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Donor cell lines considerably affect the outcome of somatic nuclear transfer in the case of bovines. | LitMetric

AI Article Synopsis

  • Different somatic cell types, especially fibroblasts, are commonly used in nuclear transfer experiments for cloning, but their effectiveness can vary based on their origin and culture conditions.
  • Previous studies have shown blastocyst rates from these experiments can be as high as 45%, prompting further investigation into why different fibroblast lines yield different developmental outcomes.
  • Findings suggest that the specific fibroblast line has a greater impact on embryo development than factors like passage number, indicating epigenetic variations in gene expression may play a crucial role in nuclear donor cell performance.

Article Abstract

Since the first successful nuclear transfer (NT) experiments were carried out, various somatic cell types have been used as donor cells for production of cloned animals. In most experiments, fibroblasts are used since they only need to be isolated and cultivated. Recently, some researchers have shown that different cell cultures from different sources possess different capacities to support preimplantation development of NT embryos. The blastocyst rates obtained in our previous studies varied and were as high as 45% in relation to the number of reconstructed embryos. This led us to question whether the origin and culture conditions of the defined male and female fibroblast lines could be responsible for the differences in developmental potency. Taking all our results into consideration, we conclude that different fibroblast lines recovered from the same tissue and cultivated under equal culture conditions could produce dramatically different blastocyst rates. The influence of cell line itself is higher than the influence of passage number. The observed effects of cell cycle stage, chromosomal aberrations, and diminished vitality are important but not sufficient to discriminate well-qualified nuclear donor cells. We speculate that some epigenetically regulated deviations in the gene expression program are responsible for these phenomena. Explanation of the underlying mechanisms should contribute to better understanding of epigenetic reprogramming and may ultimately assist reprogramming in the laboratory.

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Source
http://dx.doi.org/10.1262/jrd.18177DOI Listing

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