Department of Neurosciences, University of California, San Diego, La Jolla, CA 92093, USA.
Mol Cell Neurosci. 2012 Apr;49(4):448-55. doi: 10.1016/j.mcn.2012.02.001. Epub 2012 Feb 13.
Amyloid precursor protein (APP), the parent molecule to amyloid β peptide, is part of a larger gene family with two mammalian homologues, amyloid precursor-like protein 1 (APLP1) and amyloid precursor-like protein 2 (APLP2). Initial knock-out studies demonstrated that while single APP family gene deletions produced relatively mild phenotypes, deficiency of APLP2 and one other member of the gene family resulted in perinatal lethality, suggesting vital roles masked by functional redundancy of the other homologues. Because of the importance of APP in Alzheimer's disease, the vast majority of studies to date have concentrated on the neuronal functions of APP, leaving limited data on its homologues. APLP2 is of particular interest as it contains high sequence homology with APP, is processed similarly, is expressed in overlapping spatial and temporal patterns, and is obligatory for lethality when combined with deficiency of either APLP1 or APP but does not contain the toxic amyloid β sequence. Here we sought to test the role of APLP2 on neuronal structure and function using a combined approach involving in vitro and in vivo techniques in young and aged animals. Surprisingly, we found that unlike APP, APLP2 appears not to be essential for maintenance of dendritic structure, spine density, or synaptic function. Thus, there is clear divergence in the functional redundancy between APP and APLP2.
淀粉样前体蛋白(APP)是淀粉样β肽的母体分子,是具有两个哺乳动物同源物的较大基因家族的一部分,即淀粉样前体样蛋白 1(APLP1)和淀粉样前体样蛋白 2(APLP2)。最初的敲除研究表明,尽管单个 APP 家族基因缺失产生了相对较轻的表型,但 APLP2 和基因家族的另一个成员的缺乏导致围产期致死,这表明其他同源物的功能冗余掩盖了重要作用。由于 APP 在阿尔茨海默病中的重要性,迄今为止,绝大多数研究都集中在 APP 的神经元功能上,对其同源物的数据有限。APLP2 特别有趣,因为它与 APP 具有高度序列同源性,处理方式相似,表达模式重叠,并且与 APLP1 或 APP 的缺乏相结合时是必需的致死,但不包含有毒的淀粉样β序列。在这里,我们试图使用涉及年轻和老年动物的体外和体内技术的综合方法来测试 APLP2 对神经元结构和功能的作用。令人惊讶的是,我们发现与 APP 不同,APLP2 似乎不是维持树突结构、棘密度或突触功能所必需的。因此,APP 和 APLP2 之间的功能冗余存在明显的差异。
