В6。А-dysfprmd / genej小鼠作为异ferlin病的遗传模型

M. V. Korokin, E. Kuzubova, A. Radchenko, R. Deev, I. A. Yakovlev, A. Deikin, N. S. Zhunusov, A. Krayushkina, V. M. Pokrovsky, O. Puchenkova, K. Chaprov, N. V. Ekimova, S. N. Bardakov, O. N. Chernova, A. Emelin, I. S. Limaev
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引用次数: 0

摘要

这项工作的目的是对DYSF基因敲除小鼠的行为和病理形态学表型进行分析,该基因在异常蛋白病的发生和发展中起着重要的作用。材料和方法。B6。实验采用A-Dysfprmd/GeneJ (Bla/J)小鼠亚系。在研究过程中,根据以下测试确定肌肉活动:“倒网格”、“握力”、“吊线”、“负重游泳”、“立杆”。对骨骼肌(腓肠肌、胫骨肌)进行组织学和免疫荧光检查。我们评估了dysferlin蛋白的存在和分布,并描述了12周龄和24周龄小鼠骨骼肌特征的一般组织学变化。进行形态计量学分析,确定以下参数:坏死肌纤维比例;有中心核的纤维的比例;平均肌纤维直径。“握力”测试和“负重游泳”测试显示,与对照组相比,Bla/J亚系研究小鼠的前肢力量和耐力有所下降。采用“吊丝”试验和“竖杆”试验对运动性能的安全性进行了检验,实验小鼠与对照组的差异有统计学意义。在“倒网格”测试中检查的肢体运动协调性和肌肉力量在这些年龄标记中没有变化。随着年龄的增长,前肢握力下降,身体耐力下降,反映了潜在肌肉疾病的进展。骨骼肌的组织学方法显示肌病损伤模式的迹象:坏死的肌纤维,中度淋巴巨噬细胞浸润,位于中心位置的纤维比例增加,与对照组相比,平均纤维直径增加。在肌肉组织中未发现异常铁蛋白。考虑到所进行的测试结果,结果表明,Bla/J亚系小鼠缺乏Dysf-/-基因表达导致肌肉营养不良,在12周龄时开始出现表型疾病表现,并在24周龄时达到峰值。该疾病的组织病理学表型表现通常是非特异性的,与不同病患者的活体病理解剖检查数据相对应。所研究的Bla/J亚群小鼠是异铁素病的代表性模型,可用于评价治疗该疾病的新药物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
В6.А-DYSFPRMD/GENEJ MICE AS A GENETIC MODEL OF DYSFERLINOPATHY
The aim of the work was behavioral and pathomorphological phenotyping of the mice knockout for the DYSF gene, which plays an important role in the development and progression of dysferlinopathy.Materials and methods. A B6.A-Dysfprmd/GeneJ (Bla/J) mice subline was used in the work. During the study, a muscle activity was determined basing on the following tests: “Inverted grid”, “Grip strength”, “Wire Hanging”, “Weight-loaded swimming”, Vertical Pole”. Histological and immunofluorescent examinations of skeletal muscles (m. gastrocnemius, m. tibialis) were performed. The presence and distribution of the dysferlin protein was assessed, and general histological changes in the skeletal muscle characteristics of mice at the age of 12 and 24 weeks, were described. A morphometric analysis with the determination of the following parameters was performed: the proportion of necrotic muscle fibers; the proportion of fibers with centrally located nuclei; the mean muscle fiber diameter.Results. The “Grip strength” test and the “Weight-loaded swimming” test revealed a decrease in the strength of the forelimbs and endurance in the studied mice of the Bla/J subline compared to the control line. The safety of physical performance was checked using the “Wire Hanging” test and the “Vertical Pole” test, which showed a statistically significant difference between the studied mice and control. The coordination of movements and muscle strength of the limbs examined in the “Inverted Grid” test did not change in these age marks. Decreased grip strength of the forelimbs, decreased physical endurance with age, reflects the progression of the underlying muscular disease. Histological methods in the skeletal muscles revealed signs of a myopathic damage pattern: necrotic muscle fibers, moderate lympho-macrophage infiltration, an increase in the proportion of fibers with centrally located nuclei, and an increase in the average fiber diameter compared to the control. The dysferlin protein was not found out in the muscle tissues.Conclusion. Taking into account the results of the tests performed, it was shown that the absence of Dysf-/- gene expressionin Bla/J subline mice led to muscular dystrophy with the onset of the development of phenotypic disease manifestations at the age of 12 weeks and their peak at 24 weeks. Histopathological phenotypic manifestations of the disease are generally nonspecific and corresponded to the data of intravital pathoanatomical examination in diferlinopathy patients. The mice of the studied subline Bla/J are a representative model of dysferlinopathy and can be used to evaluate new therapeutic agents for the treatment of this disease.
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