Miller Martha J, Haxhiu Musa A, Georgiadis Paraskevi, Gudz Tatyana I, Kangas Cindy D, Macklin Wendy B
Department of Pediatrics, Case Western Reserve University and Rainbow Babies and Children's Hospital, Cleveland, Ohio 44106, USA.
J Neurosci. 2003 Mar 15;23(6):2265-73. doi: 10.1523/JNEUROSCI.23-06-02265.2003.
Pelizaeus Merzbacher disease is an X-linked dysmyelinating disorder of the CNS, resulting from mutations in the proteolipid protein (PLP) gene. An animal model for this disorder, the myelin-deficient (MD) rat, carries a point mutation in the PLP gene and exhibits a phenotype similar to the fatal, connatal disease, including extensive dysmyelination, tremors, ataxia, and death at approximately postnatal day 21 (P21). We postulated that early death might result from disruption of myelinated neural pathways in the caudal brainstem and altered ventilatory response to oxygen deprivation or hypercapnic stimulus. Using barometric plethysmography to measure respiratory function, we found that the MD rat develops lethal hypoxic depression of breathing at P21, but hypercapnic ventilatory response is normal. Histologic examination of the caudal brainstem in the MD rat at this age showed extensive dysmyelination and downregulation of NMDA and to a lesser extent GABA(A) receptors on neurons in the nucleus tractus solitarius, hypoglossal nucleus, and dorsal motor nucleus of the vagus. Unexpectedly, immunoreactive PLP/DM20 was detected in neurons in the caudal brainstem. Not all biosynthetic functions and structural elements were altered in these neurons, because phosphorylated and nonphosphorylated neurofilament and choline acetyltransferase expression were comparable between MD and wild-type rats. These findings suggest that PLP is expressed in neurons in the developing brainstem and that PLP gene mutation can selectively disrupt central processing of afferent neural input from peripheral chemoreceptors, leaving the central chemosensory system for hypercapnia intact.
佩利措伊斯-梅茨巴赫病是一种中枢神经系统的X连锁脱髓鞘疾病,由蛋白脂蛋白(PLP)基因突变引起。这种疾病的动物模型——髓磷脂缺陷(MD)大鼠,其PLP基因存在一个点突变,表现出与致命的先天性疾病相似的表型,包括广泛的脱髓鞘、震颤、共济失调,以及在出生后约第21天(P21)死亡。我们推测,早期死亡可能是由于延髓尾端脑干中有髓神经通路的破坏,以及对缺氧或高碳酸血症刺激的通气反应改变所致。通过使用气压体积描记法测量呼吸功能,我们发现MD大鼠在P21时会出现致命的低氧性呼吸抑制,但高碳酸通气反应正常。对这个年龄段的MD大鼠延髓尾端脑干进行组织学检查,结果显示广泛脱髓鞘,孤束核、舌下神经核和迷走神经背运动核中神经元上的NMDA受体下调,GABA(A)受体也有较小程度的下调。出乎意料的是,在延髓尾端脑干的神经元中检测到了免疫反应性PLP/DM20。这些神经元中的并非所有生物合成功能和结构成分都发生了改变,因为MD大鼠和野生型大鼠之间磷酸化和非磷酸化神经丝以及胆碱乙酰转移酶的表达相当。这些发现表明,PLP在发育中的脑干神经元中表达,并且PLP基因突变可以选择性地破坏来自外周化学感受器的传入神经输入的中枢处理过程,而使对高碳酸血症的中枢化学感受系统保持完整。