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Arginine Methylation of hnRNPK Inhibits the DDX3-hnRNPK Interaction to Play an Anti-Apoptosis Role in Osteosarcoma Cells
by
Chen, Chiao-Che
, Lin, Wey-Jinq
, Lin, Chao-Hsiung
, Fu, Shu-Ling
, Yang, Jen-Hao
in
Antibodies
/ Apoptosis
/ Bone cancer
/ Cell cycle
/ DNA damage
/ DNA methylation
/ E coli
/ Glycerol
/ Kinases
/ Phosphorylation
/ Plasmids
/ Proteins
/ Sarcoma
2021
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Arginine Methylation of hnRNPK Inhibits the DDX3-hnRNPK Interaction to Play an Anti-Apoptosis Role in Osteosarcoma Cells
by
Chen, Chiao-Che
, Lin, Wey-Jinq
, Lin, Chao-Hsiung
, Fu, Shu-Ling
, Yang, Jen-Hao
in
Antibodies
/ Apoptosis
/ Bone cancer
/ Cell cycle
/ DNA damage
/ DNA methylation
/ E coli
/ Glycerol
/ Kinases
/ Phosphorylation
/ Plasmids
/ Proteins
/ Sarcoma
2021
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While trying to remove the title from your shelf something went wrong :( Kindly try again later!
Do you wish to request the book?
Arginine Methylation of hnRNPK Inhibits the DDX3-hnRNPK Interaction to Play an Anti-Apoptosis Role in Osteosarcoma Cells
by
Chen, Chiao-Che
, Lin, Wey-Jinq
, Lin, Chao-Hsiung
, Fu, Shu-Ling
, Yang, Jen-Hao
in
Antibodies
/ Apoptosis
/ Bone cancer
/ Cell cycle
/ DNA damage
/ DNA methylation
/ E coli
/ Glycerol
/ Kinases
/ Phosphorylation
/ Plasmids
/ Proteins
/ Sarcoma
2021
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Arginine Methylation of hnRNPK Inhibits the DDX3-hnRNPK Interaction to Play an Anti-Apoptosis Role in Osteosarcoma Cells
Journal Article
Arginine Methylation of hnRNPK Inhibits the DDX3-hnRNPK Interaction to Play an Anti-Apoptosis Role in Osteosarcoma Cells
2021
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Overview
Heterogeneous nuclear ribonucleoprotein K (hnRNPK) is an RNA/DNA binding protein involved in diverse cell processes; it is also a p53 coregulator that initiates apoptosis under DNA damage conditions. However, the upregulation of hnRNPK is correlated with cancer transformation, progression, and migration, whereas the regulatory role of hnRNPK in cancer malignancy remains unclear. We previously showed that arginine methylation of hnRNPK attenuated the apoptosis of U2OS osteosarcoma cells under DNA damage conditions, whereas the replacement of endogenous hnRNPK with a methylation-defective mutant inversely enhanced apoptosis. The present study further revealed that an RNA helicase, DDX3, whose C-terminus preferentially binds to the unmethylated hnRNPK and could promote such apoptotic enhancement. Moreover, C-terminus-truncated DDX3 induced significantly less apoptosis than full-length DDX3. Notably, we also identified a small molecule that docks at the ATP-binding site of DDX3, promotes the DDX3-hnRNPK interaction, and induces further apoptosis. Overall, we have shown that the arginine methylation of hnRNPK suppresses the apoptosis of U2OS cells via interfering with DDX3–hnRNPK interaction. On the other hand, DDX3–hnRNPK interaction with a proapoptotic role may serve as a target for promoting apoptosis in osteosarcoma cells.
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