AAV5–Factor VIII gene transfer in severe hemophilia A
AAV5–Factor VIII gene transfer in severe hemophilia A
BACKGROUND
Patients with hemophilia A rely on exogenous factor VIII to prevent bleeding in joints, soft tissue, and the central nervous system. Although successful gene transfer has been reported in patients with hemophilia B, the large size of the factor VIII coding region has precluded improved outcomes with gene therapy in patients with hemophilia A.
METHODS
We infused a single intravenous dose of a codon-optimized adeno-associated virus serotype 5 (AAV5) vector encoding a B-domain–deleted human factor VIII (AAV5-hFVIII-SQ) in nine men with severe hemophilia A. Participants were enrolled sequentially into one of three dose cohorts (low dose [one participant], intermediate dose [one participant], and high dose [seven participants]) and were followed through 52 weeks.
RESULTS
Factor VIII activity levels remained at 3 IU or less per deciliter in the recipients of the low or intermediate dose. In the high-dose cohort, the factor VIII activity level was more than 5 IU per deciliter between weeks 2 and 9 after gene transfer in all seven participants, and the level in six participants increased to a normal value (>50 IU per deciliter) that was maintained at 1 year after receipt of the dose. In the high-dose cohort, the median annualized bleeding rate among participants who had previously received prophylactic therapy decreased from 16 events before the study to 1 event after gene transfer, and factor VIII use for participant-reported bleeding ceased in all the participants in this cohort by week 22. The primary adverse event was an elevation in the serum alanine aminotransferase level to 1.5 times the upper limit of the normal range or less. Progression of preexisting chronic arthropathy in one participant was the only serious adverse event. No neutralizing antibodies to factor VIII were detected.
CONCLUSIONS
The infusion of AAV5-hFVIII-SQ was associated with the sustained normalization of factor VIII activity level over a period of 1 year in six of seven participants who received a high dose, with stabilization of hemostasis and a profound reduction in factor VIII use in all seven participants. In this small study, no safety events were noted, but no safety conclusions can be drawn. (Funded by BioMarin Pharmaceutical; ClinicalTrials.gov number, NCT02576795. opens in new tab; EudraCT number, 2014-003880-38. opens in new tab.)
2519-2530
Rangarajan, Savita
9a5e4c7e-55ba-4a3a-b5f6-f1e269d927c3
Walsh, Liron
e83fc2bd-7bf2-44dd-94c2-19222df49a97
Lester, Will
78e4020c-cf87-468f-9122-f7b9dc725af5
Perry, David
4391bf02-c3b7-4364-87f2-34e15657b07d
Madan, Bella
07764bfb-5273-4846-9811-2d730e72c3cf
Laffan, Michael
f22012e7-7ff1-43c2-9520-bbf020428401
Yu, Hua
39ba379e-83e9-47b7-bffa-d170cf1de9dc
Vettermann, Christian
129542c2-3917-498a-b095-86248284bdb0
Pierce, Glenn F.
fa4102f0-d5f8-465b-bb17-7b7e111225d1
Wong, Wing Y.
a2a49aed-413a-4192-b9df-b97acb4cd066
Pasi, K. John
3b81e0be-6e79-4b71-95c5-45fe04b8e6dc
28 December 2017
Rangarajan, Savita
9a5e4c7e-55ba-4a3a-b5f6-f1e269d927c3
Walsh, Liron
e83fc2bd-7bf2-44dd-94c2-19222df49a97
Lester, Will
78e4020c-cf87-468f-9122-f7b9dc725af5
Perry, David
4391bf02-c3b7-4364-87f2-34e15657b07d
Madan, Bella
07764bfb-5273-4846-9811-2d730e72c3cf
Laffan, Michael
f22012e7-7ff1-43c2-9520-bbf020428401
Yu, Hua
39ba379e-83e9-47b7-bffa-d170cf1de9dc
Vettermann, Christian
129542c2-3917-498a-b095-86248284bdb0
Pierce, Glenn F.
fa4102f0-d5f8-465b-bb17-7b7e111225d1
Wong, Wing Y.
a2a49aed-413a-4192-b9df-b97acb4cd066
Pasi, K. John
3b81e0be-6e79-4b71-95c5-45fe04b8e6dc
Rangarajan, Savita, Walsh, Liron, Lester, Will, Perry, David, Madan, Bella, Laffan, Michael, Yu, Hua, Vettermann, Christian, Pierce, Glenn F., Wong, Wing Y. and Pasi, K. John
(2017)
AAV5–Factor VIII gene transfer in severe hemophilia A.
New England Journal of Medicine, 377 (26), .
(doi:10.1056/NEJMoa1708483).
Abstract
BACKGROUND
Patients with hemophilia A rely on exogenous factor VIII to prevent bleeding in joints, soft tissue, and the central nervous system. Although successful gene transfer has been reported in patients with hemophilia B, the large size of the factor VIII coding region has precluded improved outcomes with gene therapy in patients with hemophilia A.
METHODS
We infused a single intravenous dose of a codon-optimized adeno-associated virus serotype 5 (AAV5) vector encoding a B-domain–deleted human factor VIII (AAV5-hFVIII-SQ) in nine men with severe hemophilia A. Participants were enrolled sequentially into one of three dose cohorts (low dose [one participant], intermediate dose [one participant], and high dose [seven participants]) and were followed through 52 weeks.
RESULTS
Factor VIII activity levels remained at 3 IU or less per deciliter in the recipients of the low or intermediate dose. In the high-dose cohort, the factor VIII activity level was more than 5 IU per deciliter between weeks 2 and 9 after gene transfer in all seven participants, and the level in six participants increased to a normal value (>50 IU per deciliter) that was maintained at 1 year after receipt of the dose. In the high-dose cohort, the median annualized bleeding rate among participants who had previously received prophylactic therapy decreased from 16 events before the study to 1 event after gene transfer, and factor VIII use for participant-reported bleeding ceased in all the participants in this cohort by week 22. The primary adverse event was an elevation in the serum alanine aminotransferase level to 1.5 times the upper limit of the normal range or less. Progression of preexisting chronic arthropathy in one participant was the only serious adverse event. No neutralizing antibodies to factor VIII were detected.
CONCLUSIONS
The infusion of AAV5-hFVIII-SQ was associated with the sustained normalization of factor VIII activity level over a period of 1 year in six of seven participants who received a high dose, with stabilization of hemostasis and a profound reduction in factor VIII use in all seven participants. In this small study, no safety events were noted, but no safety conclusions can be drawn. (Funded by BioMarin Pharmaceutical; ClinicalTrials.gov number, NCT02576795. opens in new tab; EudraCT number, 2014-003880-38. opens in new tab.)
This record has no associated files available for download.
More information
Accepted/In Press date: 1 April 2016
e-pub ahead of print date: 9 December 2017
Published date: 28 December 2017
Identifiers
Local EPrints ID: 442595
URI: http://eprints.soton.ac.uk/id/eprint/442595
ISSN: 0028-4793
PURE UUID: 6c294118-f893-40eb-906a-5121d41d802f
Catalogue record
Date deposited: 20 Jul 2020 16:36
Last modified: 17 Mar 2024 04:02
Export record
Altmetrics
Contributors
Author:
Liron Walsh
Author:
Will Lester
Author:
David Perry
Author:
Bella Madan
Author:
Michael Laffan
Author:
Hua Yu
Author:
Christian Vettermann
Author:
Glenn F. Pierce
Author:
Wing Y. Wong
Author:
K. John Pasi
Download statistics
Downloads from ePrints over the past year. Other digital versions may also be available to download e.g. from the publisher's website.
View more statistics