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Site-specific transfer of an intact beta-globin gene cluster through a new targeting vector
Authors:Zhou Hai-sheng  Zhao Na  Li Lei  Dong Wen-ji  Wu Xue-song  Hao De-long  Guo Zhi-chen  Xia Kun  Xia Jia-hui  Liu De-pei  Liang Chih-chuan
Institution:National Laboratory of Medical Molecular Biology, Institute of Basic Medical Sciences, Chinese Academy of Medical Sciences & Peking Union Medical College, Beijing 100005, China.
Abstract:The ideal gene-therapy vector for treating genetic disorders should deliver intact therapeutic genes and their essential regulatory elements into the specific "safe genomic site" and realize long-term, self-regulatory expression. For beta-thalassemia gene therapy, viral vectors have been broadly used, but the accompanying insertional mutation and immunogenicity remain problematic. Hence, we aimed to develop new non-viral vectors that are efficient and safe in treating diseases. As previous studies have demonstrated that physiological expression of beta-globin genes requires both a 5' locus control region and 3' specific elements, we constructed a new human chromosome-derived targeting vector to transfer the intact beta-globin gene cluster into K562 cells. The whole beta-globin gene cluster was precisely integrated into the target site and expressed in a self-regulatory pattern. The results proved that the human chromosome-derived vector was specifically targeted to the human genome and this could provide a novel platform for further gene therapy research.
Keywords:Site-specific integration  β-Thalassemia  Homologous recombination  Human β-globin gene cluster  Human chromosome-derived vector
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