Department of Pathology, Drexel University COM, 245 N 15th Street, Philadelphia, PA 19102.
J Gerontol A Biol Sci Med Sci. 2014 Apr;69(4):410-9. doi: 10.1093/gerona/glt108. Epub 2013 Jul 20.
Reduced signaling through the IGF type 1 (IGF-1) receptor increases life span in multiple invertebrate organisms. Studies on mammalian longevity suggest that reducing levels of IGF-1 may also increase life span. However, the data are conflicting and complicated by the physiology of the mammalian neuroendocrine system. We have performed life-span analysis on mice homozygous for an insertion in the Igf1 gene. These mice produce reduced levels of IGF-1 and display a phenotype consistent with a significant decrease in IGF-1. Life-span analysis was carried out at three independent locations. Although the life-span data varied between sites, the maximum life span of the IGF-1-deficient mice was significantly increased and age-specific mortality rates were reduced in the IGF-1-deficient mice; however, mean life span did not differ except at one site, where mean life span was increased in female IGF-1-deficient animals. Early life mortality was noted in one cohort of IGF-1-deficient mice. The results are consistent with a significant role for IGF-1 in the modulation of life span but contrast with the published life-span data for the hypopituitary Ames and Snell dwarf mice and growth hormone receptor null mice, indicating that a reduction in IGF-1 alone is insufficient to increase both mean and maximal life span in mice.
通过减少胰岛素样生长因子 1 型(IGF-1)受体的信号传递,可以延长多种无脊椎动物的寿命。关于哺乳动物寿命的研究表明,降低 IGF-1 水平也可能延长寿命。然而,这些数据存在矛盾,并且受到哺乳动物神经内分泌系统生理学的影响。我们对 Igf1 基因插入纯合子的小鼠进行了寿命分析。这些小鼠产生的 IGF-1 水平降低,并表现出与 IGF-1 显著减少相一致的表型。寿命分析在三个独立的地点进行。尽管寿命数据在不同地点之间存在差异,但 IGF-1 缺陷小鼠的最大寿命显著延长,并且 IGF-1 缺陷小鼠的特定年龄死亡率降低;然而,除了一个地点外,平均寿命没有差异,在这个地点,雌性 IGF-1 缺陷动物的平均寿命增加。在 IGF-1 缺陷小鼠的一个队列中观察到早期生活死亡率。这些结果表明 IGF-1 在调节寿命方面起着重要作用,但与已发表的垂体前叶功能减退的 Ames 和 Snell 矮鼠以及生长激素受体缺失小鼠的寿命数据形成对比,表明单独降低 IGF-1 不足以延长小鼠的平均和最大寿命。
