Lin Yanfeng, Page David C
Howard Hughes Medical Institute, Whitehead Institute, 9 Cambridge Center, Cambridge, MA 02142, USA.
Dev Biol. 2005 Dec 15;288(2):309-16. doi: 10.1016/j.ydbio.2005.06.032. Epub 2005 Nov 28.
Genes of the DAZ family play critical roles in germ cell development in mammals and other animals. In mice, Dazl mRNA is first observed at embryonic day 11.5 (E11.5), but previous studies using Dazl-deficient mice of mixed genetic background have largely emphasized postnatal spermatogenic defects. Using an inbred C57BL/6 background, we show that Dazl is required for embryonic development and survival of XY germ cells. By E14.5, expression of germ cell markers (Mvh, Oct4, Dppa3/Stella, GCNA and MVH protein) was reduced in XY Dazl-/- gonads. By E15.5, most remaining germ cells in XY Dazl-/- embryos exhibited apoptotic morphology, and XY Dazl-/- gonads contained increased numbers of TUNEL-positive cells. The rare XY Dazl-/- germ cells that persisted until birth maintained a nuclear morphology that resembled that of wildtype germ cells at E12.5-E13.5, a critical developmental period when XY germ cells lose pluripotency and commit to a spermatogonial fate. We propose that Dazl is required as early as E12.5-E13.5, shortly after its expression is first detected, and that inbred Dazl-/- mice of C57BL/6 background provide a reproducible standard for exploring Dazl's roles in embryonic germ cell development.
DAZ家族基因在哺乳动物和其他动物的生殖细胞发育中发挥着关键作用。在小鼠中,Dazl mRNA最早在胚胎第11.5天(E11.5)被观察到,但之前使用混合遗传背景的Dazl基因缺陷小鼠的研究主要强调出生后的生精缺陷。利用近交C57BL/6背景,我们发现Dazl是XY生殖细胞胚胎发育和存活所必需的。到E14.5时,XY Dazl-/-性腺中生殖细胞标记物(Mvh、Oct4、Dppa3/Stella、GCNA和MVH蛋白)的表达降低。到E15.5时,XY Dazl-/-胚胎中大多数剩余的生殖细胞呈现凋亡形态,并且XY Dazl-/-性腺中TUNEL阳性细胞数量增加。极少数存活到出生的XY Dazl-/-生殖细胞维持着一种核形态,类似于野生型生殖细胞在E12.5 - E13.5时的核形态,这是XY生殖细胞失去多能性并确定为精原细胞命运的关键发育时期。我们提出,早在E12.5 - E13.5,即在首次检测到其表达后不久,Dazl就是必需的,并且C57BL/6背景的近交Dazl-/-小鼠为探索Dazl在胚胎生殖细胞发育中的作用提供了一个可重复的标准。
