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Crystal structure of a covalently linked Aurora-A-MYCN complex.


ABSTRACT: Formation of the Aurora-A-MYCN complex increases levels of the oncogenic transcription factor MYCN in neuroblastoma cells by abrogating its degradation through the ubiquitin proteasome system. While some small-molecule inhibitors of Aurora-A were shown to destabilize MYCN, clinical trials have not been satisfactory to date. MYCN itself is considered to be `undruggable' due to its large intrinsically disordered regions. Targeting the Aurora-A-MYCN complex rather than Aurora-A or MYCN alone will open new possibilities for drug development and screening campaigns. To overcome the challenges that a ternary system composed of Aurora-A, MYCN and a small molecule entails, a covalently cross-linked construct of the Aurora-A-MYCN complex was designed, expressed and characterized, thus enabling screening and design campaigns to identify selective binders.

SUBMITTER: Diebold M 

PROVIDER: S-EPMC9815099 | biostudies-literature | 2023 Jan

REPOSITORIES: biostudies-literature

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Crystal structure of a covalently linked Aurora-A-MYCN complex.

Diebold Mathias M   Schönemann Lars L   Eilers Martin M   Sotriffer Christoph C   Schindelin Hermann H  

Acta crystallographica. Section D, Structural biology 20230101 Pt 1


Formation of the Aurora-A-MYCN complex increases levels of the oncogenic transcription factor MYCN in neuroblastoma cells by abrogating its degradation through the ubiquitin proteasome system. While some small-molecule inhibitors of Aurora-A were shown to destabilize MYCN, clinical trials have not been satisfactory to date. MYCN itself is considered to be `undruggable' due to its large intrinsically disordered regions. Targeting the Aurora-A-MYCN complex rather than Aurora-A or MYCN alone will o  ...[more]

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