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逆转录病毒介导的人苯丙氨酸羟化酶基因向NIH 3T3细胞和肝癌细胞的转移。

Retroviral-mediated gene transfer of human phenylalanine hydroxylase into NIH 3T3 and hepatoma cells.

作者信息

Ledley F D, Grenett H E, McGinnis-Shelnutt M, Woo S L

出版信息

Proc Natl Acad Sci U S A. 1986 Jan;83(2):409-13. doi: 10.1073/pnas.83.2.409.

Abstract

Phenylketonuria (PKU) is caused by deficiency of the hepatic enzyme phenylalanine hydroxylase (PAH). A full-length human PAH cDNA sequence has been inserted into pzip-neoSV(X), which is a retroviral vector containing the bacterial neo gene. The recombinant has been transfected into psi 2 cells, which provide synthesis of the retroviral capsid. Recombinant virus was detected in the culture medium of the transfected psi 2 cells, which is capable of transmitting the human PAH gene into mouse NIH 3T3 cells by infection leading to stable incorporation of the recombinant provirus. Infected cells express PAH mRNA, immunoreactive PAH protein, and exhibit pterin-dependent phenylalanine hydroxylase activity. The recombinant virus is also capable of infecting a mouse hepatoma cell line that does not normally synthesize PAH. PAH activity is present in the cellular extracts and the entire hydroxylation system is reconstituted in the hepatoma cells infected with the recombinant viruses. Thus, recombinant viruses containing human PAH cDNA provide a means for introducing functional PAH into mammalian cells of hepatic origin and can potentially be introduced into whole animals as a model for somatic gene therapy for PKU.

摘要

苯丙酮尿症(PKU)是由肝脏酶苯丙氨酸羟化酶(PAH)缺乏引起的。全长人PAH cDNA序列已被插入到pzip-neoSV(X)中,这是一种含有细菌新霉素基因的逆转录病毒载体。该重组体已被转染到psi 2细胞中,psi 2细胞可提供逆转录病毒衣壳的合成。在转染的psi 2细胞的培养基中检测到重组病毒,该病毒能够通过感染将人PAH基因传递到小鼠NIH 3T3细胞中,导致重组前病毒的稳定整合。受感染的细胞表达PAH mRNA、免疫反应性PAH蛋白,并表现出蝶呤依赖性苯丙氨酸羟化酶活性。重组病毒还能够感染通常不合成PAH的小鼠肝癌细胞系。细胞提取物中存在PAH活性,并且在感染重组病毒的肝癌细胞中重建了整个羟化系统。因此,含有人类PAH cDNA的重组病毒为将功能性PAH引入肝脏来源的哺乳动物细胞提供了一种手段,并且有可能作为PKU体细胞基因治疗的模型引入到整个动物体内。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0caa/322868/75aaf777c3ed/pnas00306-0219-a.jpg

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