Endogenous level of TIGAR in brain is associated with vulnerability of neurons to ischemic injury--Neuroscience Bulletin

Volume 31, Issue. 5, October, 2015

Endogenous level of TIGAR in brain is associated with vulnerability of neurons to ischemic injury

Lijuan Cao1,#, Jieyu Chen1,#, Mei Li1, Yuan-Yuan Qin1, Meiling Sun1, Rui Sheng1, Feng Han2, Guanghui Wang3, Zheng-Hong Qin1

1Department of Pharmacology and Laboratory of Aging and Nervous Diseases, Jiangsu Key Laboratory of Translational Research and Therapy for Neuro-Psycho-Diseases, College of Pharmaceutical Science, Soochow University, Suzhou 215123, China
2Institute of Pharmacology, Toxicology and Biochemical Pharmaceutics, Zhejiang University, Hangzhou 310058, China
3Department of Pharmacology and Laboratory of Molecular Neuropathology, Soochow University School of Pharmaceutical Science, Suzhou 215123, China
#These authors contributed equally to this work.
Corresponding author: Zheng-Hong Qin. E-mail: qinzhenhong@suda.edu.cn

Abstract

In previous studies, we showed that TP53-induced glycolysis and apoptosis regulator (TIGAR) protects neurons against ischemic brain injury. In the present study, we investigated the developmental changes of TIGAR level in mouse brain and the correlation of TIGAR expression with the vulnerability of neurons to ischemic injury. We found that the TIGAR level was high in the embryonic stage, dropped at birth, partially recovered in the early postnatal period, and then continued to decline to a lower level in early adult and aged mice. The TIGAR expression was higher after ischemia/reperfusion in mouse brain 8 and 12 weeks after birth. Four-week-old mice had smaller infarct volumes, lower neurological scores, and lower mortality rates after ischemia than 8- and 12-week-old mice. TIGAR expression also increased in response to oxygen glucose deprivation (OGD)/reoxygenation insult or H2O2 treatment in cultured primary neurons from different embryonic stages (E16 and E20). The neurons cultured from the early embryonic period had a greater resistance to OGD and oxidative insult. Higher TIGAR levels correlated with higher pentose phosphate pathway activity and less oxidative stress. Older mice and more mature neurons had more severe DNA and mitochondrial damage than younger mice and less mature neurons in response to ischemia/reperfusion or OGD/reoxygenation insult. Supplementation of cultured neurons with nicotinamide adenine dinuclectide phosphate (NADPH) significantly reduced ischemic injury. These results suggest that TIGAR expression changes during development and its expression level may be correlated with the vulnerability of neurons to ischemic injury.

Keywords

TIGAR; NADPH; ischemia; OGD; H2O2

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