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培养条件对小鼠囊胚发育程序的影响。

Effects of culture conditions on the developmental programme of mouse blastocysts.

作者信息

Sellens M H, Sherman M I

出版信息

J Embryol Exp Morphol. 1980 Apr;56:1-22.

PMID:6931183
Abstract

We have investigated the developmental potential of mouse blastocysts cultured under a variety of conditions. A number of parameters were used as criteria for development and differentiation, namely hatching of blastocysts from the zona pellucida and their adhesion to the substratum, outgrowth and polyploidization of trophoblast cells, increase in cell number, protein content, beta-glucuronidase activity, appearance of lactate dehydrogenase A subunits, plasminogen activator production, and delta 5,3 beta hydroxysteroid dehydrogenase activity. Under optimal culture conditions, embryos grew relatively rapidly and expressed all the differentiative markers for which they were tested. Under less supportive conditions, the production of the markers was usually reduced quantitatively; the expression of some markers could also be considerably delayed or even totally prevented. In fact, embryos cultured in the least nutritive medium (one designed to support development only through pre-implantation stages) appeared to be in a state of metabolic quiescence closely resembling that of blastocysts in ovariectomy-induced delay. Overall, the results of our investigations lead us to propose that the expression of each of the aforementioned markers is probably under independent control and subject to intrinsic programming. Finally, the observation that some markers are produced by embryos in suboptimal media whereas others are not, suggests that the minimum metabolic level necessary for expression varies from one marker to another.

摘要

我们研究了在各种条件下培养的小鼠囊胚的发育潜能。一些参数被用作发育和分化的标准,即囊胚从透明带孵化及其与基质的粘附、滋养层细胞的生长和多倍体化、细胞数量增加、蛋白质含量、β-葡萄糖醛酸酶活性、乳酸脱氢酶A亚基的出现、纤溶酶原激活物的产生以及δ5,3β-羟基类固醇脱氢酶活性。在最佳培养条件下,胚胎生长相对迅速,并表达了所有测试的分化标志物。在支持性较差的条件下,标志物的产生通常在数量上减少;一些标志物的表达也可能会显著延迟甚至完全被阻止。事实上,在营养最少的培养基(一种仅设计用于支持胚胎植入前阶段发育的培养基)中培养的胚胎似乎处于一种代谢静止状态,与卵巢切除诱导延迟的囊胚非常相似。总体而言,我们的研究结果使我们提出,上述每个标志物的表达可能受独立控制,并受内在编程的影响。最后,观察到一些标志物在次优培养基中的胚胎中产生,而其他标志物则不产生,这表明表达所需的最低代谢水平因标志物而异。

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