Samuel L. Murphy scite author profile

Hepatic adeno-associated virus (AAV)-serotype 2 mediated gene transfer results in transgene product expression that is sustained in experimental animals but not in human subjects. We hypothesize that this is caused by rejection of transduced hepatocytes by AAV capsid-specific memory CD8(+) T cells reactivated by AAV vectors. Here we show that healthy subjects carry AAV capsid-specific CD8(+) T cells and that AAV-mediated gene transfer results in their expansion. No such expansion occurs in mice after AAV-mediated gene transfer. In addition, we show that AAV-2 induced human T cells proliferate upon exposure to alternate AAV serotypes, indicating that other serotypes are unlikely to evade capsid-specific immune responses.

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In vivo genome editing restores haemostasis in a mouse model of haemophilia

Haurigot

Doyon

et al. 2011

Nature

501

400

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Platelet- and megakaryocyte-derived microparticles transfer CXCR4 receptor to CXCR4-null cells and make them susceptible to infection by X4-HIV

Rozmysłowicz

Majka

Kijowski

et al. 2003

AIDS

306

250

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Capsid antigen presentation flags human hepatocytes for destruction after transduction by adeno-associated viral vectors

Pien¹,

Basner-Tschakarjan²,

Hui³

et al. 2009

J. Clin. Invest.

168

153

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Samuel L. Murphy

CD8+ T-cell responses to adeno-associated virus capsid in humans

In vivo genome editing restores haemostasis in a mouse model of haemophilia

Platelet- and megakaryocyte-derived microparticles transfer CXCR4 receptor to CXCR4-null cells and make them susceptible to infection by X4-HIV

Capsid antigen presentation flags human hepatocytes for destruction after transduction by adeno-associated viral vectors

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