Computational inference of eIF4F complex function and structure in human cancers
成果类型:
Article
署名作者:
Wu, Su; Wagner, Gerhard
署名单位:
Harvard University; Harvard Medical School
刊物名称:
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
ISSN/ISSBN:
0027-14958
DOI:
10.1073/pnas.2313589121
发表日期:
2024-01-30
关键词:
eukaryotic translation initiation
factor 4g eif4g
ribosomal entry site
messenger-rna
binding
mechanism
principles
patterns
protein
switch
摘要:
The canonical eukaryotic initiation factor 4F (eIF4F) complex, composed of eIF4G1, eIF4A1, and the cap- binding protein eIF4E, plays a crucial role in cap- dependent translation initiation in eukaryotic cells. An alternative cap- independent initiation can occur, involving only eIF4G1 and eIF4A1 through internal ribosome entry sites (IRESs). This mechanism is considered complementary to cap- dependent initiation, particularly in tumors under stress conditions. However, the selection and molecular mechanism of specific translation initiation remains poorly understood in human cancers. Thus, we analyzed gene copy number variations (CNVs) in TCGA tumor samples and found frequent amplification of genes involved in translation initiation. Copy number gains in EIF4G1 and EIF3E frequently co - occur across human cancers. Additionally, EIF4G1 expression strongly correlates with genes from cancer cell survival pathways including cell cycle and lipogenesis, in tumors with EIF4G1 amplification or duplication. Furthermore, we revealed that eIF4G1 and eIF4A1 protein levels strongly co- regulate with ribosomal subunits, eIF2, and eIF3 complexes, while eIF4E co- regulates with 4E-BP1, ubiquitination, and ESCRT proteins. Utilizing Alphafold predictions, we modeled the eIF4F structure with and without eIF4E binding. For cap- dependent initiation, our modeling reveals extensive interactions between the N- terminal eIF4E- binding domain of eIF4G1 and eIF4E. Furthermore, the eIF4G1 HEAT - 2 domain positions eIF4E near the eIF4A1 N- terminal domain (NTD), resulting in the collaborative enclosure of the RNA binding cavity within eIF4A1. In contrast, during cap- independent initiation, the HEAT - 2 domain directly binds the eIF4A1-NTD, leading to a stronger interaction between eIF4G1 and eIF4A1, thus closing the mRNA binding cavity without the involvement of eIF4E.