5-氮杂-2'-脱氧胞苷诱导的小鼠细胞毒性和肢体减少缺陷。

Rosen Mitchell B, Chernoff Neil

U.S. Environmental Protection Agency, Office of Research and Development, National Health and Environmental Effects Research Laboratory, Reproductive Toxicology Division, Research Triangle Park, North Carolina 27711, USA.

Teratology. 2002 Apr;65(4):180-90. doi: 10.1002/tera.10029.

BACKGROUND

5-Aza-2'-deoxycytidine (dAZA), causes hindlimb phocomelia in CD-1 mice. Studies in our laboratory have examined the hypothesis that compound- induced changes in gene expression may uniquely affect hindlimb pattern formation. The present study tests the hypothesis that dAZA causes limb dysplasia by inducing cytotoxicity among rapidly proliferating cells in the limb bud mesenchyme.

METHODS

Pregnant CD-1 mice were given a teratogenic dose of dAZA (i.p.) at different times on GD 10 and fetuses evaluated for skeletal development in both sets of limbs by standard methods. Using general histology and BrdU immunohistochemistry, limb mesenchymal cell death and cell proliferation were then assessed in embryos at various times post dosing, shortly after initial limb bud outgrowth. The effect of dAZA on early limb chondrogenesis was also studied using Northern analysis of scleraxis and Alcian blue staining of whole mount limb buds.

RESULTS

Compound related hindlimb defects were not restricted to a specific set of skeletal elements but consisted of a range of temporally related limb anomalies. Modest defects of the radius were observed as well. These results are consistent with a general insult to the limb mesenchyme. Mesenchymal cell death and reduced cell proliferation were also observed in both sets of limbs. The timing and location of these effects indicate a role for cytotoxicity in the etiology of dAZA induced limb defects. These effects also agree with the greater teratogenicity of dAZA in the hindlimb because they were more pronounced in that limb. The expression of scleraxis, a marker of early chondrogenesis, was reduced 12 hr after dAZA exposure, a time coincident with maximal cell death, as was the subsequent emergence of Alcian blue stained long bone anlagen.

CONCLUSIONS

These findings support the hypothesis that cytotoxic changes in the limb bud mesenchyme during early limb outgrowth can induce the proximal limb truncations characteristic of phocomelia after dAZA administration.

背景

5-氮杂-2'-脱氧胞苷（dAZA）可导致CD-1小鼠出现后肢短肢畸形。我们实验室的研究检验了这样一种假说，即化合物诱导的基因表达变化可能会独特地影响后肢模式形成。本研究检验了另一种假说，即dAZA通过诱导肢芽间充质中快速增殖细胞的细胞毒性而导致肢体发育异常。

方法

在妊娠第10天的不同时间给怀孕的CD-1小鼠腹腔注射致畸剂量的dAZA，并通过标准方法评估两组肢体骨骼发育的胎儿情况。使用常规组织学和BrdU免疫组织化学，在给药后不同时间、最初肢芽长出后不久，对胚胎中的肢体间充质细胞死亡和细胞增殖进行评估。还使用硬骨素的Northern分析和全胚肢芽的阿尔新蓝染色研究了dAZA对早期肢体软骨形成的影响。

结果

与化合物相关的后肢缺陷并不局限于特定一组骨骼元素，而是由一系列与时间相关的肢体异常组成。还观察到了桡骨的轻度缺陷。这些结果与对肢体间充质的一般性损伤一致。在两组肢体中均观察到间充质细胞死亡和细胞增殖减少。这些效应的时间和位置表明细胞毒性在dAZA诱导的肢体缺陷病因中起作用。这些效应也与dAZA在后肢中更大的致畸性一致，因为它们在后肢中更明显。硬骨素（一种早期软骨形成的标志物）的表达在dAZA暴露后12小时降低，这与最大细胞死亡时间一致，随后出现阿尔新蓝染色的长骨原基也是如此。