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1H, 13C and 15N backbone and side-chain resonance assignments of the human oncogenic protein NCYM

by Kono, Fumiaki , Nakatani, Kazuma , Peters, Judith , Barthe, Philippe , Mouhand, Assia , Suenaga, Yusuke , Roumestand, Christian , Tamada, Taro , Hippo, Yoshitaka , Matsuo, Tatsuhito

in Animal models / Antineoplastic drugs / Apoptosis / Biochemistry / Biological and Medical Physics / Biophysics / Chromatography / Circular dichroism / Experiments / Genes / Glycerol / Life Sciences / Metastases / Metastasis / Neuroblastoma / NMR / Nuclear magnetic resonance / Phosphorylation / Physics / Physics and Astronomy / Polymer Sciences / Protein structure / Proteins / Secondary structure / Tumors / X-ray scattering

2024

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1H, 13C and 15N backbone and side-chain resonance assignments of the human oncogenic protein NCYM

by Kono, Fumiaki , Nakatani, Kazuma , Peters, Judith , Barthe, Philippe , Mouhand, Assia , Suenaga, Yusuke , Roumestand, Christian , Tamada, Taro , Hippo, Yoshitaka , Matsuo, Tatsuhito

2024

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1H, 13C and 15N backbone and side-chain resonance assignments of the human oncogenic protein NCYM

by Kono, Fumiaki , Nakatani, Kazuma , Peters, Judith , Barthe, Philippe , Mouhand, Assia , Suenaga, Yusuke , Roumestand, Christian , Tamada, Taro , Hippo, Yoshitaka , Matsuo, Tatsuhito

2024

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Journal Article

1H, 13C and 15N backbone and side-chain resonance assignments of the human oncogenic protein NCYM

Kono, Fumiaki,

Nakatani, Kazuma,

Peters, Judith,

Barthe, Philippe,

Mouhand, Assia,

Suenaga, Yusuke,

Roumestand, Christian,

Tamada, Taro,

Hippo, Yoshitaka,

Matsuo, Tatsuhito

2024

Overview

NCYM is a cis-antisense gene of MYCN oncogene and encodes an oncogenic protein that stabilizes MYCN via inhibition of GSK3b. High NCYM expression levels are associated with poor clinical outcomes in human neuroblastomas, and NCYM overexpression promotes distant metastasis in animal models of neuroblastoma. Using vacuum-ultraviolet circular dichroism and small-angle X-ray scattering, we previously showed that NCYM has high flexibility with partially folded structures; however, further structural characterization is required for the design of anti-cancer agents targeting NCYM. Here we report the 1 H, 15 N and 13 C nuclear magnetic resonance assignments of NCYM. Secondary structure prediction using Secondary Chemical Shifts and TALOS-N analysis demonstrates that the structure of NCYM is essentially disordered, even though residues in the central region of the peptide clearly present a propensity to adopt a dynamic helical structure. This preliminary study provides foundations for further analysis of interaction between NCYM and potential partners.

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Publisher

Springer Netherlands,Springer Nature B.V,Springer

Subject

Animal models

/ Antineoplastic drugs

/ Apoptosis

/ Biochemistry

/ Biological and Medical Physics

/ Biophysics

/ Chromatography