TY - JOUR
T1 - Post-conditioning protects cardiomyocytes from apoptosis via PKC ε-interacting with calcium-sensing receptors to inhibit endo(sarco)plasmic reticulum-mitochondria crosstalk
AU - Dong, Shiyun
AU - Teng, Zongyan
AU - Lu, Fang Hao
AU - Zhao, Ya Jun
AU - Li, Hulun
AU - Ren, Huan
AU - Chen, He
AU - Pan, Zhen Wei
AU - Lv, Yan Jie
AU - Yang, Bao Feng
AU - Tian, Ye
AU - Xu, Chang Qing
AU - Zhang, Wei Hua
PY - 2010/8
Y1 - 2010/8
N2 - The intracellular Ca 2+ concentration ([Ca 2+] i) is increased during cardiac ischemia/reperfusion injury (IRI), leading to endo(sarco)plasmic reticulum (ER) stress. Persistent ER stress, such as with the accumulation of [Ca 2+] i, results in apoptosis. Ischemic post-conditioning (PC) can protect cardiomyocytes from IRI by reducing the [Ca 2+] i via protein kinase C (PKC). The calcium-sensing receptor (CaR), a G protein-coupled receptor, causes the production of inositol phosphate (IP 3) to increase the release of intracellular Ca 2+ from the ER. This process can be negatively regulated by PKC through the phosphorylation of Thr-888 of the CaR. This study tested the hypothesis that PC prevents cardiomyocyte apoptosis by reducing the [Ca 2+] i through an interaction of PKC with CaR to alleviate [Ca 2+] ER depletion and [Ca 2+] m elevation by the ER-mitochondrial associated membrane (MAM). Cardiomyocytes were post-conditioned after 3 h of ischemia by three cycles of 5 min of reperfusion and 5 min of re-ischemia before 6 h of reperfusion. During PC, PKC ε translocated to the cell membrane and interacted with CaR. While PC led to a significant decrease in [Ca 2+] i, the [Ca 2+] ER was not reduced and [Ca 2+] m was not increased in the PC and GdCl 3-PC groups. Furthermore, there was no evident ψ m collapse during PC compared with ischemia/reperfusion (I/R) or PKC inhibitor groups, as evaluated by laser confocal scanning microscopy. The apoptotic rates detected by TUNEL and Hoechst33342 were lower in PC and GdCl 3-PC groups than those in I/R and PKC inhibitor groups. Apoptotic proteins, including m-calpain, BAP31, and caspase-12, were significantly increased in the I/R and PKC inhibitor groups. These results suggested that PKC ε interacting with CaR protected post-conditioned cardiomyocytes from programmed cell death by inhibiting disruption of the mitochondria by the ER as well as preventing calcium-induced signaling of the apoptotic pathway.
AB - The intracellular Ca 2+ concentration ([Ca 2+] i) is increased during cardiac ischemia/reperfusion injury (IRI), leading to endo(sarco)plasmic reticulum (ER) stress. Persistent ER stress, such as with the accumulation of [Ca 2+] i, results in apoptosis. Ischemic post-conditioning (PC) can protect cardiomyocytes from IRI by reducing the [Ca 2+] i via protein kinase C (PKC). The calcium-sensing receptor (CaR), a G protein-coupled receptor, causes the production of inositol phosphate (IP 3) to increase the release of intracellular Ca 2+ from the ER. This process can be negatively regulated by PKC through the phosphorylation of Thr-888 of the CaR. This study tested the hypothesis that PC prevents cardiomyocyte apoptosis by reducing the [Ca 2+] i through an interaction of PKC with CaR to alleviate [Ca 2+] ER depletion and [Ca 2+] m elevation by the ER-mitochondrial associated membrane (MAM). Cardiomyocytes were post-conditioned after 3 h of ischemia by three cycles of 5 min of reperfusion and 5 min of re-ischemia before 6 h of reperfusion. During PC, PKC ε translocated to the cell membrane and interacted with CaR. While PC led to a significant decrease in [Ca 2+] i, the [Ca 2+] ER was not reduced and [Ca 2+] m was not increased in the PC and GdCl 3-PC groups. Furthermore, there was no evident ψ m collapse during PC compared with ischemia/reperfusion (I/R) or PKC inhibitor groups, as evaluated by laser confocal scanning microscopy. The apoptotic rates detected by TUNEL and Hoechst33342 were lower in PC and GdCl 3-PC groups than those in I/R and PKC inhibitor groups. Apoptotic proteins, including m-calpain, BAP31, and caspase-12, were significantly increased in the I/R and PKC inhibitor groups. These results suggested that PKC ε interacting with CaR protected post-conditioned cardiomyocytes from programmed cell death by inhibiting disruption of the mitochondria by the ER as well as preventing calcium-induced signaling of the apoptotic pathway.
KW - Calcium
KW - Calcium-sensing receptor
KW - ER-mitochondrial associated membrane (MAM)
KW - Post-conditioning
KW - Protein kinase C
UR - https://www.scopus.com/pages/publications/77955013436
U2 - 10.1007/s11010-010-0450-5
DO - 10.1007/s11010-010-0450-5
M3 - Article
C2 - 20383739
AN - SCOPUS:77955013436
SN - 0300-8177
VL - 341
SP - 195
EP - 206
JO - Molecular and Cellular Biochemistry
JF - Molecular and Cellular Biochemistry
IS - 1-2
ER -