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[囊性纤维化的基因治疗前景]

[Gene therapy perspectives in cystic fibrosis].

作者信息

Midro A T, Kulczycki L L, Sledziewski A

机构信息

Zakład Genetyki Klinicznej Instytutu Połoznictwa i Chorób Kobiecych Akademii Medycznej, Białymstoku.

出版信息

Postepy Hig Med Dosw. 1993;47(4):221-30.

PMID:8309849
Abstract

Cystic fibrosis (CF) is a frequent autosomal recessive genetic disease. The isolation of the gene at the CF locus assigned to the long arm of chromosome 7 band q 31 and defining description of its protein named CFTR (cystic fibrosis transmembrane conductance regulator) promoted understanding the basic biochemical defect. Brief review of relevant literature demonstrates that glycoprotein CFTR is a chloride channel and is activated by a combination of phosphorylation by protein kinase A and binding of ATP. Most common mutation of CF gene, a deletion of the three nucleotides encoding phenylalanine (Delta F508) results in disturbance of chloride transport through membrane of epithelial cells involved in pathomechanism of CF. The way for gene therapy in CF is open, however therapeutic progress is noted on both pharmacologic arena and on the gene cure front. Recombinant vectors utilizing the adenovirus system with high efficiency of CFTR gene transfer to airway epithelium demonstrated in a rat model look promising. The use of retroviruses for CFTR transfer is also advanced mode of somatic gene therapy. An alternative approach suggesting the use of germ line cells is prerequisite of the development of the preimplantation/preconception genetic CF diagnosis. A number of safety and efficacy issues have to be addressed for all approaches before human trials can be implemented.

摘要

囊性纤维化(CF)是一种常见的常染色体隐性遗传病。位于7号染色体长臂q31带的CF基因座上的基因被分离出来,并对其名为CFTR(囊性纤维化跨膜传导调节因子)的蛋白质进行了明确描述,这促进了人们对基本生化缺陷的理解。对相关文献的简要回顾表明,糖蛋白CFTR是一种氯离子通道,可通过蛋白激酶A的磷酸化作用与ATP结合的共同作用而被激活。CF基因最常见的突变是编码苯丙氨酸的三个核苷酸缺失(ΔF508),这导致参与CF发病机制的上皮细胞膜上的氯离子转运受到干扰。CF的基因治疗途径已经开启,然而在药物治疗领域和基因治疗前沿都取得了治疗进展。在大鼠模型中,利用腺病毒系统将CFTR基因高效转移到气道上皮的重组载体显示出了前景。使用逆转录病毒进行CFTR转移也是体细胞基因治疗的先进模式。另一种建议使用生殖系细胞的方法是植入前/受孕前CF基因诊断发展的先决条件。在进行人体试验之前,所有方法都必须解决一些安全性和有效性问题。

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