MicroRNA调控神经可塑性在抑郁症中作用研究进展

doi:10.3969/j.issn.2095-1396.2017.03.003

神经药理学报 ›› 2017, Vol. 7 ›› Issue (3): 12-20.DOI: 10.3969/j.issn.2095-1396.2017.03.003

MicroRNA调控神经可塑性在抑郁症中作用研究进展

任倩，王真真，陈乃宏

1. 中国医学科学院，药物研究所 & 神经科学中心，北京 100050，中国
2. 湖南中医药大学药学院，长沙，410208，中国

出版日期:2017-06-26 发布日期:2017-12-01
通讯作者: 陈乃宏，男，博士，研究员；研究方向：神经药理及神经分子生物学；Tel：+86-10-63165177，Fax：86-10-63165211，E-mail：chennh@imm.ac.cn
作者简介:任倩，女，硕士，研究生；研究方向：神经药理及神经分子生物学；Tel：+86-10-63165211，E-mail：renqian@imm.ac.cn
基金资助:
国家自然科学基金项目（No.81573636，U1402221，81560663），北京协和医学院“协和青年基金”（ No.3332016058），中央级公益性科研院所基本科研业务费专项资金（No.2014RC03，2016RC350002），湖南省重点研发计划项目（No.2015SK2029-1），湖南省教育厅高校科研经费开放基金项目（No.15K091），新药作用机制研究与药效评价北京市重点实验室资助项目（No.BZ0150）

Regulation of Neuroplasticity by MicroRNA in Depression Disorder

REN Qian 1，WANG Zhen-zhen 1，CHEN Nai-hong 1，2

1. State Key Laboratory of Bioactive Substances and Functions of Natural Medicines，Institute of Materia Medica & Neuroscience Center，Chinese Academy of Medical Sciences and Peking Union Medical College，Beijing，100050，China
2. College of Pharmacy，Hunan University of Chinese Medicine，Changsha，410208，China

Online:2017-06-26 Published:2017-12-01
Contact: 陈乃宏，男，博士，研究员；研究方向：神经药理及神经分子生物学；Tel：+86-10-63165177，Fax：86-10-63165211，E-mail：chennh@imm.ac.cn
About author:任倩，女，硕士，研究生；研究方向：神经药理及神经分子生物学；Tel：+86-10-63165211，E-mail：renqian@imm.ac.cn
Supported by:
国家自然科学基金项目（No.81573636，U1402221，81560663），北京协和医学院“协和青年基金”（ No.3332016058），中央级公益性科研院所基本科研业务费专项资金（No.2014RC03，2016RC350002），湖南省重点研发计划项目（No.2015SK2029-1），湖南省教育厅高校科研经费开放基金项目（No.15K091），新药作用机制研究与药效评价北京市重点实验室资助项目（No.BZ0150）

摘要/Abstract

摘要： 抑郁症是一种危害人类身心健康的慢性、易复发的常见精神心理疾病，有很高的致死致残率。MicroRNA（miRNA）是一类近年发现的在生物体内广泛分布的长约 22 个核苷酸的新型微小非编码 RNA。它通常是通过与靶 mRNA 的 3’UTR 结合，抑制 mRNA 翻译或调节 mRNA 降解来调控生物体内一系列的生理、病理过程。近年来研究表明抑郁症患者神经元结构和功能，神经元突触传递与可塑性等发生改变，基因表达增加，而 miRNA 发挥重要的调控作用。该文就近年来miRNA 在抑郁症中调控神经可塑性的研究进展进行综述，以期为深入认识和治疗抑郁症带来新的启示。

关键词: miRNA , mRNA, 抑郁症, 神经可塑性

Abstract: Depression is a debilitating disease. It is easy to relapse and has high mortality disability. MicroRNA （miRNA），recently discovered as a novel small non-coding RNA and widely distributed in the body，is a class of length of 22 nucleotides. It usually inhibits mRNA translation or mediate mRNA degradation to control a series of physiological and pathological processes by binding to target mRNA 3’UTR in vivo. Recent studies show that patients with depression disorder are involved in the changes of neuronal structures and function，the disorder of neuroplasticity and synaptic transmission，as well as increasing mRNA. miRNA plays an important role in these process. In this review，in order to further understand and find better the treatment of depression，we summarize the recent studies of miRNA about neuroplasticity in depression disorder.

Key words: miRNA, mRNA, depression, neuroplasticity

中图分类号:

R964

任倩，王真真，陈乃宏. MicroRNA调控神经可塑性在抑郁症中作用研究进展[J]. 神经药理学报, 2017, 7(3): 12-20.

