Protein target highlights in CASP15: Analysis of models by structure providers.

Leila T Alexander,Xian Xia,Andrea Lia,Gira Bhabha,Felipe Opazo,Yusupha Bayo,Andriy Kryshtafovych,Maya Topf,Charlie J Hitchman,Manickam Gurusaran,Petri Kursula,Samuel Rommelaere,Maria Logotheti,Sigurbjörn Markússon,Andrew L Lovering,Kuan‐Lin Wu,Pietro Roversi,Dominic Gilzer,Cécile Breyton,Han Xiao,Mark A Wilson,Shiheng Liu,Séraphine Degroux,Rhys Grinter,Chris Greening,Jonathan M Grimes,Owen R Davies,Torsten Schwede,Benedikte S Erlandsen,Hartmut H Niemann,Mitchell D Miller,John Moult,Janani Durairaj,James Chen,Ashleigh Kropp,Luciano A Abriata,Peter L Freddolino,Krzysztof Fidelis,Simon G Caulton,Shaoyong Lu ,W C Zhang ,Bruno Lemaître ,K.j.f Satchell ,M.d Hartmann ,J.r Keown ,Mónica Rosas‐Lemus ,Nathan J Smith ,G Minasov ,G.n Phillips ,Zhou Zh ,D.c Ekiert

doi:10.1002/prot.26545

Abstract

We present an in-depth analysis of selected CASP15 targets, focusing on their biological and functional significance. The authors of the structures identify and discuss key protein features and evaluate how effectively these aspects were captured in the submitted predictions. While the overall ability to predict three-dimensional protein structures continues to impress, reproducing uncommon features not previously observed in experimental structures is still a challenge. Furthermore, instances with conformational flexibility and large multimeric complexes highlight the need for novel scoring strategies to better emphasize biologically relevant structural regions. Looking ahead, closer integration of computational and experimental techniques will play a key role in determining the next challenges to be unraveled in the field of structural molecular biology.

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