Abstract
There have been major changes since the incidents of leukemia development in X-SCID patients after the treatments using retroviral gene therapy. Due to the risk of oncogenesis caused by retroviral insertional activation of host genes, most of the efforts focused on the lentiviral therapies. However, a relative clonal dominance was detected in a patient with β-thalassemia Major, two years after the subject received genetically modified hematopoietic stem cells using lentiviral vectors. This disappointing result of the recent clinical trial using lentiviral vector tells us that the current and most advanced vector systems does not have enough safety. In this review, various safety features that have been tried for the retroviral gene therapy are introduced and the possible new ways of improvements are discussed. Additional feature of chromatin insulators, co-transduction of a suicidal gene under the control of an inducible promoter, conditional expression of the transgene only in appropriate target cells, targeted transduction, cell type-specific expression, targeted local administration, splitting of the viral genome, and site specific insertion of retroviral vector are discussed here.
Highlights
Retroviral vectors have been the most preferred gene transfer systems in clinical gene therapy until the incident of a human trial for the X-linked severe combined immunodeficiency (SCID) [1,2,3]
The potential risk of insertional oncogenesis was realized in the trial, infants with X-SCID were cured by retrovirus-mediated ex-vivo gene transfer, and the trial was credited as the first unequivocal success for gene therapy [4]
Applications of gene therapy protocols have been continuously expanded to wide variety of acquired and inherited diseases, such as cancer, SCID, and other life threatening diseases
Summary
Retroviral vectors have been the most preferred gene transfer systems in clinical gene therapy until the incident of a human trial for the X-linked severe combined immunodeficiency (SCID) [1,2,3]. Clonal populations share an integration site in HMGA2 gene This incident raised a question about whether the use of lentiviral and modified SIN retroviral vectors containing insulators can decrease the risk of insertional mutagenesis in hematopoietic stem cells. Insulator containing retroviral vectors will be less prone to silencing of the transgene expression as a result of chromosome positional effect [73], and at the same time, will have less chance of causing aberrant induction of host genes near the site of incorporation as it has no viral enhancer. The proviral form of this vector does not contain HIV-1 U3 region transcriptional regulatory elements and is flanked by the enhancer-blocking -globin insulators These observations indicate that the usage of SARs in addition to insulators could significantly improve transgene expression and lower the risk of uncontrolled activation of cellular proto-oncogenes at or near the site of incorporation. Combination of a strong SA, deleting cryptic SD in the transgene [89], using an improved polyadenylation signal [90], the removal of LTR promoter, and the insulator will largely prevent the interactions of the retroviral splice donor with downstream chromosome sequences
Sign-in/Register to view highlights & summary Sign-in/Register to access full text options 
Free) 
Talk to us
Join us for a 30 min session where you can share your feedback and ask us any queries you have
Schedule a call