REN Qian,WANG Zhen-zhen,CHEN Nai-hong. Regulation of Neuroplasticity by MicroRNA in Depression Disorder[J]. Acta Neuropharmacologica, 2017, 7(3): 12-20.

参考文献

[1] Natascha Bushati, Stephen M Cohen. microRNA functions[J]. Annu Rev Cell Dev Biol, 2007, 23: 175-205.

[2] Kwak PB, Iwasaki S, Tomari Y. The microRNA pathway and cancer[J]. Cancer Sci, 2010, 101(11): 2309-2315.

[3] Abrar Qurashi, Jin Peng. Small RNA-mediated gene regulation in neurodevelopmental disorders[J]. Curr Psychiatry Rep, 2010, 12(2): 154-161.

[4] Jeffrey S Ross, J Andrew Carlson, Graham Brock. miRNA: the new gene silencer[J]. Am J Clin Pathol, 2007, 128(5): 830-836.

[5] Nuray Varol, Ece Konac, Serhat Gurocak, et al. The realm of microRNAs in cancers[J]. Mol Biol Rep, 2011, 38(2): 1079-1089.

[6] Kenneth S Kosik. The neuronal microRNA system[J]. Nat Rev Neurosci, 2006, 7(12): 911-920.

[7] Li Long-cheng, Steven T Okino, Zhao Hong, et al. Small dsRNAs induce transcriptional activation in human cells[J]. Proc Natl Acad Sci USA, 2006, 103(46): 17337-17342.

[8] Heh-In Im, Paul J Kenny. MicroRNAs in neuronal function and dysfunction[J]. Trends Neurosci, 2012, 35(5): 325-334.

[9] Michalak P. RNA world-the dark matter of evolutionary genomics[J]. J Evol Biol, 2006, 19(6): 1768-1774.

[10] Robert F Place, Li Long-cheng, Deepa Pookot, et al. MicroRNA-373 induces expression of genes with complementary promoter sequences[J]. Proc Natl Acad Sci USA, 2008, 105(5): 1608-1613.

[11] John Tsang, Zhu Jun, Alexander van Oudenaarden. MicroRNA-mediated feedback and feedforward loops are recurrent network motifs in mammals[J]. Mol Cell, 2007, 26(5): 753-767.

[12] Oved K, Morag A, Pasmanik-Chor M, et al. Genome-wide expression profiling of human lymphoblastoid cell lines implicates integrin beta-3 in the mode of action of antidepressants[J]. Transl Psychiatry, 2013, 3: e313.

[13] Shobha Vasudevan, Tong Ying-chun, Joan A Steitz. Switching from repression to activation: microRNAs can up-regulate translation[J]. Science, 2007, 318(5858):1931-1934.

[14] Zhou Yi-ming, John Ferguson, Joseph T Chang, et al. Inter- and intra-combinatorial regulation by transcription factors and microRNAs[J]. BMC Genomics, 2007, 8: 396.

[15] Caroline Dias, Feng Jian, Sun Hao-sheng, et al. beta-catenin mediates stress resilience through Dicer1/microRNA regulation[J]. Nature, 2014, 516(7529): 51-55.

[16] Vivien Wang, Wu Wei. MicroRNA-based therapeutics for cancer[J]. Bio Drugs, 2009, 23(1): 15-23.

[17] Carlo M Croce. Causes and consequences of microRNA dysregulation in cancer[J]. Nat Rev Genet, 2009, 10(10): 704-714.

[18] Sai Yendamuri, George A Calin. The role of microRNA in human leukemia: a review[J]. Leukemia, 2009, 23(7): 1257-1263.

[19] Marika Kapsimali, Wigard P Kloosterman, Ewart de Bruijn, et al. MicroRNAs show a wide diversity of expression profiles in the developing and mature central nervous system[J]. Genome Biol, 2007, 8(8): R173.

[20] Lena Smirnova, Anja Grafe, Andrea Seiler, et al. Regulation of miRNA expression during neural cell specification[J]. Eur J Neurosci, 2005, 21(6): 1469-1477.

[21] Lorenzo F Sempere, Sarah Freemantle, Ian Pitha-Rowe, et al. Expression profiling of mammalian microRNAs uncovers a subset of brain-expressed microRNAs with possible roles in murine and human neuronal differentiation[J]. Genome Biol, 2004, 5(3): R13.

[22] Erno Vreugdenhil, Eugene Berezikov. Fine-tuning the brain: MicroRNAs[J]. Front Neuroendocrinol, 2010, 31(2):128-133.

