analysed over 1,500 biopsy samples from 16 different datasets sourced from Gene Expression Omnibus (GEO) and ArrayExpress. The team were able to identify three distinct subtypes of these MYCN non-amplified cases based on their transcriptional signatures -- patterns of gene expression that can provide valuable insights into biological processes. The first subgroup makes up around half of MYCN non-amplified cases and has the best prognosis, with a long-term survival rate of over 85 per cent, despite some cases being clinically classified as high risk. Subgroup 2, representing a quarter of MYCN non-amplified cases, had the worst outcomes with a long-term survival rate of 50%. Interestingly, this group had a similar genetic signature to cases where MYCN is amplified. Researchers found a protein called Aurora Kinase A (AURKA) was expressed at significantly higher levels than in the other two subgroups. On further analysis, they found that AURKA mRNA levels alone could predict overall survival. This suggests that patients within the subgroup may benefit from treatment with AURKA inhibitors. Meanwhile, Subgroup 3, which made up another quarter of MYCN non-amplified cases, is characterised by an 'inflamed' gene signature, with significantly higher levels of activity in immune cells. Further analysis indicates that patients in this subgroup were predicted to respond better to immunotherapy. Dr Wang added: "This research opens new avenues for personalised medicine in the treatment of neuroblastomas. By leveraging transcriptional subtyping, we are now equipped to offer more precise prognosis and tailor therapies accordingly for patients with MYCN non-amplified neuroblastomas, potentially improving outcomes and quality of life." The project was supported by the UK Medical Research Council and the Natural Science Foundation of China.

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