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Anti-leukemic mechanisms of pegylated arginase I in acute lymphoblastic T-cell leukemia.


ABSTRACT: New treatments for adults with acute lymphoblastic T-cell leukemia (T-ALL) are urgently needed, as the current rate of overall remission in these patients is only about 40 percent. We recently showed the potential therapeutic benefit of the pegylated-human-arginase I (peg-Arg I) in T-ALL. However, the mechanisms by which peg-Arg I induces an anti-T-ALL effect remained unknown. Our results show the induction of T-ALL cell apoptosis by peg-Arg I, which associated with a global arrest in protein synthesis and with the phosphorylation of the eukaryotic-translation-initiation factor 2 alpha (eIF2?). Inhibition of eIF2? phosphorylation in T-ALL cells prevented the apoptosis induced by peg-Arg I, whereas the expression of a phosphomimetic eIF2? form increased the sensibility of T-ALL cells to peg-Arg I. Phosphorylation of eIF2? by peg-Arg I was mediated through kinases PERK and GCN2 and down-regulation of phosphatase GADD34. GCN2 and decreased GADD34 promoted T-ALL cell apoptosis after treatment with peg-Arg I, whereas PERK had an unexpected anti-apoptotic role. Additional results showed that phospho-eIF2? signaling further increased the anti-leukemic effects induced by peg-Arg I in T-ALL-bearing mice. These results suggest the central role of phospho-eIF2? in the anti-T-ALL effects induced by peg-Arg I and support its study as a therapeutic target.

SUBMITTER: Morrow K 

PROVIDER: S-EPMC3594435 | biostudies-literature | 2013 Mar

REPOSITORIES: biostudies-literature

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Anti-leukemic mechanisms of pegylated arginase I in acute lymphoblastic T-cell leukemia.

Morrow K K   Hernandez C P CP   Raber P P   Del Valle L L   Wilk A M AM   Majumdar S S   Wyczechowska D D   Reiss K K   Rodriguez P C PC  

Leukemia 20120828 3


New treatments for adults with acute lymphoblastic T-cell leukemia (T-ALL) are urgently needed, as the current rate of overall remission in these patients is only about 40 percent. We recently showed the potential therapeutic benefit of the pegylated-human-arginase I (peg-Arg I) in T-ALL. However, the mechanisms by which peg-Arg I induces an anti-T-ALL effect remained unknown. Our results show the induction of T-ALL cell apoptosis by peg-Arg I, which associated with a global arrest in protein sy  ...[more]

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