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首页> 外文期刊>Journal of Applied Genetics >Impact of gene therapy for canine monogenic diseases on the progress of preclinical studies
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Impact of gene therapy for canine monogenic diseases on the progress of preclinical studies

机译:基因治疗对犬一一疾病对临床前研究进展的影响

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摘要

Rapid progress in knowledge of the organization of the dog genome has facilitated the identification of the mutations responsible for numerous monogenic diseases, which usually present a breed-specific distribution. The majority of these diseases have clinical and molecular counterparts in humans. The affected dogs have thus become valuable models for preclinical studies of gene therapy for problems such as eye diseases, immunodeficiency, lysosomal storage diseases, hemophilia, and muscular dystrophy. Successful gene therapies in dogs have significantly contributed to decisions to run clinical trials for several human diseases, such as Leber's congenital amaurosis 2-LCA2 (caused by a mutation of RPE65), X-linked retinitis pigmentosa-XLRP (caused by mutation RPGR), and achromatopsia (caused by mutation of CNGB3). Promising results were also obtained for canine as follows: hemophilia (A and B), mucopolysaccharidoses (MPS I, MPS IIIB, MPS VII), leukocyte adhesion deficiency (CLAD), and muscular dystrophy (a counterpart of human Duchenne dystrophy). Present knowledge on molecular background of canine monogenic diseases and their successful gene therapies prove that dogs have an important contribution to preclinical studies.
机译:对狗基因组组织的知识的快速进展促进了对许多单一的疾病负责的突变,这通常具有特异性分布。这些疾病的大多数患有人类的临床和分子对应物。因此,受影响的犬因此成为基因治疗的临床前研究的有价值模型,诸如眼疾病,免疫缺陷,溶酶体储存疾病,血友病和肌营养不良症等问题。狗的成功基因疗法有显着促进对几种人类疾病进行临床试验的决策,例如Leber的先天性阿颈病2-LCA2(由RPE65的突变引起的),X连接的视网膜炎Pigmentosa-XLRP(由突变RPGR引起),和致瘤(由CNGB3的突变引起)。对于犬类而言,也可以如下获得有希望的结果:血友病(A和B),粘多糖(MPS I,MPS IIIB,MPS VII),白细胞粘附缺陷(包层)和肌营养不良(人杜南营养不良的对应物)。目前有关犬单一疾病的分子背景的知识及其成功的基因疗法证明狗对临床前研究具有重要贡献。

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