Characterization of a CD46 transgenic pig and protection of transgenic kidneys against hyperacute rejection in non‐immunosuppressed baboons

Loveland, Bruce E.; Milland, Julie; Kyriakou, Peter; Thorley, Bruce R; Christiansen, Dale; Lanteri, Marc; Regensburg, Mark; Duffield, Maureen; French, Arthur B.; Williams, Lindsay; Baker, Louise; Brandon, Malcolm R.; Xing, Pei‐Xiang; Kahn, D

doi:10.1046/j.1399-3089.2003.00103_11_2.x

Cited by 109 publications

(88 citation statements)

References 29 publications

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“…Several efforts have been made to eliminate the detrimental effect of the complement cascade's activation on the xenograft, including the use of specific soluble complement inhibitors, such as soluble complement receptor type 1 (Lam et al 2005), or the cobra venom factor (Kobayashi et al 1997), and the production of animals transgenic for human complement regulatory proteins (CRP), such as hCD55, hCD46, or hCD59 (Fodor et al 1994;Cozzi and White 1995;McCurry et al 1995;Cowan et al 2000;Loveland et al 2004;Menoret et al 2004). This approach represents an elegant strategy for down-regulating local complement activation on the xenograft while preserving systemic complement activity as a first line of defense.…”

Section: Preventing the Activation Of The Complement Cascade Triggerementioning

confidence: 99%

Immunological Challenges and Therapies in Xenotransplantation

Vadori

2014

Cold Spring Harbor Perspectives in Medicine

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Section: Preventing the Activation Of The Complement Cascade Triggerementioning

confidence: 99%

Immunological Challenges and Therapies in Xenotransplantation

Vadori

2014

Cold Spring Harbor Perspectives in Medicine

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“…One pig line has however been reported as expressing abundant and ubiquitous expression of CD46, from a minigene, and this prevented hyperacute kidney rejection in non-immunosuppressed baboons for several days even without GGTA1 inactivation (Loveland et al, 2004). …”

Section: Cd46mentioning

confidence: 99%

“…The substituted CD46 cDNA sequence was used for the construction of a CD46 minigene according to Loveland et al, (2004).…”

Section: The Cd46 Minigenementioning

confidence: 99%

“…As the CD46 expression levels of the mg2 minigene were not quantified by Loveland et al, (2004), a direct comparison of expression levels is not possible.…”

Section: The Cd46 Minigenementioning

confidence: 99%

“…The transplantation of CD46 transgenic porcine kidneys into nonimmunosuppressed baboons clearly revealed a control of complement activation and an inhibition of hyperacute rejection (Loveland et al, 2004). The CD46 transgenic pigs were further modified by a homozygous GGTA1 knockout (Hara et al, 2008) and are now distributed by Revivicor Inc., Blacksburg, USA.…”

Section: The Cd46 Minigenementioning

confidence: 99%

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Multi‐transgenic pigs for xenotransplantation

Fischer

Kraner-Scheiber

Flisikowski

et al. 2013

Xenotransplantation

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Genetically modified pigs offer a solution to the severe shortage of organs available for human transplantation. Inactivation of the α1,3‐galactosyltransferase gene, responsible for α1,3‐Gal epitope synthesis (1–2) was a major breakthrough and essentially solved the problem of hyperacute rejection. However, further modifications of donor pigs are required to enable long term xenograft survival. These include expression of complement regulatory, antithrombotic, endothelium protective and immuno‐regulatory transgenes. Current evidence indicates that complement regulator transgenes, such as CD46 and CD55, must be expressed at least fivefold more than their human endogenous equivalent to effectively protect grafted tissue (3). To explore means of achieving high expression, we produced a series of BAC‐ and PAC‐vector constructs containing different sized genomic complement regulatory genes, from 70 to 190 kb, under the control of endogenous or CAGGs (CMV enhancer chicken β actin) promoter sequences. Using these vectors we obtained high levels of CD46 and CD55 expression in vitro. To prepare multi‐transgene “packages” for introduction into animals, the most effective constructs were combined with one or two further xenoprotective transgenes, including A20 (4), HO‐1 (5), thrombomodulin (6) and CTLA4‐Ig (LEA 29Y). In cotransfection experiments single cell clones expressing up to five different xenogenes could be detected. Achieving desired levels of transgene expression in an animal is not only a function of the transgene construct, but also of the location at which it integrates. Position effect variation in expression of random transgenes is well‐documented. Transgene placement by gene targeting at a permissive locus offers a useful means of achieving reliable transgene expression. In mice the ROSA26 locus is widely used to support ubiquitous expression of inserted transgenes (7–8). Murine ROSA26 encodes no functional genes and extensive gene targeting of this locus has not led to deleterious effects on development or physiology (9). To enable a similar approach in pigs, we recently identified a strong candidate for the porcine ROSA26 locus. Gene targeted placement of a neomycin reporter gene construct under the control of the ROSA26 promoter showed expression in all examined porcine tissues of all three germ layers. This strongly suggests that porcine ROSA 26 may resemble the murine locus as a suitably permissive site for transgene expression. We are currently proceeding with gene targeting to place various xenoprotective transgene constructs at this locus. References: 1. Dai Y, Vaught TD, Boone J et al. Targeted disruption of the alpha1,3‐ galactosyltransferase gene in cloned pigs. Nat Biotechnol 2002; 20: 251–255. 2. Lai L, Kolber‐Simonds D, Park K et al. Production of alpha‐1,3‐galactosyltransferase knockout pigs by nuclear transfer cloning. Science 2002; 295: 1089–1092. 3. Miyagawa S, Fukuta D, Kitano E et al. Effect of tandem forms of DAF(CD55) on complement‐mediated xenogeneic cell lysis. Xenotransplantation 20...

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Xenoimmunity

Cowan

d’Apice

2014

Textbook of Organ Transplantation

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Characterization of a CD46 transgenic pig and protection of transgenic kidneys against hyperacute rejection in non‐immunosuppressed baboons

Cited by 109 publications

References 29 publications

Immunological Challenges and Therapies in Xenotransplantation

Immunological Challenges and Therapies in Xenotransplantation

Multi‐transgenic pigs for xenotransplantation

Xenoimmunity

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