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Dominant-interfering forms of MEF2 generated by caspase cleavage contribute to NMDA-induced neuronal apoptosis

被引:116
作者
Okamoto, S
Li, Z
Ju, C
Schölzke, MN
Mathews, E
Cui, JK
Salvesen, GS
Bossy-Wetzel, E
Lipton, SA [1 ]
机构
[1] Burnham Inst, Ctr Neurosci & Aging, La Jolla, CA 92037 USA
[2] Burnham Inst, Apoptosis & Cell Death Res Program, La Jolla, CA 92037 USA
[3] Univ Calif San Diego, Mol Pathol Grad Program, La Jolla, CA 92093 USA
来源
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA | 2002年 / 99卷 / 06期
关键词
D O I
10.1073/pnas.022036399
中图分类号
O [数理科学和化学]; P [天文学、地球科学]; Q [生物科学]; N [自然科学总论];
学科分类号
07 ; 0710 ; 09 ;
摘要
Myocyte enhancer factor-2 (MEF2) transcription factors are activated by p38 mitogen-activated protein kinase during neuronal and myogenic differentiation. Recent work has shown that stimulation of this pathway is antiapoptotic during development but proapoptotic in mature neurons exposed to excitotoxic or other stress. We now report that excitotoxic (N-methyl-D-aspartate) insults to mature cerebrocortical neurons activate caspase-3, 7, in turn cleaving MEF2A, C, and D isoforms. MEF2 cleavage fragments containing a truncated transactivation domain but preserved DNA-binding domain block MEF2 transcriptional activity via dominant interference. Transfection of constitutively active MEF2 (MEF2C-CA) rescues MEF2 transcriptional activity after N-methyl-D-aspartate insult and prevents neuronal apoptosis. Conversely, dominant-interfering MEF2 abrogates neuroprotection by MEF2C-CA. These results define a pathway to excitotoxic neuronal stress/apoptosis via caspase-catalyzed cleavage of MEF2. Additionally, we show that similar MEF2 cleavage fragments are generated in vivo during focal stroke damage. Hence, this pathway appears to nave pathophysiological relevance in vivo.
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收藏
页码:3974 / 3979
页数:6
相关论文
共 39 条
[1]   APOPTOSIS AND NECROSIS - 2 DISTINCT EVENTS INDUCED, RESPECTIVELY, BY MILD AND INTENSE INSULTS WITH N-METHYL-D-ASPARTATE OR NITRIC-OXIDE SUPEROXIDE IN CORTICAL CELL-CULTURES [J].
BONFOCO, E ;
KRAINC, D ;
ANKARCRONA, M ;
NICOTERA, P ;
LIPTON, SA .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1995, 92 (16) :7162-7166
[2]   Mitochondrial and extramitochondrial apoptotic signaling pathways in cerebrocortical neurons [J].
Budd, SL ;
Tenneti, L ;
Lishnak, T ;
Lipton, SA .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 2000, 97 (11) :6161-6166
[3]   New perspectives on glaucoma [J].
Dreyer, EB ;
Lipton, SA .
JAMA-JOURNAL OF THE AMERICAN MEDICAL ASSOCIATION, 1999, 281 (04) :306-308
[4]   Activation of a caspase 3-related cysteine protease is required for glutamate-mediated apoptosis of cultured cerebellar granule neurons [J].
Du, YS ;
Bales, KR ;
Dodel, RC ;
HamiltonByrd, E ;
Horn, JW ;
Czilli, DL ;
Simmons, LK ;
Ni, BH ;
Paul, SM .
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1997, 94 (21) :11657-11662
[5]   Activation of the transcription factor MEF2C by the MAP kinase p38 in inflammation [J].
Han, J ;
Jiang, Y ;
Li, Z ;
Kravchenko, VV ;
Ulevitch, RJ .
NATURE, 1997, 386 (6622) :296-299
[6]   EXPRESSION OF A MADS BOX GENE, MEF2D, IN NEURONS OF THE MOUSE CENTRAL-NERVOUS-SYSTEM - IMPLICATION OF ITS BINARY FUNCTION IN MYOGENIC AND NEUROGENIC CELL LINEAGES [J].
IKESHIMA, H ;
IMAI, S ;
SHIMODA, K ;
HATA, J ;
TAKANO, T .
NEUROSCIENCE LETTERS, 1995, 200 (02) :117-120
[7]  
Jordan J, 1997, J NEUROCHEM, V68, P1612
[8]   Activation and involvement of p38 mitogen-activated protein kinase in glutamate-induced apoptosis in rat cerebellar granule cells [J].
Kawasaki, H ;
Morooka, T ;
Shimohama, S ;
Kimura, J ;
Hirano, T ;
Gotoh, Y ;
Nishida, E .
JOURNAL OF BIOLOGICAL CHEMISTRY, 1997, 272 (30) :18518-18521
[9]  
Kikuchi M, 2000, J NEUROSCI, V20, P5037
[10]   EFFECT OF NITRIC-OXIDE PRODUCTION ON THE REDOX MODULATORY SITE OF THE NMDA RECEPTOR CHANNEL COMPLEX [J].
LEI, SZ ;
PAN, ZH ;
AGGARWAL, SK ;
CHEN, HSV ;
HARTMAN, J ;
SUCHER, NJ ;
LIPTON, SA .
NEURON, 1992, 8 (06) :1087-1099
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