4.8 Article

TEX14 is essential for intercellular bridges and fertility in male mice

Publisher

NATL ACAD SCIENCES
DOI: 10.1073/pnas.0505123103

Keywords

cytoplasmic bridges; knockout mouse; male infertility; male sterility; ring canals

Funding

  1. NICHD NIH HHS [HD12629, HD07495, P30 HD007495, HD44858, R03 HD047514, U54 HD012629, HD42454, U54 HD042454, U54 HD007495, R01 HD044858, T32 HD007495, P50 HD012629, HD47514] Funding Source: Medline
  2. NIGMS NIH HHS [T32GM07330, T32 GM007330] Funding Source: Medline
  3. NIMH NIH HHS [F30 MH066542, F30MH066542] Funding Source: Medline

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Cytokinesis in somatic cells concludes with the formation of a midbody, which is abscised to form individual daughter cells. In contrast, germ cell cytokinesis results in a permanent intercellular bridge connecting the daughter cells through a large cytoplasmic channel. During spermatogenesis, proposed roles for the intercellular bridge include germ cell communication, synchronization, and chromosome dosage compensation in haploid cells. Although several essential components of the midbody have recently been identified, essential components of the vertebrate germ cell intercellular bridge have until now not been described. Herein, we show that testis-ex pressed gene 14 (TEX14) is a novel protein that localizes to germ cell intercellular bridges. In the absence of TEX14, intercellular bridges are not observed by using electron microscopy and other markers. Spermatogenesis in Tex14(-/-) mice progresses through the transit amplification of diploid spermatogonia and the expression of early meiotic markers but halts before the completion of the first meiotic division. Thus, TEX14 is required for intercellular bridges in vertebrate germ cells, and these studies provide evidence that the intercellular bridge is essential for spermatogenesis and fertility.

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