一种源自患者的新型 RyR1 突变会损害小鼠的肌肉功能和钙稳态。

IF 3.3 2区 医学 Q1 PHYSIOLOGY Journal of General Physiology Pub Date : 2024-04-01 Epub Date: 2024-03-04 DOI:10.1085/jgp.202313486
Sofia Benucci, Alexis Ruiz, Martina Franchini, Lucia Ruggiero, Dario Zoppi, Rebecca Sitsapesan, Chris Lindsay, Pawel Pelczar, Laura Pietrangelo, Feliciano Protasi, Susan Treves, Francesco Zorzato
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引用次数: 0

摘要

RYR1 是与先天性肌病相关的最常见的突变基因,先天性肌病是一组严重程度不一的早发性神经肌肉疾病。一些显性 RYR1 基因突变的功能效应已被证实;然而,对于隐性突变,这些效应可能取决于多种因素,如低常等位基因的形成,或取决于它们是同卵还是复合杂合。在这里,我们从功能上描述了一种新的转基因小鼠模型,该模型敲入了在一名早产且四肢活动受限的严重患儿身上发现的突变基因。该患儿携带同型c.14928C>G RYR1突变,导致p.F4976L置换。体内和体外试验显示,与 WT 或杂合子同窝鼠相比,同合子小鼠疲劳更早,肌肉产生的力量明显更小。电子显微镜、生物化学和生理学分析表明,RyR1 p.F4976L同源小鼠的肌肉具有以下特性:(1)含有较少的钙释放单位,并出现肌纤维变性区域;(2)含有较少的RyR1蛋白;(3)纤维显示较小的电诱发钙瞬态;(4)其SR具有较小的钙储存。此外,单通道记录表明,RyR1 p.F4976L 在 100 μM [Ca2+]存在下表现出更高的 Po 值。我们的小鼠模型部分再现了人类同基因突变患者的临床表现,并为了解该突变的功能性影响提供了重要依据。这些结果将有助于理解具有类似 RYR1 突变的患者的病理。
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A novel, patient-derived RyR1 mutation impairs muscle function and calcium homeostasis in mice.

RYR1 is the most commonly mutated gene associated with congenital myopathies, a group of early-onset neuromuscular conditions of variable severity. The functional effects of a number of dominant RYR1 mutations have been established; however, for recessive mutations, these effects may depend on multiple factors, such as the formation of a hypomorphic allele, or on whether they are homozygous or compound heterozygous. Here, we functionally characterize a new transgenic mouse model knocked-in for mutations identified in a severely affected child born preterm and presenting limited limb movement. The child carried the homozygous c.14928C>G RYR1 mutation, resulting in the p.F4976L substitution. In vivo and ex vivo assays revealed that homozygous mice fatigued sooner and their muscles generated significantly less force compared with their WT or heterozygous littermates. Electron microscopy, biochemical, and physiological analyses showed that muscles from RyR1 p.F4976L homozygous mice have the following properties: (1) contain fewer calcium release units and show areas of myofibrillar degeneration, (2) contain less RyR1 protein, (3) fibers show smaller electrically evoked calcium transients, and (4) their SR has smaller calcium stores. In addition, single-channel recordings indicate that RyR1 p.F4976L exhibits higher Po in the presence of 100 μM [Ca2+]. Our mouse model partly recapitulates the clinical picture of the homozygous human patient and provides significant insight into the functional impact of this mutation. These results will help understand the pathology of patients with similar RYR1 mutations.

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来源期刊
CiteScore
6.00
自引率
10.50%
发文量
88
审稿时长
6-12 weeks
期刊介绍: General physiology is the study of biological mechanisms through analytical investigations, which decipher the molecular and cellular mechanisms underlying biological function at all levels of organization. The mission of Journal of General Physiology (JGP) is to publish mechanistic and quantitative molecular and cellular physiology of the highest quality, to provide a best-in-class author experience, and to nurture future generations of independent researchers. The major emphasis is on physiological problems at the cellular and molecular level.
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