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Literature DB >> 15610612

Rapid construction of capsid-modified adenoviral vectors through bacteriophage lambda Red recombination.

Abstract

There are extensive efforts to develop cell-targeting adenoviral vectors for gene therapy wherein endogenous cell-binding ligands are ablated and exogenous ligands are introduced by genetic means. Although current approaches can genetically manipulate the capsid genes of adenoviral vectors, these approaches can be time-consuming and require multiple steps to produce a modified viral genome. We present here the use of the bacteriophage lambda Red recombination system as a valuable tool for the easy and rapid construction of capsid-modified adenoviral genomes.

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Year: 2004 PMID： 15610612 DOI： 10.1089/hum.2004.15.1125

Source DB: PubMed Journal: Hum Gene Ther ISSN： 1043-0342 Impact factor: 5.695

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Cited

23 in total

1. Open reading frame E3-10.9K of subspecies B1 human adenoviruses encodes a family of late orthologous proteins that vary in their predicted structural features and subcellular localization.

Authors: Kathryn M Frietze; Samuel K Campos; Adriana E Kajon
Journal: J Virol Date: 2010-08-25 Impact factor: 5.103

2. Real-time monitoring of NKCC2 endocytosis by total internal reflection fluorescence (TIRF) microscopy.

Authors: Ankita Bachhawat Jaykumar; Paulo S Caceres; Ibrahim Sablaban; Bakhos A Tannous; Pablo A Ortiz
Journal: Am J Physiol Renal Physiol Date: 2015-11-04

3. Selection of muscle-binding peptides from context-specific peptide-presenting phage libraries for adenoviral vector targeting.

Authors: Debadyuti Ghosh; Michael A Barry
Journal: J Virol Date: 2005-11 Impact factor: 5.103

Rapid construction of capsid-modified adenoviral vectors through bacteriophage lambda Red recombination.

1. Open reading frame E3-10.9K of subspecies B1 human adenoviruses encodes a family of late orthologous proteins that vary in their predicted structural features and subcellular localization.

2. Real-time monitoring of NKCC2 endocytosis by total internal reflection fluorescence (TIRF) microscopy.

3. Selection of muscle-binding peptides from context-specific peptide-presenting phage libraries for adenoviral vector targeting.

4. Cryoelectron microscopy of protein IX-modified adenoviruses suggests a new position for the C terminus of protein IX.

5. Metabolic biotinylation of recombinant antibody by biotin ligase retained in the endoplasmic reticulum.

Review 6. Current advances and future challenges in Adenoviral vector biology and targeting.

7. Mucosal vaccination by adenoviruses displaying reovirus sigma 1.

8. Coagulation factor X shields adenovirus type 5 from attack by natural antibodies and complement.

9. IIIa deleted adenovirus as a single-cycle genome replicating vector.

10. Derivation of a triple mosaic adenovirus for cancer gene therapy.