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1. Transplacental delivery of factor IX Fc-fusion protein ameliorates bleeding phenotype of newborn hemophilia B mice.

2. Small extracellular vesicles carrying reovirus, tumor antigens, interferon-β, and damage-associated molecular patterns for efficient tumor treatment.

3. Pre-treatment of oncolytic reovirus improves tumor accumulation and intratumoral distribution of PEG-liposomes.

4. Development of an adenovirus vector lacking the expression of virus-associated RNAs.

5. An effective gene-knockdown using multiple shRNA-expressing adenovirus vectors.

6. Optimization of a microRNA expression vector for function analysis of microRNA.

7. Adenovirus serotype 35 vector-induced innate immune responses in dendritic cells derived from wild-type and human CD46-transgenic mice: Comparison with a fiber-substituted Ad vector containing fiber proteins of Ad serotype 35.

8. Prevention of hepatic ischemia-reperfusion injury by pre-administration of catalase-expressing adenovirus vectors.

9. Suppressive effects of sugar-modified cationic liposome/NF-kappaB decoy complexes on adenovirus vector-induced innate immune responses.

10. Efficient gene delivery in human and rodent mast cells using adenovirus vectors.

11. Modification of pIX or hexon based on fiberless Ad vectors is not effective for targeted Ad vectors.

12. Effective tumor targeted gene transfer using PEGylated adenovirus vector via systemic administration.

13. Efficient gene transfer into murine pancreatic islets using adenovirus vectors.

14. Comparison of gene expression efficiency and innate immune response induced by Ad vector and lipoplex.

15. The short consensus repeats 1 and 2, not the cytoplasmic domain, of human CD46 are crucial for infection of subgroup B adenovirus serotype 35.

16. Efficient regulation of gene expression using self-contained fiber-modified adenovirus vectors containing the tet-off system.

17. Effect of DNA/liposome mixing ratio on the physicochemical characteristics, cellular uptake and intracellular trafficking of plasmid DNA/cationic liposome complexes and subsequent gene expression.

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