Production of gene-targeted sheep by nuclear transfer from cultured somatic cells

K. J. McCreath; J. Howcroft; K. H.S. Campbell; A. Colman; A. E. Schnleke; A. J. Kind

doi:10.1038/35016604

Production of gene-targeted sheep by nuclear transfer from cultured somatic cells

K. J. McCreath, J. Howcroft, K. H.S. Campbell, A. Colman, A. E. Schnleke, A. J. Kind

Research output: Contribution to a Journal (Peer & Non Peer) › Article › peer-review

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Abstract

It is over a decade since the first demonstration that mouse embryonic stem cells could be used to transfer a predetermined genetic modification to a whole animal. The extension of this technique to other mammalian species, particularly livestock, might bring numerous biomedical benefits, for example, ablation of xenoreactive transplantation antigens, inactivation of genes responsible for neuropathogenic disease and precise placement of transgenes designed to produce proteins for human therapy. Gene targeting has not yet been achieved in mammals other than mice, however, because functional embryonic stem cells have not been derived. Nuclear transfer from cultured somatic cells provides an alternative means of cell-mediated transgenesis. Here we describe efficient and reproducible gene targeting in fetal fibroblasts to place a therapeutic transgene at the ovine α1 (I) procollagen (COL1A1) locus and the production of live sheep by nuclear transfer.

Original language	English
Pages (from-to)	1066-1069
Number of pages	4
Journal	Nature
Volume	405
Issue number	6790
DOIs	https://doi.org/10.1038/35016604
Publication status	Published - 29 Jun 2000
Externally published	Yes

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title = "Production of gene-targeted sheep by nuclear transfer from cultured somatic cells",

abstract = "It is over a decade since the first demonstration that mouse embryonic stem cells could be used to transfer a predetermined genetic modification to a whole animal. The extension of this technique to other mammalian species, particularly livestock, might bring numerous biomedical benefits, for example, ablation of xenoreactive transplantation antigens, inactivation of genes responsible for neuropathogenic disease and precise placement of transgenes designed to produce proteins for human therapy. Gene targeting has not yet been achieved in mammals other than mice, however, because functional embryonic stem cells have not been derived. Nuclear transfer from cultured somatic cells provides an alternative means of cell-mediated transgenesis. Here we describe efficient and reproducible gene targeting in fetal fibroblasts to place a therapeutic transgene at the ovine α1 (I) procollagen (COL1A1) locus and the production of live sheep by nuclear transfer.",

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AU - McCreath, K. J.

AU - Howcroft, J.

AU - Campbell, K. H.S.

AU - Colman, A.

AU - Schnleke, A. E.

AU - Kind, A. J.

PY - 2000/6/29

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N2 - It is over a decade since the first demonstration that mouse embryonic stem cells could be used to transfer a predetermined genetic modification to a whole animal. The extension of this technique to other mammalian species, particularly livestock, might bring numerous biomedical benefits, for example, ablation of xenoreactive transplantation antigens, inactivation of genes responsible for neuropathogenic disease and precise placement of transgenes designed to produce proteins for human therapy. Gene targeting has not yet been achieved in mammals other than mice, however, because functional embryonic stem cells have not been derived. Nuclear transfer from cultured somatic cells provides an alternative means of cell-mediated transgenesis. Here we describe efficient and reproducible gene targeting in fetal fibroblasts to place a therapeutic transgene at the ovine α1 (I) procollagen (COL1A1) locus and the production of live sheep by nuclear transfer.

AB - It is over a decade since the first demonstration that mouse embryonic stem cells could be used to transfer a predetermined genetic modification to a whole animal. The extension of this technique to other mammalian species, particularly livestock, might bring numerous biomedical benefits, for example, ablation of xenoreactive transplantation antigens, inactivation of genes responsible for neuropathogenic disease and precise placement of transgenes designed to produce proteins for human therapy. Gene targeting has not yet been achieved in mammals other than mice, however, because functional embryonic stem cells have not been derived. Nuclear transfer from cultured somatic cells provides an alternative means of cell-mediated transgenesis. Here we describe efficient and reproducible gene targeting in fetal fibroblasts to place a therapeutic transgene at the ovine α1 (I) procollagen (COL1A1) locus and the production of live sheep by nuclear transfer.

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Production of gene-targeted sheep by nuclear transfer from cultured somatic cells

Abstract

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