Liver specific microRNA 122 target sequences incorporated in AAV vectors efficiently inhibits transgene expression in the liver英文文献.pdfVIP
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Gene Therapy (2010), 1–8
2010 Macmillan Publishers Limited All rights reserved 0969-7128/10
/gt
ORIGINAL ARTICLE
Liver-specific microRNA-122 target sequences
incorporated in AAV vectors efficiently inhibits
transgene expression in the liver
1 1
C Qiao , Z Yuan , J Li, B He, H Zheng, C Mayer, J Li and X Xiao
Vectors based on adeno-associated virus (AAV) are effective in gene delivery in vivo. Tissue-specific gene expression is often
needed to minimize ectopic expression in unintended cells and undesirable consequences. Here, we investigated whether
incorporation of target sequences of tissue-specific microRNA (miRNA) into AAV vectors could inhibit ectopic expression in
tissues such as the liver and hematopoietic cells. First we inserted liver-specific miR-122 target sequences (miR-122T) into the
3¢-untranslated region (UTR) of a number of AAV vectors. After intravenous delivery in mice, we found that five copies of the
20mer miR-122T reduced liver expression of luciferase by 50-fold and b-galactosidase (LacZ) by 70-fold. Five copies of
miR-122T also reduced mRNA levels of a secretable protein (myostatin propeptide) from the AAV vector plasmid by 23-fold in
the liver. However, gene expression in other tissues, including the heart was not inhibited. Similarly, we inserted four copies of
miR-142-3pT or miR-142-5pT, both hematopoietic lineage-specific, into the 3¢-UTR of the AAV-luciferase vector. We wished to
see whether they could prolong transgene expression by inhibiting expression in antigen-presenting cells. However, in vivo
luciferase gene expression in major tissues declined with time, regardless of the miR-142 target sequences used. Quantitative
analysis of the vector D
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