Lee C C, Surtees R, Duchen L W
Department of Neuropathology, Institute of Neurology, London, UK.
Brain. 1992 Jun;115 ( Pt 3):935-55. doi: 10.1093/brain/115.3.935.
Cycloleucine (CL), an inhibitor of methionine adenosyltransferase, has previously been used to produce an experimental model of subacute combined degeneration of the spinal cord. A re-investigation of its effects on the morphology of the nervous system and on brain concentrations of methionine and S-adenosylmethionine (SAM) was undertaken. Cycloleucine was administered as a single dose intraperitoneally (2 mg/g body weight) to young mice aged 21 d and adults aged 6 or 10 wks. The 21-day-old mice showed clinical evidence of toxicity within 24 h and thereafter developed progressive muscle weakness and ataxia. Animals did not survive longer than 1 wk. Light and electron microscopic examination of the central and peripheral nervous systems showed that intramyelinic vacuolation developed in the white matter of brain and cord within 12 h. The intramyelinic vacuolation in the white matter of brain and cord became more severe with longer survival, vacuoles coalescing and secondary axonal degeneration becoming evident. There was no myelin vacuolation in peripheral nerves. Axonal lesions occurred in the distal parts of motor nerves within 12-24 h resulting in degeneration of intramuscular nerve fibres and terminals. Later there was evidence of axonal degeneration in tibial and sciatic nerves. Many dorsal root ganglion cells became vacuolated or necrotic and numerous degenerated fibres were noted in the white matter of the spinal cord, particularly in the gracile funiculus. The optic nerves were not affected at any stage. In adult mice the pathology consisted of distal motor axonal degeneration which developed at 1-2 d. Little or no intramyelinic vacuolation in white matter was noted. Brain concentrations of SAM were reduced and levels of methionine became greatly elevated. The morphological effects of CL are considered to be the result of SAM deficiency impairing transmethylation processes known to be important in the formation and stabilization of myelin through the methylation of myelin basic protein. The immature developing central nervous system is much more vulnerable than the fully myelinated adult brain and spinal cord. The distal, predominantly motor axonopathy is a new observation and may be a reflection of the importance of transmethylation processes in the maintenance of axonal terminal membranes and the mechanisms of release of acetylcholine at the neuromuscular junction.
环亮氨酸(CL)是蛋氨酸腺苷转移酶的抑制剂,此前已被用于建立脊髓亚急性联合变性的实验模型。我们对其对神经系统形态以及脑内蛋氨酸和S-腺苷甲硫氨酸(SAM)浓度的影响进行了重新研究。将环亮氨酸以单次腹腔注射的方式(2毫克/克体重)给予21日龄的幼鼠以及6周龄或10周龄的成年小鼠。21日龄的小鼠在24小时内出现中毒的临床症状,随后逐渐发展为进行性肌无力和共济失调。动物存活时间不超过1周。对中枢和外周神经系统进行光镜和电镜检查发现,脑和脊髓白质在12小时内出现髓鞘内空泡形成。随着存活时间延长,脑和脊髓白质中的髓鞘内空泡化变得更加严重,空泡融合,继发性轴突变性变得明显。外周神经未出现髓鞘空泡化。运动神经远端在12 - 24小时内出现轴突损伤,导致肌内神经纤维和终末变性。随后,在胫神经和坐骨神经中也有轴突变性的证据。许多背根神经节细胞出现空泡化或坏死,并且在脊髓白质中,特别是薄束中,发现大量变性纤维。视神经在任何阶段均未受影响。成年小鼠的病理变化包括在1 - 2天出现的远端运动轴突变性。白质中几乎没有或没有髓鞘内空泡化。脑内SAM浓度降低,蛋氨酸水平大幅升高。CL的形态学影响被认为是SAM缺乏损害转甲基过程的结果,已知转甲基过程通过髓鞘碱性蛋白的甲基化在髓鞘形成和稳定中起重要作用。未成熟的发育中的中枢神经系统比完全髓鞘化的成体脑和脊髓更易受损。远端主要为运动性轴索性病变是一项新的观察结果,可能反映了转甲基过程在维持轴突终末膜以及神经肌肉接头处乙酰胆碱释放机制中的重要性。
