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Mutations in the PKM2 exon-10 region are associated with reduced allostery and increased nuclear translocation.


ABSTRACT: PKM2 is a key metabolic enzyme central to glucose metabolism and energy expenditure. Multiple stimuli regulate PKM2's activity through allosteric modulation and post-translational modifications. Furthermore, PKM2 can partner with KDM8, an oncogenic demethylase and enter the nucleus to serve as a HIF1α co-activator. Yet, the mechanistic basis of the exon-10 region in allosteric regulation and nuclear translocation remains unclear. Here, we determined the crystal structures and kinetic coupling constants of exon-10 tumor-related mutants (H391Y and R399E), showing altered structural plasticity and reduced allostery. Immunoprecipitation analysis revealed increased interaction with KDM8 for H391Y, R399E, and G415R. We also found a higher degree of HIF1α-mediated transactivation activity, particularly in the presence of KDM8. Furthermore, overexpression of PKM2 mutants significantly elevated cell growth and migration. Together, PKM2 exon-10 mutations lead to structure-allostery alterations and increased nuclear functions mediated by KDM8 in breast cancer cells. Targeting the PKM2-KDM8 complex may provide a potential therapeutic intervention.

SUBMITTER: Chen TJ 

PROVIDER: S-EPMC6420622 | biostudies-literature | 2019

REPOSITORIES: biostudies-literature

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Mutations in the PKM2 exon-10 region are associated with reduced allostery and increased nuclear translocation.

Chen Tsan-Jan TJ   Wang Hung-Jung HJ   Liu Jai-Shin JS   Cheng Hsin-Hung HH   Hsu Sheng-Chieh SC   Wu Meng-Chen MC   Lu Chien-Hung CH   Wu Yu-Fang YF   Wu Jing-Wen JW   Liu Ying-Yuan YY   Kung Hsing-Jien HJ   Wang Wen-Ching WC  

Communications biology 20190315


PKM2 is a key metabolic enzyme central to glucose metabolism and energy expenditure. Multiple stimuli regulate PKM2's activity through allosteric modulation and post-translational modifications. Furthermore, PKM2 can partner with KDM8, an oncogenic demethylase and enter the nucleus to serve as a HIF1α co-activator. Yet, the mechanistic basis of the exon-10 region in allosteric regulation and nuclear translocation remains unclear. Here, we determined the crystal structures and kinetic coupling co  ...[more]

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