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着床前小鼠胚胎发育过程中氨基酸转运系统b0,+和L活性的变化。

Changes in the activities of amino acid transport systems b0,+ and L during development of preimplantation mouse conceptuses.

作者信息

Van Winkle L J, Campione A L, Gorman J M, Weimer B D

机构信息

Department of Biochemistry, Chicago Osteopathic Health Systems/CCOM, Downers Grove, IL 60515.

出版信息

Biochim Biophys Acta. 1990 Jan 15;1021(1):77-84. doi: 10.1016/0005-2736(90)90387-4.

Abstract

Uptake of leucine, lysine, and arginine was predominantly Na(+)-independent in mouse conceptuses through the 8-cell stage of development, and two components of saturable transport were detected for each of these amino acids. Uptake of cationic substrates from solutions near 1 microM was inhibited most strongly by bulky cationic and zwitterionic amino acids whose carbon skeletons do not branch at the alpha or beta positions. By this criterion, system b0,+ accounted for most of the Na(+)-independent arginine and lysine transport in eggs and conceptuses throughout preimplantation development. A small, leucine-resistant, cation-preferring component of amino acid transport was also detected in these cells. Leucine uptake was inhibited most strongly by bicyclic, branched-chain or benzenoid, zwitterionic amino acids in eggs and conceptuses prior to formation of blastocysts. Therefore, it appeared to be taken up mainly by system L, while system b0,+ accounted for a smaller portion of leucine uptake during this developmental period. In blastocysts, in contrast, system L was less conspicuous, and system b0,+ was primarily responsible for Na(+)-independent leucine uptake. The Vmax values for transport of amino acids by system b0,+ increased by up to 30-fold in conceptuses between the 1-cell and blastocyst stages. In contrast, the Vmax value for leucine transport via system L decreased while the Km value increased between these two developmental stages. Although several explanations for these changes are possible, we favor the hypothesis that the density of system L transport sites in plasma membranes decreases while the number of system b0,+ sites increases during development of blastocysts from 1-cell conceptuses.

摘要

在小鼠胚胎发育到8细胞阶段之前,亮氨酸、赖氨酸和精氨酸的摄取主要不依赖于Na⁺,并且针对每种氨基酸都检测到了两个可饱和转运成分。从接近1微摩尔的溶液中摄取阳离子底物,受到碳骨架在α或β位不分支的大体积阳离子和两性离子氨基酸的最强抑制。根据这一标准,在整个着床前发育过程中,系统b0,+占卵子和胚胎中大部分不依赖于Na⁺的精氨酸和赖氨酸转运。在这些细胞中还检测到了一种小的、对亮氨酸有抗性、偏好阳离子的氨基酸转运成分。在囊胚形成之前,卵子和胚胎中的亮氨酸摄取受到双环、支链或苯环类两性离子氨基酸的最强抑制。因此,它似乎主要通过系统L摄取,而在这个发育阶段,系统b0,+占亮氨酸摄取的比例较小。相比之下,在囊胚中,系统L不太明显,系统b0,+主要负责不依赖于Na⁺的亮氨酸摄取。在1细胞和囊胚阶段之间的胚胎中,系统b0,+转运氨基酸的Vmax值增加了高达30倍。相比之下,在这两个发育阶段之间,通过系统L转运亮氨酸的Vmax值下降,而Km值增加。尽管对这些变化有几种可能解释,但我们倾向于这样的假设:在从1细胞胚胎发育成囊胚的过程中,质膜中系统L转运位点的密度降低,而系统b0,+位点的数量增加。

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