Abstract
Src family tyrosine kinases (SFKs) phosphorylate caspase-8A at tyrosine (Y) 397 resulting in suppression of apoptosis. In addition, the phosphorylation of caspase-8A at other sites including Y465 has been implicated in the regulation of caspase-8 activity. However, the functional consequences of these modifications on caspase-8 processing/activity have not been elucidated. Moreover, various Src substrates are known to act as potent Src regulators, but no such role has been explored for caspase-8. We asked whether the newly identified caspase-8 phosphorylation sites might regulate caspase-8 activation and conversely, whether caspase-8 phosphorylation might affect Src activity. Here we show that Src phosphorylates caspase-8A at multiple tyrosine sites; of these, we have focused on Y397 within the linker region and Y465 within the p12 subunit of caspase-8A. We show that phosphomimetic mutation of caspase-8A at Y465 prevents its cleavage and the subsequent activation of caspase-3 and suppresses apoptosis. Furthermore, simultaneous phosphomimetic mutation of caspase-8A at Y397 and Y465 promotes the phosphorylation of c-Src at Y416 and increases c-Src activity. Finally, we demonstrate that caspase-8 activity prevents its own tyrosine phosphorylation by Src. Together these data reveal that dual phosphorylation converts caspase-8 from a pro-apoptotic to a pro-survival mediator. Specifically, tyrosine phosphorylation by Src renders caspase-8 uncleavable and thereby inactive, and at the same time converts it to a Src activator. This novel dynamic interplay between Src and caspase-8 likely acts as a potent signal-integrating switch directing the cell towards apoptosis or survival.
Highlights
Caspase-8, the apical caspase in the extrinsic pathway of apoptosis, is activated by the ligation of death receptors [1,2,3,4]
We show that phosphomimetic mutation of caspase-8A at Y465 suppresses apoptosis by inhibiting caspase-8 cleavage, whereas simultaneous phosphomimetic mutation of caspase8A at Y397 and Y465 activates c-Src, suggesting that dual phosphorylation converts caspase-8 from a pro-apoptotic to a pro-survival protein that serves as a Src substrate and Src activator
We showed that in caspase-8A, Y8 within the N-terminal domain; Y243, Y310 and Y351 within the p18 subunit; Y397 within the linker region and Y465 within the p12 subunit could be phosphorylated by Src family tyrosine kinases (SFKs) (Table 2 and Fig 1A)
Summary
Caspase-8, the apical caspase in the extrinsic pathway of apoptosis, is activated by the ligation of death receptors [1,2,3,4]. Pro-caspase-8 is expressed as a zymogen consisting of an N-terminal pro-domain, with two death effector domains (DED) [5,6,7,8,9], followed by a large (p18) and a small (p12) enzyme subunits. Caspase-8 activation requires its dimerization (in proximity) followed by a 2-step cleavage after aspartic acid (D) residues. The mature caspase-8 enzyme, consisting of two p18 and two p12 subunits [5,6,7,8,9,10,11,12], cleaves and activates downstream proteases including caspase-3, to allow apoptosis to proceed
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