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日本犬X连锁型肌营养不良症(CXMDJ)的主要临床和组织病理学特征

Major clinical and histopathological characteristics of canine X-linked muscular dystrophy in Japan, CXMDJ.

作者信息

Shimatsu Yoshiki, Yoshimura Madoka, Yuasa Katsutoshi, Urasawa Nobuyuki, Tomohiro Masayuki, Nakura Masao, Tanigawa Manabu, Nakamura Akinori, Takeda Shin'ichi

机构信息

Department of Molecular Therapy, National Institute of Neuroscience, National Center of Neurology and Psychiatry, Kodaira, Tokyo, Japan.

出版信息

Acta Myol. 2005 Oct;24(2):145-54.

Abstract

Canine X-linked muscular dystrophy (CXMD), which was found in a colony of golden retriever, is caused by a mutation in the dystrophin gene and it is a useful model of Duchenne muscular dystrophy (DMD). To investigate the pathogenesis and to develop therapy of DMD, we have established a beagle-based CXMD colony in Japan (CXMDJ) and examined their phenotypes. The mortality by 3 days of age in the third generation (G3) of CXMDJ dogs, 32.3%, was considerably higher than that in normal G3 littermates, 13.3%. Serum creatine kinase (CK) levels of G3 CXMDJ were significantly higher than that of normal male dogs with two peaks: at shortly after birth and around 2 months of age. Diaphragm muscle involvement occurred shortly after birth and was more severe than that of limb muscles. Stress during whelping might be associated with the neonatal death and respiratory muscle involvement. Gait disturbance was also noticed after 2 months of age. The involvement of limb and temporal muscles was observed from 2 months of age, which corresponded with the second peak of serum CK. Macroglossia, dysphagia, drooling and jaw joint contracture were overt from 4 months of age. We noticed severe macroglossia and hypertrophy of the sublingual muscles at the age of 12 months, and these were important features of this model, because dysphagia is one of major symptoms in older DMD patients. Overall, the phenotypes of CXMDJ were roughly identical to those of CXMD dogs in the literature. Beagle-based CXMDJ is smaller and easier to handle than golden retriever, therefore they are a useful model for DMD.

摘要

犬X连锁肌营养不良(CXMD)在一群金毛猎犬中被发现,它由肌营养不良蛋白基因突变引起,是杜氏肌营养不良(DMD)的一个有用模型。为了研究DMD的发病机制并开发治疗方法,我们在日本建立了一个基于比格犬的CXMD群体(CXMDJ)并检查了它们的表型。CXMDJ犬第三代(G3)在3日龄时的死亡率为32.3%,显著高于正常G3同窝仔犬的13.3%。G3 CXMDJ的血清肌酸激酶(CK)水平显著高于正常雄性犬,有两个峰值:出生后不久和2个月龄左右。膈肌受累在出生后不久就出现,且比肢体肌肉更严重。分娩时的应激可能与新生儿死亡和呼吸肌受累有关。2个月龄后也注意到步态障碍。从2个月龄开始观察到肢体和颞肌受累,这与血清CK的第二个峰值相对应。4个月龄时出现巨舌、吞咽困难、流涎和下颌关节挛缩。我们在12个月龄时注意到严重的巨舌和舌下肌肥大,这些是该模型的重要特征,因为吞咽困难是老年DMD患者的主要症状之一。总体而言,CXMDJ的表型与文献中CXMD犬的表型大致相同。基于比格犬的CXMDJ比金毛猎犬体型更小且更易于处理,因此它们是DMD的一个有用模型。

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