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   An update on targeted gene repair in mammalian cells: Methods and mechanisms  
   
نویسنده jensen n.m. ,dalsgaard t. ,jakobsen m. ,nielsen r.r. ,sørensen c.b. ,bolund l. ,jensen t.g.
منبع journal of biomedical science - 2011 - دوره : 18 - شماره : 1
چکیده    Transfer of full-length genes including regulatory elements has been the preferred gene therapy strategy for clinical applications. however,with significant drawbacks emerging,targeted gene alteration (tga) has recently become a promising alternative to this method. by means of tga,endogenous dna repair pathways of the cell are activated leading to specific genetic correction of single-base mutations in the genome. this strategy can be implemented using single-stranded oligodeoxyribonucleotides (ssodns),small dna fragments (sdfs),triplex-forming oligonucleotides (tfos),adeno-associated virus vectors (aavs) and zinc-finger nucleases (zfns). despite difficulties in the use of tga,including lack of knowledge on the repair mechanisms stimulated by the individual methods,the field holds great promise for the future. the objective of this review is to summarize and evaluate the different methods that exist within this particular area of human gene therapy research. © 2011 jensen et al; licensee biomed central ltd.
آدرس institute of human genetics,bartholin building,university of aarhus,8000 aarhus c, Denmark, institute of human genetics,bartholin building,university of aarhus,8000 aarhus c, Denmark, institute of human genetics,bartholin building,university of aarhus,8000 aarhus c, Denmark, institute of human genetics,bartholin building,university of aarhus,8000 aarhus c, Denmark, institute of human genetics,bartholin building,university of aarhus,8000 aarhus c, Denmark, institute of human genetics,bartholin building,university of aarhus,8000 aarhus c, Denmark, institute of human genetics,bartholin building,university of aarhus,8000 aarhus c, Denmark
 
     
   
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