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Chromatin-to-nucleoprotamine transition is controlled by the histone H2B variant TH2B.

Genes & development (2013-07-26)
Emilie Montellier, Fayçal Boussouar, Sophie Rousseaux, Kai Zhang, Thierry Buchou, François Fenaille, Hitoshi Shiota, Alexandra Debernardi, Patrick Héry, Sandrine Curtet, Mahya Jamshidikia, Sophie Barral, Hélène Holota, Aurélie Bergon, Fabrice Lopez, Philippe Guardiola, Karin Pernet, Jean Imbert, Carlo Petosa, Minjia Tan, Yingming Zhao, Matthieu Gérard, Saadi Khochbin
RESUMEN

The conversion of male germ cell chromatin to a nucleoprotamine structure is fundamental to the life cycle, yet the underlying molecular details remain obscure. Here we show that an essential step is the genome-wide incorporation of TH2B, a histone H2B variant of hitherto unknown function. Using mouse models in which TH2B is depleted or C-terminally modified, we show that TH2B directs the final transformation of dissociating nucleosomes into protamine-packed structures. Depletion of TH2B induces compensatory mechanisms that permit histone removal by up-regulating H2B and programming nucleosome instability through targeted histone modifications, including lysine crotonylation and arginine methylation. Furthermore, after fertilization, TH2B reassembles onto the male genome during protamine-to-histone exchange. Thus, TH2B is a unique histone variant that plays a key role in the histone-to-protamine packing of the male genome and guides genome-wide chromatin transitions that both precede and follow transmission of the male genome to the egg.

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Anti-β-actina monoclonal antibody produced in mouse, clone AC-15, ascites fluid
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ReBlot Plus Kit
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Anti-Histone H2B Antibody, Upstate®, from rabbit