Compensatory axon sprouting for very slow axonal die-back in a transgenic model of spinal muscular atrophy type III.

IF 0.8 4区工程技术 Q3 MATHEMATICS, APPLIED

Quarterly Journal of Mechanics and Applied Mathematics Pub Date : 2017-03-01 Epub Date: 2017-01-25 DOI:10.1113/JP273404

Esther Udina, Charles T Putman, Luke R Harris, Neil Tyreman, Victoria E Cook, Tessa Gordon

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引用次数: 0

Abstract

Key points: Smn^+/- transgenic mouse is a model of the mildest form of spinal muscular atrophy. Although there is a loss of spinal motoneurons in 11-month-old animals, muscular force is maintained. This maintained muscular force is mediated by reinnervation of the denervated fibres by surviving motoneurons. The spinal motoneurons in these animals do not show an increased susceptibility to death after nerve injury and they retain their regenerative capacity. We conclude that the hypothesized immaturity of the neuromuscular system in this model cannot explain the loss of motoneurons by systematic die-back.

Abstract: Spinal muscular atrophy (SMA) is a common autosomal recessive disorder in humans and is the leading genetic cause of infantile death. Patients lack the SMN1 gene with the severity of the disease depending on the number of copies of the highly homologous SMN2 gene. Although motoneuron death in the Smn^+/- transgenic mouse model of the mildest form of SMA, SMA type III, has been reported, we have used retrograde tracing of sciatic and femoral motoneurons in the hindlimb with recording of muscle and motor unit isometric forces to count the number of motoneurons with intact neuromuscular connections. Thereby, we investigated whether incomplete maturation of the neuromuscular system induced by survival motoneuron protein (SMN) defects is responsible for die-back of axons relative to survival of motoneurons. First, a reduction of ∼30% of backlabelled motoneurons began relatively late, at 11 months of age, with a significant loss of 19% at 7 months. Motor axon die-back was affirmed by motor unit number estimation. Loss of functional motor units was fully compensated by axonal sprouting to retain normal contractile force in four hindlimb muscles (three fast-twitch and one slow-twitch) innervated by branches of the sciatic nerve. Second, our evaluation of whether axotomy of motoneurons in the adult Smn^+/- transgenic mouse increases their susceptibility to cell death demonstrated that all the motoneurons survived and they sustained their capacity to regenerate their nerve fibres. It is concluded the systematic die-back of motoneurons that innervate both fast- and slow-twitch muscle fibres is not related to immaturity of the neuromuscular system in SMA.

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脊髓性肌肉萎缩症 III 型转基因模型中极慢轴突回缩的补偿性轴突萌发。

要点Smn+/- 转基因小鼠是脊髓性肌萎缩症最轻型的模型。虽然 11 个月大的小鼠会丧失脊髓运动神经元，但肌肉力量仍能保持。这种肌肉力量的维持是通过存活的运动神经元对失去神经支配的纤维进行再神经支配来实现的。这些动物的脊髓运动神经元在神经损伤后并没有表现出更高的易死性，而且它们仍具有再生能力。摘要：脊髓性肌萎缩症（SMA）是人类常见的常染色体隐性遗传疾病，也是婴儿死亡的主要遗传原因。患者缺乏 SMN1 基因，疾病的严重程度取决于高度同源的 SMN2 基因的拷贝数。虽然有报道称最轻型 SMA（SMA III 型）的 Smn+/- 转基因小鼠模型中存在运动神经元死亡，但我们利用逆行追踪后肢坐骨神经和股运动神经元并记录肌肉和运动单元等长力的方法来计算具有完整神经肌肉连接的运动神经元数量。因此，我们研究了存活运动神经元蛋白（SMN）缺陷引起的神经肌肉系统不完全成熟是否是轴突回缩而非运动神经元存活的原因。首先，背标运动神经元减少的时间相对较晚，在11个月大时减少了30%，在7个月大时显著减少了19%。运动神经元数量的估计证实了运动轴突的死亡。在坐骨神经分支支配的四块后肢肌肉（三块快肌腱肌肉和一块慢肌腱肌肉）中，功能性运动单位的缺失被轴突萌发完全补偿，从而保持了正常的收缩力。其次，我们对成年 Smn+/- 转基因小鼠运动神经元的轴突切除是否会增加它们对细胞死亡的易感性进行了评估，结果表明所有的运动神经元都存活了下来，而且它们保持了再生神经纤维的能力。结论是，支配快慢肌纤维的运动神经元的系统性死亡与 SMA 神经肌肉系统的不成熟无关。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Quarterly Journal of Mechanics and Applied Mathematics 物理-力学

CiteScore

1.90

自引率

11.10%

发文量

审稿时长

>12 weeks

期刊介绍： The Quarterly Journal of Mechanics and Applied Mathematics publishes original research articles on the application of mathematics to the field of mechanics interpreted in its widest sense. In addition to traditional areas, such as fluid and solid mechanics, the editors welcome submissions relating to any modern and emerging areas of applied mathematics.