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利用 Cre/lox 介导的体内嵌合体细胞消融技术生成退行性疾病的小鼠模型。

Generating mouse models of degenerative diseases using Cre/lox-mediated in vivo mosaic cell ablation.

机构信息

Department of Otology and Laryngology, Harvard Medical School, Boston, Massachusetts, USA.

出版信息

J Clin Invest. 2011 Jun;121(6):2462-9. doi: 10.1172/JCI45081. Epub 2011 May 16.

Abstract

Most degenerative diseases begin with a gradual loss of specific cell types before reaching a threshold for symptomatic onset. However, the endogenous regenerative capacities of different tissues are difficult to study, because of the limitations of models for early stages of cell loss. Therefore, we generated a transgenic mouse line (Mos-iCsp3) in which a lox-mismatched Cre/lox cassette can be activated to produce a drug-regulated dimerizable caspase-3. Tissue-restricted Cre expression yielded stochastic Casp3 expression, randomly ablating a subset of specific cell types in a defined domain. The limited and mosaic cell loss led to distinct responses in 3 different tissues targeted using respective Cre mice: reversible, impaired glucose tolerance with normoglycemia in pancreatic β cells; wound healing and irreversible hair loss in the skin; and permanent moderate deafness due to the loss of auditory hair cells in the inner ear. These mice will be important for assessing the repair capacities of tissues and the potential effectiveness of new regenerative therapies.

摘要

大多数退行性疾病在达到症状发作的阈值之前,都是从特定细胞类型的逐渐丧失开始的。然而,由于对细胞丢失早期阶段模型的限制,不同组织的内源性再生能力很难研究。因此,我们生成了一种转基因小鼠品系(Mos-iCsp3),其中lox 失配 Cre/lox 盒可被激活以产生药物调控的二聚化半胱天冬酶-3。组织特异性 Cre 表达导致 Casp3 的随机表达,随机消除特定细胞类型的一个子集在一个定义的区域。有限的和镶嵌的细胞丢失导致使用各自的 Cre 小鼠靶向的 3 种不同组织产生不同的反应:胰腺β细胞中可逆的、伴正常血糖的葡萄糖耐量受损;皮肤中的伤口愈合和不可逆的脱发;以及内耳听觉毛细胞丢失导致的永久性中度耳聋。这些小鼠对于评估组织的修复能力和新的再生治疗方法的潜在有效性将非常重要。

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