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Compound
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Target Concepts:
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Query: UMLS:C0022116 (
ischemia
)
91,303
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
alphaB-crystallin (alphaBC) is a small heat shock protein expressed at high levels in the myocardium where it protects from
ischemia
-reperfusion damage.
Ischemia
-reperfusion activates p38 MAP kinase, leading to the phosphorylation of alphaBC on serine 59 (P-alphaBC-S59), enhancing its ability to protect myocardial cells from damage. In the heart,
ischemia
-reperfusion also causes the translocation of alphaBC from the cytosol to other cellular locations, one of which was recently shown to be mitochondria. However, it is not known whether alphaBC translocates to mitochondria during
ischemia
-reperfusion, nor is it known whether alphaBC phosphorylation takes place before or after translocation. In the present study, analyses of mitochondrial fractions isolated from mouse hearts subjected to various times of ex vivo
ischemia
-reperfusion showed that alphaBC translocation to mitochondria was maximal after 20 min of
ischemia
and then declined steadily during reperfusion. Phosphorylation of mitochondrial alphaBC was maximal after 30 min of
ischemia
, suggesting that at least in part it occurred after alphaBC association with mitochondria. Consistent with this was the finding that translocation of activated p38 to mitochondria was maximal after only 10 min of
ischemia
. The overexpression of alphaBC-
AAE
, which mimics alphaBC phosphorylated on serine 59, has been shown to stabilize mitochondrial membrane potential and to inhibit apoptosis. In the present study, infection of neonatal rat cardiac myocytes with adenovirus-encoded alphaBC-
AAE
decreased peroxide-induced mitochondrial cytochrome c release. These results suggest that during
ischemia
alphaBC translocates to mitochondria, where it is phosphorylated and contributes to modulating mitochondrial damage upon reperfusion.
...
PMID:Kinetics of the translocation and phosphorylation of alphaB-crystallin in mouse heart mitochondria during ex vivo ischemia. 1925 88