Changes in intranuclear chromatin architecture induce bipolar nuclear localization of histone variant H1T2 in male haploid spermatids

Raffaella Catena, Lorenza Ronfani, Paolo Sassone-Corsi, Irwin Davidson

Research output: Contribution to journalArticle

Abstract

Spermiogenesis entails a major biochemical and morphological restructuring of the germ cell packing the DNA into the condensed spermatid nucleus. H1T2 is a histone H1 variant selectively and transiently expressed in male haploid germ cells during spermiogenesis that specifically localizes to a chromatin domain at the apical pole under the acrosome. We explored the mechanisms determining polar localization of H1T2 in spermatids. In acrosome-deficient round spermatids of hrb-/- and gopc-/- mice, H1T2 localization is not altered, indicating that proper acrosome development is not required for specifying nuclear polarity. In contrast, in late round spermatids from trf2-/- or hmgb2-/- mice, a bipolar H1T2 localization was observed revealing that polarity is modified by loss of proteins specifying chromatin architecture. Our results show that intranuclear chromatin organization is critical for correct polar localization of H1T2 and that H1T2 can be a useful molecular marker revealing chromatin disorganization in spermatids.

Original languageEnglish
Pages (from-to)231-238
Number of pages8
JournalDevelopmental Biology
Volume296
Issue number1
DOIs
Publication statusPublished - Aug 1 2006

    Fingerprint

Keywords

  • Acrosome
  • Chromocenter
  • GOPC
  • HMGB2
  • HRB
  • Spermatogenesis
  • TRF2/TLF

ASJC Scopus subject areas

  • Developmental Biology

Cite this