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Sarcospan-deficient mouse as a model for clinical disorders associated with sarcospan mutations

机译:Sarcospan缺陷小鼠作为与sarcospan突变相关的临床疾病的模型

摘要

Disclosed is a transgenic knockout mouse whose genome has a homozygous disruption in its endogenous sarcospan gene, wherein the disruption prevents the synthesis of functional sarcospan in cells of the mouse. The mouse is characterized as exhibiting from 1.4 to 6.8 fold larger epididymal fat pad deposits as compared to the epididymal fat pad deposits of a wild type mouse. Methods for production of the mouse are presented. Also disclosed are cells derived from the transgenic knockout mouse. The mouse can be used in a method for identifying therapeutic agents for the treatment of an individual diagnosed with a metabolic disorder associated with a reduction or loss of expression of wild-type sarcospan. An example of such a disorder is weight gain in the individual associated with a reduction or loss of expression of wild-type sarcospan. These specific methods are also provided.
机译:公开了一种转基因敲除小鼠,其基因组在其内源性sarcospan基因中具有纯合破坏,其中所述破坏阻止了小鼠细胞中功能性sarcospan的合成。与野生型小鼠的附睾脂肪垫沉积物相比,该小鼠的特征在于表现出大1.4至6.8倍的附睾脂肪垫沉积物。提出了产生小鼠的方法。还公开了衍生自转基因敲除小鼠的细胞。所述小鼠可以用于鉴定治疗剂的方法,所述治疗剂用于治疗被诊断患有与野生型肌节表达减少或丧失相关的代谢异常的个体。这种疾病的一个例子是个体体重增加,其与野生型肌节的表达减少或丧失有关。还提供了这些特定的方法。

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