Clades of Adeno-Associated Viruses Are Widely Disseminated in Human Tissues

Gao, Guangping; Vandenberghe, Luk; Alvira, Mauricio R.; Lü, You; Calcedo, Roberto; Zhou, Xiangyang; Wilson, James M.

doi:10.1128/jvi.78.12.6381-6388.2004

Cited by 880 publications

(773 citation statements)

References 21 publications

(22 reference statements)

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“…38 For generation of the targeted d-sarcoglycan vectors, we used pMT187VNSTRLPXX2, pDGDVP and pdsCMV-MLC0.26-SGCD, a derivate of pdsAAV-CMV-GFP 54 with the murine d-sarcoglycan cDNA introduced with BsrGI/NheI under the control of a MluI/HindIII fragment of the CMV-enhanced myosin light chain (CMVenhMLC) promoter. 38 For construction of control d-sarcoglycan or luciferase vectors with AAV9 capsids, we used p5E18-VD2-9 55 (kindly provided by Drs Guangping Gao and Jim Wilson) instead of pMT187VNSTRLPXX2. Transfections were performed by calcium phosphate precipitation or PolyFect Transfection Reagent (Qiagen) and vector productions were purified using an iodixanol density gradient.…”

Section: Production and Titration Of Aav Particlesmentioning

confidence: 99%

Heart-targeted adeno-associated viral vectors selected by in vivo biopanning of a random viral display peptide library

et al. 2010

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Selection of targeted vectors from virus display peptide libraries is a versatile and efficient approach to improve vector specificity and efficiency. This strategy has been used to target various cell types in vitro. Here, we report the screening of an adeno-associated virus type 2 (AAV2) display peptide library in vivo to select vectors specifically homing to heart tissue after systemic application in mice. Selected library clones indicated superior specificity of gene transfer compared with wild-type AAV2, AAV9 and a heparin binding-deficient AAV2 mutant. Such targeted vectors were able to reconstitute expression of d-sarcoglycan in the heart of adult d-sarcoglycan knockout mice after systemic gene transfer in vivo, attesting to the therapeutic potential of this approach.

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Section: Production and Titration Of Aav Particlesmentioning

confidence: 99%

Heart-targeted adeno-associated viral vectors selected by in vivo biopanning of a random viral display peptide library

et al. 2010

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“…4 Currently, 12 naturally occurring serotypes of AAV and several primate isolates have been isolated and studied as gene delivery vehicles. 5,6 Clinical trials with rAAV2 vectors have been performed in hemophilia B (factor IX deficiency) patients via intramuscular injection or by targeting the liver. 3,7 No specific side effects were observed from these trials.…”

Section: Introductionmentioning

confidence: 99%

“…In this study, we report the first descriptive analysis that follows a disease cohort longitudinally to examine NAb development and persistence in response to natural AAV exposure. Samples were assayed for NAbs directed against three different serotypes of AAV (AAV2, 5 and 8), each of which represents widely divergent clades of AAV phylogenetically, 6 and each of which has been proposed and/or tested as a potential clinical vector for gene therapy of hemophilia. 3,[23][24][25][26] …”

Section: Introductionmentioning

confidence: 99%

Neutralizing antibodies against adeno-associated virus examined prospectively in pediatric patients with hemophilia

Li¹,

Narkbunnam

Samulski³

et al. 2011

Gene Ther

186

184

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The Joint Outcome Study Investigators 7Recombinant adeno-associated virus (rAAV) is a promising gene delivery vector and has recently been used in patients with hemophilia. One limitation of AAV application is that most humans have experienced wild-type AAV serotype 2 exposure, which frequently generates neutralizing antibodies (NAbs) that may inhibit rAAV2 vector transduction. Employing alternative serotypes of rAAV vectors may circumvent this problem. We investigated the development of NAbs in early childhood by examining sera gathered prospectively from 62 children with hemophilia A, participating in a multi-institutional hemophilia clinical trial (the Joint Outcome Study). Clinical applications in hemophilia therapy have been suggested for serotypes AAV2, AAV5 and AAV8, therefore NAbs against these serotypes were serially assayed over a median follow-up of 4 years. NAbs prevalence increased during early childhood for all serotypes. NAbs against AAV2 (43.5%) were observed more frequently and at higher titers compared with both AAV5 (25.8%) and AAV8 (22.6%). NAbs against AAV5 or AAV8 were rarely observed in the absence of co-prevalent and higher titer AAV2 NAbs, suggesting that NAbs to AAV5 and AAV8 were detected following AAV2 exposure due to partial cross-reactivity of AAV2-directed NAbs. The results may guide rational design of clinical trials using alternative AAV serotypes and suggest that younger patients who are given AAV gene therapy will benefit from the lower prevalence of NAbs.

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“…Since then, several other AAV serotypes have been identified with slight variations in amino-acid capsid identity. AAV serotypes 1-8 share about 60% amino-acid capsid homology, [18][19][20][21][22] the largest amino-acid variations being concentrated to the hypervariable regions exposed on the capsid surface. 23 Variation in capsid structure affects viral tropism and expression kinetics in terms of the onset and expression levels of therapeutic genes, and the use of different serotypes may allow for a more cellspecific gene transfer.…”

Section: Introductionmentioning

confidence: 99%

Cellular tropism and transduction properties of seven adeno-associated viral vector serotypes in adult retina after intravitreal injection

et al. 2008

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Recombinant adeno-associated virus (rAAV) vectors are increasingly being used as tools for gene therapy, and clinical trials have begun in patients with genetically linked retinal disorders. Intravitreal injection is optimal for the transduction of retinal ganglion cells (RGCs), although complete selectivity has not been achieved. There may also be advantages in using intravitreal approaches for the transduction of photoreceptors. Here we compared the cellular tropism and transduction efficiency of rAAV2/1, -2/2, -2/3, -2/4, -2/5, -2/6 and -2/8 in adult rat retina after intravitreal injection. Each vector encoded green fluorescent protein (GFP), and the number, laminar distribution and morphology of transduced GFP + cells were determined using fluorescent microscopy. Assessment of transduced cell phenotype was based on cell morphology and immunohistochemistry. rAAV2/2 and rAAV2/6 transduced the greatest number of cells, whereas rAAV2/5 and rAAV2/8 were least efficient. Most vectors primarily transduced RGCs; however, rAAV2/6 had a more diverse tropism profile, with 46% identified as amacrine or bipolar cells, 23% as RGCs and 22% as Mü ller cells. Mü ller cells were also frequently transduced by rAAV2/4. The highest photoreceptor transduction was seen after intravitreal rAAV2/3 injection. These data facilitate the design and selection of rAAV vectors to target specific retinal cells, potentially leading to an improved gene therapy for various human retinal pathologies.

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Clades of Adeno-Associated Viruses Are Widely Disseminated in Human Tissues

Cited by 880 publications

References 21 publications

Heart-targeted adeno-associated viral vectors selected by in vivo biopanning of a random viral display peptide library

Heart-targeted adeno-associated viral vectors selected by in vivo biopanning of a random viral display peptide library

Neutralizing antibodies against adeno-associated virus examined prospectively in pediatric patients with hemophilia

Cellular tropism and transduction properties of seven adeno-associated viral vector serotypes in adult retina after intravitreal injection

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