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Home - Cell Biology - Unlocking the Dynamic Disorder of a Key Cancer Suppressor

Cell Biology

Unlocking the Dynamic Disorder of a Key Cancer Suppressor

Last updated: March 18, 2026 11:01 pm
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Unlocking the Dynamic Disorder of a Key Cancer Suppressor

A new study in Biophysical Journal provides a detailed structural analysis of the proline-rich domain (PRD) within the tumor suppressor protein p53. Using extensive all-atom molecular dynamics simulations validated by biophysical methods, researchers characterized this region as an intrinsically disordered domain. The PRD samples a highly heterogeneous conformational ensemble, with an average end-to-end distance of 52.5 Å and a radius of gyration of 21.8 Å. This intrinsic flexibility is central to the protein’s ability to modulate its molecular interactions and conformational dynamics, which are critical for its function in cell cycle regulation and the DNA damage response.

Study Significance: This research offers a crucial structural framework for understanding how mutations in p53’s disordered regions can disrupt its tumor-suppressive activity, a frequent event in oncogenesis. For cell biologists and cancer researchers, these findings refine models of protein folding and post-translational modifications that govern p53’s switch between active and inactive states. The computational and biophysical methodology also sets a benchmark for analyzing other intrinsically disordered proteins involved in key signaling pathways and phase separation.

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