Literature DB >> 20460584

Oocyte-type linker histone B4 is required for transdifferentiation of somatic cells in vivo.

Nobuyasu Maki1, Rinako Suetsugu-Maki, Shozo Sano, Kenta Nakamura, Osamu Nishimura, Hiroshi Tarui, Katia Del Rio-Tsonis, Keita Ohsumi, Kiyokazu Agata, Panagiotis A Tsonis.   

Abstract

The ability to reprogram in vivo a somatic cell after differentiation is quite limited. One of the most impressive examples of such a process is transdifferentiation of pigmented epithelial cells (PECs) to lens cells during lens regeneration in newts. However, very little is known of the molecular events that allow newt cells to transdifferentiate. Histone B4 is an oocyte-type linker histone that replaces the somatic-type linker histone H1 during reprogramming mediated by somatic cell nuclear transfer (SCNT). We found that B4 is expressed and required during transdifferentiation of PECs. Knocking down of B4 decreased proliferation and increased apoptosis, which resulted in considerable smaller lens. Furthermore, B4 knockdown altered gene expression of key genes of lens differentiation and nearly abolished expression of gamma-crystallin. These data are the first to show expression of oocyte-type linker histone in somatic cells and its requirement in newt lens transdifferentiation and suggest that transdifferentiation in newts might share common strategies with reprogramming after SCNT.

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Year:  2010        PMID: 20460584      PMCID: PMC2923362          DOI: 10.1096/fj.10-159285

Source DB:  PubMed          Journal:  FASEB J        ISSN: 0892-6638            Impact factor:   5.191


  23 in total

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3.  Controlling gene loss of function in newts with emphasis on lens regeneration.

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Review 10.  Human regeneration: An achievable goal or a dream?

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