[23] Roberto Fiore, Gabriele Siegel, Gerhard Schratt. MicroRNA function in neuronal development, plasticity and disease[J]. Biochim Biophys Acta, 2008, 1779(8): 471-478.

[24] Victor Ambros. The functions of animal microRNAs[J]. Nature, 2004, 431(7006): 350-355.

[25] Pablo Landgraf, Mirabela Rusu, Robert Sheridan, et al. A mammalian microRNA expression atlas based on small RNA library sequencing[J]. Cell, 2007, 129(7): 1401-1414.

[26] Chiaki Itami, Fumitaka Kimura. Concurrently-induced plasticity due to convergence of distinct forms of spike timing-dependent plasticity in the developing barrel cortex[J]. Eur J Neurosci, 2016, DOI: 10.1111/ejn.13431.

[27] Mary P Heyer, Paul J Kenny. MicroRNA-mediated repression combats depression[J]. Neuron, 2014, 83(2): 253-254.

[28] Nirit Kara, Galila Agam, Grant W Anderson, et al. Lack of effect of chronic ketamine administration on depression-like behavior or frontal cortex autophagy in female and male ICR mice[J]. Behav Brain Res, 2016, 317:576-580.

[29] Bas van Bommel, Marina Mikhaylova. Talking to the neighbours: The molecular and physiological mechanisms of clustered synaptic plasticity[J]. Neurosci Biobehav Rev, 2016, 71: 352-361.

[30] Hu Zhong-hua, Yu Dan-ni, Gu Qin-hua, et al. miR-191 and miR-135 are required for long-lasting spine remodelling associated with synaptic long-term depression[J]. Nat Commun, 2014, 5:3263.

[31] Mariana Alonso, Cecile Viollet, Marie-Madeleine Gabellec, et al. Olfactory discrimination learning increases the survival of adult-born neurons in the olfactory bulb[J]. J Neurosci, 2006, 26(41):10508-10513.

[32] Orly Lazarov, Mark P Mattson, Daniel A Peterson, et al. When neurogenesis encounters aging and disease[J]. Trends Neurosci, 2010, 33(12): 569-579.

[33] Orna Issler, Sharon Haramati, Evan D Paul, et al. MicroRNA 135 is essential for chronic stress resiliency, antidepressant efficacy, and intact serotonergic activity[J]. Neuron, 2014, 83(2): 344-360.

[34] Philip S Choi, Lisa Zakhary, Wen-Yee Choi, et al. Members of the miRNA-200 family regulate olfactory neurogenesis[J]. Neuron, 2008, 57(1): 41-55.

[35] Juan Pablo Lopez, Raymond Lim, Cristiana Cruceanu, et al. miR-1202 is a primate-specific and brain-enriched microRNA involved in major depression and antidepressant treatment[J]. Nat Med, 2014, 20(7): 764-768.

[36] Cheng Li-chun, Erika Pastrana, Masoud Tavazoie, et al. miR-124 regulates adult neurogenesis in the subventricular zone stem cell niche[J]. Nat Neurosci, 2009, 12(4): 399-408.

[37] Ziats M N, Rennert O M. Identification of differentially expressed microRNAs across the developing human brain[J]. Mol Psychiatry, 2014, 19(7): 848-852.

[38] Chen Hai-ming, Wang Nu-lang, Margit Burmeister, et al. MicroRNA expression changes in lymphoblastoid cell lines in response to lithium treatment[J]. Int J Neuropsychopharmacol, 2009, 12(7): 975-981.

[39] Keith E Szulwach, Li Xue-kun, Richard D Smrt, et al. Cross talk between microRNA and epigenetic regulation in adult neurogenesis[J]. J Cell Biol, 2010, 189(1): 127-141.

[40] Krassimira A Garbett, Andrea Vereczkei, Sara Kalman, et al. Coordinated messenger RNA/microRNA changes in fibroblasts of patients with major depression[J]. Biol Psychiatry, 2015, 77(3):256-265.

[41] Jin Peng, Daniela C Zarnescu, Stephanie Ceman, et al T. Biochemical and genetic interaction between the fragile X mental retardation protein and the microRNA pathway[J]. Nat Neurosci, 2004, 7(2): 113-117.

[42] Michael Geaghan, Murray J Cairns. MicroRNA and posttranscriptional dysregulation in psychiatry[J]. Biol Psychiatry, 2015, 78(4): 231-239.

[43] Amy A Caudy, Mike Myers, Gregory J Hannon, et al. Fragile X-related protein and VIG associate with the RNA interference machinery[J]. Genes Dev, 2002, 16(19): 2491-2496.

