igf - 1信号传导及其对寿命的影响。

Martin Holzenberger
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引用次数: 14

摘要

胰岛素和胰岛素样信号调节多种动物的生存和寿命,从线虫和苍蝇到高等脊椎动物和哺乳动物。近年来,研究表明脑igf - 1受体和脑IRS2通过神经内分泌机制、能量代谢控制和改良应激抵抗来控制哺乳动物的寿命。此外,研究表明胰岛素受体底物分子在胰岛素和IGF受体的下游参与了寿命的延长。我们最近的研究表明,产后早期饮食在促生长轴的发育中起着重要作用,生长激素分泌的神经内分泌可塑性部分取决于产后营养。我们还发现,心血管和代谢疾病的患病率随着促生长功能的发展而变化。神经内分泌途径也是药物治疗的主要目标,最近有报道称,成年小鼠服用雷帕霉素确实可以延长小鼠的寿命。在人类衰老方面,新的研究发现了几个促生长轴基因是长寿的决定因素,最近的一项研究表明,胰岛素/IGF通路下游信号分子FOXO3A的变异与人类的极端长寿有关。最后,在百岁老人中发现了几种人类IGF-IR的功能突变。
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Igf-I signaling and effects on longevity.

Insulin and insulin-like signaling regulate survival and lifespan in a variety of animal species, from nematodes and flies to higher vertebrates and mammals. Recently, it was shown that brain IGF-I receptor and brain IRS2 control mammalian lifespan, and that this occurs through neuroendocrine mechanisms, control of energy metabolism and modified stress resistance. Furthermore, it was demonstrated that insulin receptor substrate molecules are implicated downstream of insulin and IGF receptors in the extension of lifespan. We showed recently that early postnatal diet plays a significant role in the development of the somatotropic axis, and that part of the neuroendocrine plasticity of growth hormone secretion depends on postnatal nutrition. We also showed that the prevalence of cardiovascular and metabolic pathologies varied with the development of somatotropic function. Neuroendocrine pathways are also prime targets for pharmacological treatments, and administration of rapamycin to adult mice has indeed recently been reported to prolong lifespan in mice. With respect to human aging, new studies identified several genes of the somatotropic axis as longevity determinants, and a recent study shows that variants of FOXO3A, downstream signaling molecule in the insulin/IGF pathway, are associated with extreme longevity in humans. Finally, several functional mutations of the human IGF-IR have been discovered in centenarians.

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