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小鼠早期胚胎中细胞骨架β-肌动蛋白和γ-肌动蛋白mRNA的定量变化以及肌节肌动蛋白基因转录本明显缺失。

Quantitative changes in cytoskeletal beta- and gamma-actin mRNAs and apparent absence of sarcomeric actin gene transcripts in early mouse embryos.

作者信息

Taylor K D, Pikó L

机构信息

Developmental Biology Laboratory, VA Medical Center, Sepulveda, California 91343.

出版信息

Mol Reprod Dev. 1990 Jun;26(2):111-21. doi: 10.1002/mrd.1080260204.

Abstract

Actin is known to be synthesized both during oogenesis and in cleavage-stage embryos in mice. Cytoskeletal beta-actin appears to be the major component, followed by gamma-actin, but the synthesis of alpha-actin has also been inferred from protein electrophoretic patterns. We have studied the expression of cytoskeletal (beta- and gamma-) and sarcomeric (alpha-cardiac and alpha-skeletal) actin genes at the level of the individual mRNAs in blot hybridization experiments using isoform-specific RNA probes. The results show that there are about 2 x 10(4) beta-actin mRNA molecules in the fully grown oocyte; this number drops to about one-half in the egg and less than one-tenth in the late two-cell embryo but increases rapidly during cleavage to about 3 x 10(5) molecules in the late blastocyst. The amount of gamma-actin mRNA is similar to that of beta-actin in oocytes and eggs but only about 40% as much in late blastocysts, indicating a differential accumulation of these mRNAs during cleavage. The developmental pattern of beta- and gamma-actin mRNA provides a striking example of the transition from maternal to embryonic control that occurs at the two-cell stage and involves the elimination of most or all of the maternal actin mRNA. There was no detectable alpha-cardiac or alpha-skeletal mRNA (i.e., less than 1,000 molecules per embryo) at any stage from oocyte to late blastocyst, suggesting that the sarcomeric actin genes are silent during preimplantation development.

摘要

已知在小鼠的卵子发生过程以及卵裂期胚胎中都会合成肌动蛋白。细胞骨架β-肌动蛋白似乎是主要成分,其次是γ-肌动蛋白,但从蛋白质电泳图谱中也推断出了α-肌动蛋白的合成。我们在印迹杂交实验中使用同工型特异性RNA探针,在单个mRNA水平上研究了细胞骨架(β-和γ-)以及肌节(α-心脏和α-骨骼肌)肌动蛋白基因的表达。结果表明,在完全成熟的卵母细胞中约有2×10⁴个β-肌动蛋白mRNA分子;这个数量在卵子中降至约一半,在晚期二细胞胚胎中则少于十分之一,但在卵裂过程中迅速增加,在晚期囊胚中达到约3×10⁵个分子。γ-肌动蛋白mRNA的量在卵母细胞和卵子中与β-肌动蛋白相似,但在晚期囊胚中仅为其约40%,表明这些mRNA在卵裂过程中存在差异积累。β-和γ-肌动蛋白mRNA的发育模式为从母源性控制向胚胎性控制的转变提供了一个显著例子,这种转变发生在二细胞阶段,涉及消除大部分或所有母源性肌动蛋白mRNA。从卵母细胞到晚期囊胚的任何阶段都未检测到α-心脏或α-骨骼肌mRNA(即每个胚胎少于1000个分子),这表明肌节肌动蛋白基因在植入前发育过程中是沉默的。

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