中国神经精神疾病杂志
中國神經精神疾病雜誌
중국신경정신질병잡지
CHINESE JOURNAL OF NERVOUS AND MENTAL DISEASES
2013年
11期
641-645
,共5页
修芸%张蕾%仇玄%陈林%卢伟%彭超%程国华%晁凤蕾%唐勇
脩蕓%張蕾%仇玄%陳林%盧偉%彭超%程國華%晁鳳蕾%唐勇
수예%장뢰%구현%진림%로위%팽초%정국화%조봉뢰%당용
精神分裂症%MK-801%NMDA阻断%胼胝体%脱髓鞘
精神分裂癥%MK-801%NMDA阻斷%胼胝體%脫髓鞘
정신분렬증%MK-801%NMDA조단%변지체%탈수초
Schizophrenia%MK-801%NMDA antagonism%Corpus callosum%Demyelization
目的:探讨白质/髓鞘损伤在N-甲基-D-天冬氨酸(N-methyl-D aspartate,NMDA)受体阻断致精神分裂症(schizophrenia,SZ)中的作用。方法雄性C57 BL/6J小鼠(8周龄)48只,随机分为地卓西平马来酸盐(dizocilpine, MK-801)慢性给药M1组(0.25mg/kg)、M2组(0.50mg/kg)和M3组(1.00mg/kg)及对照组(生理盐水)。以Morris水迷宫、探孔和转棒测试检验小鼠行为学改变,运用免疫组化、透射电镜及体视学方法观察其胼胝体内髓鞘的改变。结果各模型组小鼠与对照组比较,空间学习记忆能力无明显下降(均P>0.05),M1和M3组小鼠较对照组表现出对新环境探索减少的SZ阴性症状;大脑胼胝体区MBP染色M1组(179±10)%、M2组(235±7)%、M3组(152±9)%小鼠较对照组(288±18)%均降低(均P<0.01),其内有髓神经纤维髓鞘出现板层分离、节段性脱髓鞘等病变,M3组小鼠胼胝体内损伤有髓神经纤维比例高于对照组[(22.42±4.24)%vs.(3.84±1.35)%],差异有统计学意义(P<0.01)。结论胼胝体脱髓鞘改变可能是MK-801慢性给药诱导SZ的病因之一。
目的:探討白質/髓鞘損傷在N-甲基-D-天鼕氨痠(N-methyl-D aspartate,NMDA)受體阻斷緻精神分裂癥(schizophrenia,SZ)中的作用。方法雄性C57 BL/6J小鼠(8週齡)48隻,隨機分為地卓西平馬來痠鹽(dizocilpine, MK-801)慢性給藥M1組(0.25mg/kg)、M2組(0.50mg/kg)和M3組(1.00mg/kg)及對照組(生理鹽水)。以Morris水迷宮、探孔和轉棒測試檢驗小鼠行為學改變,運用免疫組化、透射電鏡及體視學方法觀察其胼胝體內髓鞘的改變。結果各模型組小鼠與對照組比較,空間學習記憶能力無明顯下降(均P>0.05),M1和M3組小鼠較對照組錶現齣對新環境探索減少的SZ陰性癥狀;大腦胼胝體區MBP染色M1組(179±10)%、M2組(235±7)%、M3組(152±9)%小鼠較對照組(288±18)%均降低(均P<0.01),其內有髓神經纖維髓鞘齣現闆層分離、節段性脫髓鞘等病變,M3組小鼠胼胝體內損傷有髓神經纖維比例高于對照組[(22.42±4.24)%vs.(3.84±1.35)%],差異有統計學意義(P<0.01)。結論胼胝體脫髓鞘改變可能是MK-801慢性給藥誘導SZ的病因之一。
목적:탐토백질/수초손상재N-갑기-D-천동안산(N-methyl-D aspartate,NMDA)수체조단치정신분렬증(schizophrenia,SZ)중적작용。방법웅성C57 BL/6J소서(8주령)48지,수궤분위지탁서평마래산염(dizocilpine, MK-801)만성급약M1조(0.25mg/kg)、M2조(0.50mg/kg)화M3조(1.00mg/kg)급대조조(생리염수)。이Morris수미궁、탐공화전봉측시검험소서행위학개변,운용면역조화、투사전경급체시학방법관찰기변지체내수초적개변。결과각모형조소서여대조조비교,공간학습기억능력무명현하강(균P>0.05),M1화M3조소서교대조조표현출대신배경탐색감소적SZ음성증상;대뇌변지체구MBP염색M1조(179±10)%、M2조(235±7)%、M3조(152±9)%소서교대조조(288±18)%균강저(균P<0.01),기내유수신경섬유수초출현판층분리、절단성탈수초등병변,M3조소서변지체내손상유수신경섬유비례고우대조조[(22.42±4.24)%vs.(3.84±1.35)%],차이유통계학의의(P<0.01)。결론변지체탈수초개변가능시MK-801만성급약유도SZ적병인지일。
Objective To explore the role of white matter injuries in the schizophrenia induced by the NMDA re-ceptor antagonist. Methods Adult male C57BL/6J mice (8 week old) were equally divided into four groups. One group was sub-chronically treated with saline solution, and the other three groups were intraperitoneally treated with MK-801 at dose of 0.025 mg/mL (M1), 0.050 mg/mL (M2) and 0.100 mg/mL (M3) in a volume 10 ml per kilogram body weight. All ani-mals were tested using Morris water maze at the 9th-15th day and using the Hole Board exploration as well as Rota Rod performance tests on the 16th day. The myelin basic protein (MBP) and the ultrastructure of the myelin sheaths in the cor-pus callosum were then examined using immunohistochemical methods, transmission electron microscope technique and stereological methods. Results The repeated sub-chronic MK-801 treatment did not induce impairment of spatial learning and memory in Morris water maze. The MK-801 treatment at 0.25 mg/kg and 1.00 mg/kg but not at 0.50 mg/kg resulted in less exploration to a new environment. The myelin staining with anti-MBP antibody was less intense in all three schizo-phrenic groups when compared to saline control group (P<0.01). Furthermore, MK-801 treatment caused pathological al-terations of the myelin sheaths including segmental demyelination of myelinated fibers and splitting of myelin sheath lamel- lae in schizophrenic groups. The ratio of the injured myelinated nerve fibers in the corpus callosum of MK-801 treated mice [M3 group, (22.42 ± 4.24)%] was significantly higher when compared to the control mice [(3.84 ± 1.35)%,P<0.01)]. Conclusions The present study demonstrated the white matter damages, mainly low MBP expression and segmental demye-lization in the corpus callosum in the mice sub-chronic treated with MK-801, indicating that the white matter changes might be involved in the schizophrenia induced by NMDA antagonist.