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淀粉样前体样蛋白2(APLP2)是阿尔茨海默病前体蛋白家族的成员之一,在小鼠分裂细胞中进行正确的基因组分离时不可或缺。

APLP2, a member of the Alzheimer precursor protein family, is required for correct genomic segregation in dividing mouse cells.

作者信息

Rassoulzadegan M, Yang Y, Cuzin F

机构信息

Unité 470 de l'Institut National de la Santé et de la Recherche Médicale, Université de Nice, 06108 Nice, France.

出版信息

EMBO J. 1998 Aug 17;17(16):4647-56. doi: 10.1093/emboj/17.16.4647.

Abstract

The mouse amyloid precursor-like protein 2 (APLP2) belongs to the Alzheimer peptide precursor family. A possible role in pre-implantation development had been suggested previously, and was investigated further by creating a large deletion in the genomic locus. While heterozygous mice developed normally, homozygous embryos were arrested before reaching the blastocyst stage. One-cell embryos which contained protein of maternal origin underwent a limited number of cleavages. The progressive disappearance of the protein at stages 4 and beyond correlated with the appearance of extensive cytopathological effects. Nuclear DNA contents of the arrested embryos departed widely from the normal 2-4C value, thus suggesting a role for the protein in replication and/or segregation of the embryonic genome. Embryonic mortality was not due to the untimely initiation of programmed cell death, and it occurred before the stage at which apoptotic cells normally appear. The same abnormal distribution of DNA contents was seen in primary cultures of Aplp2 +/- embryonic fibroblasts following transfection of an expression vector for Aplp2 antisense RNA with green fluorescent protein (GFP) expressed from a co-transfected construct. Daughter cells derived from a GFP-positive cell showed abnormal DNA contents both >4C and <2C, thus indicating a role for the protein in the mitotic segregation of the genome and establishment of the proper nuclear structure.

摘要

小鼠淀粉样前体样蛋白2(APLP2)属于阿尔茨海默肽前体家族。先前已有人提出其在植入前发育中可能发挥作用,并通过在基因组位点产生大片段缺失进行了进一步研究。杂合子小鼠发育正常,而纯合子胚胎在到达囊胚阶段之前就停滞发育。含有母源蛋白的单细胞胚胎经历了有限次数的分裂。在4期及以后阶段该蛋白的逐渐消失与广泛的细胞病理效应的出现相关。停滞胚胎的核DNA含量与正常的2-4C值相差很大,因此表明该蛋白在胚胎基因组的复制和/或分离中发挥作用。胚胎死亡并非由于程序性细胞死亡的过早启动,且发生在正常情况下凋亡细胞出现的阶段之前。在用共转染构建体表达的绿色荧光蛋白(GFP)转染Aplp2 +/-胚胎成纤维细胞的表达载体后,在原代培养物中也观察到了相同的DNA含量异常分布。源自GFP阳性细胞的子细胞显示出DNA含量异常,既有>4C的也有<2C的,因此表明该蛋白在基因组的有丝分裂分离和正确核结构的建立中发挥作用。

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