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Author Contributions
Acknowledgments
Introduction
Cerebral ischemia-reperfusion (I/R) injury is a pathological phenomenon that occurs after restoration of blood supply to meclofenamate tissues subsequent to ischemia or hypoxia (Carden and Granger, 2000). It typically occurs after therapeutic thrombolysis in patients with acute ischemic stroke. I/R injury aggravates neuronal insult and may lead to disability and death (Bai and Lyden, 2015, Pan et al., 2007). Treatment outcomes of I/R are typically poor; innovative approaches are required to prevent brain damage induced by I/R (Eltzschig and Eckle, 2011).
Recent studies have demonstrated a pivotal role of autophagy in the regulation of I/R-induced neuronal cell injury (Descloux et al., 2015, Gabryel et al., 2012, Xu et al., 2012, Xu et al., 2013, Zhang et al., 2013). Autophagy is an essential intracellular catabolic pathway responsible for the turnover of long-lived proteins and cellular components (Feng et al., 2014). Based on the mechanism of substrate-delivery to lysosome, three different forms of autophagic pathways are recognized: macroautophagy, microautophagy, and chaperone-mediated autophagy (Feng et al., 2014). Macroautophagy, hereinafter referred to as autophagy, initiates with the formation of double-membraned phagophore (also known as isolation membrane), which encapsulates intracellular materials and matures into an autophagosome (He and Klionsky, 2009). Autophagosome fuses with lysosome and degrades engulfed cargo for recycling.
Activation of autophagy in the reperfusion phase of I/R has been demonstrated in rodent brain as well as in cultured neurons following oxygen-glucose deprivation (OGD)/reperfusion (OGD/R) (Zhang et al., 2013). The autophagy inhibitor, 3-methyladenine (3-MA), has been shown to prevent death of hippocampal CA1 neurons in a rat model of I/R injury (Wang et al., 2011), which suggests that autophagic cell death may contribute to hippocampal damage induced by I/R. However, the regulatory role of autophagy in neuronal damage is yet to be fully elucidated.
Calcium overload, caused by increased Ca2+ influx from extracellular environment or release from intracellular stores, is known to be an initial event in ischemic neuronal damage in brain (D'Orsi et al., 2015, Pringle, 2004). Ca2+ influx through ion channels formed by α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid-type (AMPA-type) glutamate receptor (AMPAR) are shown to be involved in hypoxic-ischemic brain injury (Deng et al., 2003, Gerace et al., 2015, Tang and Xing, 2013). Four subunits, namely GluR1-4, have been identified as the main components of Ca2+-permeable AMPAR channels (Liu and Savtchouk, 2012). Degradation of GluR1 in hippocampal neurons has been shown to be regulated by autophagy (Shehata et al., 2012), which implies an association between autophagic pathway and GluR-modulated Ca2+ influx.
Hippocampus is particularly vulnerable to I/R injury (Kirino and Sano, 1984). Abundant expression of GluR1, GluR2, and GluR3 are found in hippocampal neurons (Shi et al., 2001). Based on this body of evidence, we investigated the role of autophagy in mediating OGD/R injury in cultured hippocampal neurons. The association between autophagy and AMPARs was also explored.
Results
Discussion
In this study, we observed a rapid and sustained induction of autophagy in cultured rat hippocampal neurons following OGD/R injury. Pretreatment with 3-MA significantly reduced the intracellular Ca2+ concentration and GluR expression in hippocampal neurons. Increased expression of autophagy-related proteins, LC3-II and Beclin 1, and reduced expression of autophagy-specific substrate p62/SQSTM 1, has been widely detected in neuronal cells following OGD/R injury (Yu et al., 2014, Zhang et al., 2013). Our results are consistent with previous reports. Compared to 0.5-h of OGD treatment, prolonged OGD treatment (1h) exacerbated autophagic activity. Administration of 3-MA significantly abolished autophagy induction as well as cell injury, indicating autophagy may play a deleterious role in hippocampal survival following OGD/R.