[44] Aliza P Wingo, Lunn M Almli, Jennifer S Stevens, et al. DICER1 and microRNA regulation in post-traumatic stress disorder with comorbid depression[J]. Nat Commun, 2015, 6: 10106.

[45] Laura M Fiori, Juan Pablo Lopez, Stephane Richard-Devantoy, et al. Investigation of miR-1202, miR-135a, and miR-16 in Major Depressive Disorder and Antidepressant Response[J]. Int J Neuropsychopharmacol, 2017, DOI: 10.1016/j.pnpbp.2015.02.003 .

[46] Giovanni Lugli, John Larson, Maryann E Martone, et al. Dicer and eIF2c are enriched at postsynaptic densities in adult mouse brain and are modified by neuronal activity in a calpain-dependent manner[J]. J Neurochem, 2005, 94(4):896-905.

[47] William T Carrick, Brandi Burks, Murray J Cairns, et al. Noncoding RNA regulation of dopamine signaling in diseases of the central nervous system[J]. Front Mol Biosci, 2016, 3: 69.

[48] Giovanni Lugli, Vetle I Torvik, john Larson, et al. Expression of microRNAs and their precursors in synaptic fractions of adult mouse forebrain[J]. J Neurochem, 2008, 106(2): 650-661.

[49] Lopez Juan Pablo, Fiori Laura M, Cruceanu Cristiana, et al. MicroRNAs 146a/b-5 and 425-3p and 24-3p are markers of antidepressant response and regulate MAPK/Wnt-system genes[J]. Nat Commun, 2017, 8:15497.

[50] Gerhard M Schratt, Fabian Tuebing, Elizabeth A Nigh, et al. A brain-specific microRNA regulates dendritic spine development[J]. Nature, 2006, 439(7074): 283-289.

[51] Bhaskar Roy, Michael Dunbar, Richard C Shelton, et al. Identification of MicroRNA-124-3p as a putative epigenetic signature of major depressive disorder[J]. Neuropsychopharmacology, 2017, 42(4):864-875.

[52] Gerhard M Schratt, Elizabeth A Nigh, Wen G Chen, et al. BDNF regulates the translation of a select group of mRNAs by a mammalian target of rapamycin-phosphatidylinositol 3-kinase-dependent pathway during neuronal development[J]. J Neurosci, 2004, 24(33):7366-7377.

[53] Gabriele Siegel, Gregor Obernosterer, Roberto Fiore, et al. A functional screen implicates microRNA-138-dependent regulation of the depalmitoylation enzyme APT1 in dendritic spine morphogenesis[J]. Nat Cell Biol, 2009, 11(6):705-716.

[54] Rong Han, Liu Tie-bang, Yang Kong-jun, et al. MicroRNA-134 plasma levels before and after treatment for bipolar mania[J]. J Psychiatr Res, 2011, 45(1):92-95.

[55] Priyamvada Rajasethupathy, Ferdinando Fiumara, Robert Sheridan, et al. Characterization of small RNAs in Aplysia reveals a role for miR-124 in constraining synaptic plasticity through CREB[J]. Neuron, 2009, 63(6):803-817.

[56] Xu Yong, Li Fei, Zhang Bo, et al. MicroRNAs and target site screening reveals a pre-microRNA-30e variant associated with schizophrenia[J]. Schizophr Res, 2010, 119(1-3):219-227.

[57] Gary A Wayman, Monika Davare, Hideaki Ando, et al. An activity-regulated microRNA controls dendritic plasticity by down-regulating p250GAP[J]. Proc Natl Acad Sci USA, 2008, 105(26):9093-9098.

[58] Soren Impey, Monika Davare, Adam Lesiak, et al. An activity-induced microRNA controls dendritic spine formation by regulating Rac1-PAK signaling[J]. Mol Cell Neurosci, 2010, 43(1):146-156.

[59] Mojtaba Khaksarian, Hossein Mostafavi, Masoud Soleimani M, et al. Regulation of connexin 43 and microRNA expression via beta2-adrenoceptor signaling in 1321N1 astrocytoma cells[J]. Mol Med Rep, 2015, 12(2):1941-1950.

[60] Arianna Rinaldi, Sara Vincenti, Francesca De Vito, et al. Stress induces region specific alterations in microRNAs expression in mice[J]. Behav Brain Res, 2010, 208(1):265-269.

[61] Shusaku Uchida, Kumiko Hara, Ayumi Kobayashi, et al. Early life stress enhances behavioral vulnerability to stress through the activation of REST4-mediated gene transcription in the medial prefrontal cortex of rodents[J]. J Neurosci, 2010, 30(45):15007-15018.

