4.5 Article

Cold shock domain family members YB-1 and MSY4 share essential functions during murine embryogenesis

Journal

MOLECULAR AND CELLULAR BIOLOGY
Volume 26, Issue 22, Pages 8410-8417

Publisher

AMER SOC MICROBIOLOGY
DOI: 10.1128/MCB.01196-06

Keywords

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Funding

  1. NHLBI NIH HHS [F32 HL077048] Funding Source: Medline
  2. NIDDK NIH HHS [R37 DK038682, DK38682, R56 DK038682] Funding Source: Medline

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Three cold shock domain (CSD) family members (YB-1, MSY2, and MSY4) exist in vertebrate species ranging from frogs to humans. YB-1 is expressed throughout embryogenesis and is ubiquitously expressed in adult animals; it protects cells from senescence during periods of proliferative stress. YB-1-deficient embryos die unexpectedly late in embryogenesis (embryonic day 18.5 [E18.5] to postnatal day 1) with a runting phenotype. We have now determined that MSY4, but not MSY2, is also expressed during embryogenesis; its abundance declines substantially from E9.5 to E17.5 and is undetectable on postnatal day I (adult mice express MSY4 in testes only). Whole-mount analysis revealed similar patterns of YB-1 and MSY4 RNA expression in E11.5 embryos. To determine whether MSY4 delays the death of YB-1-deficient embryos, we created and analyzed MSY4-deficient mice and then generated YB-1 and MSY4 double-knockout embryos. MSY4 is dispensable for normal development and survival, but the testes of adult mice have excessive spermatocyte apoptosis and seminiferous tubule degeneration. Embryos doubly deficient for YB-1 and MSY4 are severely runted and die much earlier (E8.5 to E11.5) than YB-1-deficient embryos, suggesting that MSY4 indeed shares critical cellular functions with YB-1 in the embryonic tissues where they are coexpressed.

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