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In vivo engineering of lymphocytes after systemic exosome-associated AAV delivery
by
Maguire, Casey A.
, Moon, James J.
, Mingozzi, Federico
, Kleinstiver, Benjamin P.
, Meliani, Amine
, Hanlon, Killian S.
, Breuer, Cort B.
, Volak, Adrienn
, Natasan, Jeya-shree
in
42/44
/ 631/326/596/2561
/ 631/61/2300
/ Animals
/ Biochemistry, Molecular Biology
/ CD4 antigen
/ CD8 antigen
/ Clinical trials
/ Dendritic cells
/ Dependovirus - genetics
/ Exosomes - genetics
/ Gene therapy
/ Gene transfer
/ Gene Transfer Techniques
/ Genetic Engineering
/ Genetic Vectors - administration & dosage
/ Genetics
/ Genomes
/ Green Fluorescent Proteins - genetics
/ Green Fluorescent Proteins - metabolism
/ Humanities and Social Sciences
/ Immunology
/ Immunotherapy
/ Life Sciences
/ Lymphocytes
/ Lymphocytes B
/ Lymphocytes T
/ Macrophages
/ Male
/ Membrane proteins
/ Mice
/ Mice, Inbred C57BL
/ Molecular biology
/ mRNA
/ multidisciplinary
/ Science
/ Science (multidisciplinary)
/ Stem cell transplantation
/ Stem cells
/ T-Lymphocytes - cytology
/ T-Lymphocytes - metabolism
/ T-Lymphocytes - virology
/ Transduction, Genetic
/ Transgenes
/ Vectors (Biology)
2020
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In vivo engineering of lymphocytes after systemic exosome-associated AAV delivery
by
Maguire, Casey A.
, Moon, James J.
, Mingozzi, Federico
, Kleinstiver, Benjamin P.
, Meliani, Amine
, Hanlon, Killian S.
, Breuer, Cort B.
, Volak, Adrienn
, Natasan, Jeya-shree
in
42/44
/ 631/326/596/2561
/ 631/61/2300
/ Animals
/ Biochemistry, Molecular Biology
/ CD4 antigen
/ CD8 antigen
/ Clinical trials
/ Dendritic cells
/ Dependovirus - genetics
/ Exosomes - genetics
/ Gene therapy
/ Gene transfer
/ Gene Transfer Techniques
/ Genetic Engineering
/ Genetic Vectors - administration & dosage
/ Genetics
/ Genomes
/ Green Fluorescent Proteins - genetics
/ Green Fluorescent Proteins - metabolism
/ Humanities and Social Sciences
/ Immunology
/ Immunotherapy
/ Life Sciences
/ Lymphocytes
/ Lymphocytes B
/ Lymphocytes T
/ Macrophages
/ Male
/ Membrane proteins
/ Mice
/ Mice, Inbred C57BL
/ Molecular biology
/ mRNA
/ multidisciplinary
/ Science
/ Science (multidisciplinary)
/ Stem cell transplantation
/ Stem cells
/ T-Lymphocytes - cytology
/ T-Lymphocytes - metabolism
/ T-Lymphocytes - virology
/ Transduction, Genetic
/ Transgenes
/ Vectors (Biology)
2020
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In vivo engineering of lymphocytes after systemic exosome-associated AAV delivery
by
Maguire, Casey A.
, Moon, James J.
, Mingozzi, Federico
, Kleinstiver, Benjamin P.
, Meliani, Amine
, Hanlon, Killian S.
, Breuer, Cort B.
, Volak, Adrienn
, Natasan, Jeya-shree
in
42/44
/ 631/326/596/2561
/ 631/61/2300
/ Animals
/ Biochemistry, Molecular Biology
/ CD4 antigen
/ CD8 antigen
/ Clinical trials
/ Dendritic cells
/ Dependovirus - genetics
/ Exosomes - genetics
/ Gene therapy
/ Gene transfer
/ Gene Transfer Techniques
/ Genetic Engineering
/ Genetic Vectors - administration & dosage
/ Genetics
/ Genomes
/ Green Fluorescent Proteins - genetics
/ Green Fluorescent Proteins - metabolism
/ Humanities and Social Sciences
/ Immunology
/ Immunotherapy
/ Life Sciences
/ Lymphocytes
/ Lymphocytes B
/ Lymphocytes T
/ Macrophages
/ Male
/ Membrane proteins
/ Mice
/ Mice, Inbred C57BL
/ Molecular biology
/ mRNA
/ multidisciplinary
/ Science
/ Science (multidisciplinary)
/ Stem cell transplantation
/ Stem cells
/ T-Lymphocytes - cytology
/ T-Lymphocytes - metabolism
/ T-Lymphocytes - virology
/ Transduction, Genetic
/ Transgenes
/ Vectors (Biology)
2020
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In vivo engineering of lymphocytes after systemic exosome-associated AAV delivery
Journal Article
In vivo engineering of lymphocytes after systemic exosome-associated AAV delivery
2020
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Overview
Ex-vivo
gene therapy using stem cells or T cells transduced by retroviral or lentiviral vectors has shown remarkable efficacy in the treatment of immunodeficiencies and cancer. However, the process is expensive, technically challenging, and not readily scalable to large patient populations, particularly in underdeveloped parts of the world. Direct
in vivo
gene therapy would avoid these issues, and such approaches with adeno-associated virus (AAV) vectors have been shown to be safe and efficacious in clinical trials for diseases affecting differentiated tissues such as the liver and CNS. However, the ability to transduce lymphocytes with AAV
in vivo
after systemic delivery has not been carefully explored. Here, we show that both standard and exosome-associated preparations of AAV8 vectors can effectively transduce a variety of immune cell populations including CD4
+
T cells, CD8
+
T cells, B cells, macrophages, and dendritic cells after systemic delivery in mice. We provide direct evidence of T cell transduction through the detection of AAV genomes and transgene mRNA, and show that intracellular and transmembrane proteins can be expressed. These findings establish the feasibility of AAV-mediated
in vivo
gene delivery to immune cells which will facilitate both basic and applied research towards the goal of direct
in vivo
gene immunotherapies.
Publisher
Nature Publishing Group UK,Nature Publishing Group
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