[62] Shusaku Uchida, Akira Nishida, Kumiko Hara, et al. Characterization of the vulnerability to repeated stress in Fischer 344 rats: possible involvement of microRNA-mediated down-regulation of the glucocorticoid receptor[J]. Eur J Neurosci, 2008, 27(9).2250-2261.

[63] Erno Vreugdenhil, Carla S Verissimo, Rob Mariman, et al. MicroRNA 18 and 124a down-regulate the glucocorticoid receptor: implications for glucocorticoid responsiveness in the brain[J]. Endocrinology, 2009, 150(5):2220-2228.

[64] Zheng Ge, Minli Pan, Jin Wei-min, et al. MicroRNA-135a is up-regulated and aggravates myocardial depression in sepsis via regulating p38 MAPK/NF-kappaB pathway[J]. Int Immunopharmacol, 2017, 45:6-12.

[65] Kawashima H, Numakawa T, Kumamaru E, et al. Glucocorticoid attenuates brain-derived neurotrophic factor-dependent upregulation of glutamate receptors via the suppression of microRNA-132 expression[J]. Neuroscience, 2010, 165(4):1301-1311.

[66] Zhou Min, Wang Mao-hua, Wang Xiao-bin, et al. Abnormal expression of MicroRNAs induced by chronic unpredictable mild stress in rat hippocampal tissues[J]. Mol Neurobiol, 2017, DOI: 10.1007/s12035-016-0365-6.

[67] Ngan Vo, Matthew E Klein, Olga Varlamova, et al. A cAMP-response element binding protein-induced microRNA regulates neuronal morphogenesis[J]. Proc Natl Acad Sci USA, 2005, 102(45):16426-16431.

[68] Nikolaos Mellios, Huang Hsien-Sung, Anastasia Grigorenko, et al. A set of differentially expressed miRNAs, including miR-30a-5p, act as post-transcriptional inhibitors of BDNF in prefrontal cortex[J]. Hum Mol Genet, 2008, 17(19):3030-3042.

[69] Ari Meerson, Luisa Cacheaux, Ki Ann Goosens, et al. Changes in brain MicroRNAs contribute to cholinergic stress reactions[J]. J Mol Neurosci, 2010, 40(1-2):47-55.

[70] Short A K, Yeshurun S, Powell R, et al. Exercise alters mouse sperm small noncoding RNAs and induces a transgenerational modification of male offspring conditioned fear and anxiety[J]. Transl Psychiatry, 2017, 7(5):e1114.

[71] Grazyna Rajkowska. Histopathology of the prefrontal cortex in major depression: what does it tell us about dysfunctional monoaminergic circuits?[J]. Prog Brain Res, 2000, 126: 397-412.

[72] Angelica Torres-Berrio, Juan Pablo Lopez, Rosemary C Bagot, et al. DCC Confers Susceptibility to Depression-like Behaviors in Humans and Mice and Is Regulated by miR-218[J]. Biol Psychiatry, 2017, 81(4):306-315.

[73] Witold Konopka, Anna Kiryk, Martin Novak, et al. MicroRNA loss enhances learning and memory in mice[J]. J Neurosci, 2010, 30(44):14835-14842.

[74] de Kloet E R, Fitzsimons C P, Datson N A, et al. Glucocorticoid signaling and stress-related limbic susceptibility pathway: about receptors, transcription machinery and microRNA[J]. Brain Res, 2009, 1293: 129-141.

[75] Anne Baudry, Sophie Mouillet-Richard, Benoit Schneider, et al. miR-16 targets the serotonin transporter: a new facet for adaptive responses to antidepressants[J]. Science, 2010, 329(5998): 1537-1541.

[76] Carmine M Pariante, Andrew H Miller. Glucocorticoid receptors in major depression: relevance to pathophysiology and treatment[J]. Biol Psychiatry, 2001, 49(5):391-404.

[77] Jonathan D Turner, Simone R Alt, Cao Lei, et al. Transcriptional control of the glucocorticoid receptor: CpG islands, epigenetics and more[J]. Biochem Pharmacol, 2010, 80(12):1860-1868.

[78] Wasserman D, Wasserman J, Sokolowski M. Genetics of HPA-axis, depression and suicidality[J]. Eur Psychiatry, 2010, 25(5): 278-280.

[79] Gao Jun, Wang Wen-yuan, Mao Ying-wei, et al. A novel pathway regulates memory and plasticity via SIRT1 and miR-134[J]. Nature, 2010, 466(7310): 1105-1109.

MicroRNA调控神经可塑性在抑郁症中作用研究进展

Regulation of Neuroplasticity by MicroRNA in Depression Disorder

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