RRC ID 81932
Author Suzuki Y, Tsubota S, Kadomatsu K, Sakamoto K.
Title Identification of APBB1 as a substrate for anaplastic lymphoma kinase.
Journal J Biochem
Abstract Anaplastic lymphoma kinase (ALK) is a well-known oncogene involved in various malignancies such as anaplastic large cell lymphoma, lung cancer and neuroblastoma. Several substrates for fused ALK have been identified and their biological functions have been described. However, the lack of a comprehensive identification of ALK substrates limits our understanding of the biological roles of receptor ALK. Thus, this study aimed to identify novel ALK substrates and characterize their biological functions. We screened the interactors of the kinase domain of receptor ALK using proximity-dependent biotin identification and identified 43 interactors. We narrowed down the candidates by evaluating whether these interactors were downstream of ALK in a neuroblastoma cell line, NB-1. Amongst these, we identified amyloid beta precursor protein-binding family B member 1 (APBB1) as an ALK downstream molecule involved in NB-1 cell viability. Finally, we assessed the kinase-substrate relationship between ALK and APBB1 and found that ALK phosphorylated multiple tyrosine residues in APBB1 both in-cell and in-tube assays, with tyrosine 269 as a major target. In conclusion, we successfully identified a new substrate for receptor ALK. Our results may help further elucidate the molecular mechanism of ALK downstream signalling in neuroblastoma.
Volume 176(5)
Pages 395-403
Published 2024-11-4
DOI 10.1093/jb/mvae055
PII 7729936
PMID 39115278
MeSH Anaplastic Lymphoma Kinase* / genetics Anaplastic Lymphoma Kinase* / metabolism Cell Line, Tumor Cytokines Humans Neuroblastoma / enzymology Neuroblastoma / metabolism Neuroblastoma / pathology Phosphorylation Receptor Protein-Tyrosine Kinases / genetics Receptor Protein-Tyrosine Kinases / metabolism Substrate Specificity
Resource
DNA material CSII-CMV-MCS-IRES2-Venus (RDB04383)