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KMID : 1005220080230020067
Journal of Embryo Transfer
2008 Volume.23 No. 2 p.67 ~ p.76
Factors Affecting the Efficiency of Animal Cloning by Somatic Cell Nuclear Transfer
Kim Min-Goo

Park Chi-Hun
Seo Hee-Won
Choi Yo-Han
Lee Chang-Kyu
Ka Hak-Hyun
Lee Sang-Goo
Lee Chang-Kyu
Park Chi-Hun
Lee Sang-Goo
Seo Hee-Won
Choi Yo-Han
Ka Hak-Hyun
Abstract
Since the birth of Dolly using fully differentiated somatic cells as a nuclear donor, viable clones were generated successfully in many mammalian species. These achievements in animal cloning demonstrate developmental potential of terminally differentiated somatic cells. At the same time, the somatic cell nuclear transfer (SCNT) technique provides the opportunities to study basic and applied biosciences. However, the efficiency generating viable offsprings by SCNT remains extremely low. There are several explanations why cloned embryos cannot fully develop into viable animals and what factors affect developmental potency of reconstructed embryos by the SCNT technique. The most critical and persuasive explanation for inefficiency in SCNT cloning is incomplete genomic reprogramming, such as DNA methylation and histone modification. Numerous studies on genomic reprogramming demonstrated that incorrect DNA methylation and aberrant epigenetic reprogramming are considerably correlated with abnormal development of SCNT cloned embryos even though its mechanism is not fully understood. The SCNT technique is useful in cloning farm animals because pluripotent stem cells are not established in farm animal species. Therapeutic cloning combined with genetic manipulation will help to control various human diseases. Also, the SCNT technique provides a chance to overcome excessive demand for the organs by production of transgenic animals as xenotransplantation resources. Here, we describe the factors affecting the efficiency of generating cloned farm animals by the SCNT technique and discuss future directions of animal cloning by SCNT to improve the cloning efficiency.
KEYWORD
animal, cloning, somatic cell nuclear transfer, DNA methylation, epigenetic reprogramming
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