Adult neurogenesis and "immature" neurons in mammals: an evolutionary trade-off in plasticity?

IF 2.7 3区 医学 Q1 ANATOMY & MORPHOLOGY
Brain Structure & Function Pub Date : 2024-11-01 Epub Date: 2023-10-13 DOI:10.1007/s00429-023-02717-9
Luca Bonfanti, Chiara La Rosa, Marco Ghibaudi, Chet C Sherwood
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Abstract

Neuronal plasticity can vary remarkably in its form and degree across animal species. Adult neurogenesis, namely the capacity to produce new neurons from neural stem cells through adulthood, appears widespread in non-mammalian vertebrates, whereas it is reduced in mammals. A growing body of comparative studies also report variation in the occurrence and activity of neural stem cell niches between mammals, with a general trend of reduction from small-brained to large-brained species. Conversely, recent studies have shown that large-brained mammals host large amounts of neurons expressing typical markers of neurogenesis in the absence of cell division. In layer II of the cerebral cortex, populations of prenatally generated, non-dividing neurons continue to express molecules indicative of immaturity throughout life (cortical immature neurons; cINs). After remaining in a dormant state for a very long time, these cINs retain the potential of differentiating into mature neurons that integrate within the preexisting neural circuits. They are restricted to the paleocortex in small-brained rodents, while extending into the widely expanded neocortex of highly gyrencephalic, large-brained species. The current hypothesis is that these populations of non-newly generated "immature" neurons might represent a reservoir of developmentally plastic cells for mammalian species that are characterized by reduced stem cell-driven adult neurogenesis. This indicates that there may be a trade-off between various forms of plasticity that coexist during brain evolution. This balance may be necessary to maintain a "reservoir of plasticity" in brain regions that have distinct roles in species-specific socioecological adaptations, such as the neocortex and olfactory structures.

Abstract Image

哺乳动物的成年神经发生和“未成熟”神经元:可塑性的进化权衡?
神经元的可塑性在不同动物种类的形式和程度上有显著差异。成年神经发生,即成年后从神经干细胞产生新神经元的能力,在非哺乳动物脊椎动物中普遍存在,而在哺乳动物中则有所减少。越来越多的比较研究也报告了哺乳动物之间神经干细胞生态位的出现和活动的变化,从大脑较小的物种到大脑较大的物种,总体趋势是减少。相反,最近的研究表明,在没有细胞分裂的情况下,大脑较大的哺乳动物拥有大量表达典型神经发生标志物的神经元。在大脑皮层的第二层,产前产生的未分裂神经元群体在一生中继续表达表明不成熟的分子(皮层未成熟神经元;cINs)。在长期处于休眠状态后,这些cIN保留了分化为成熟神经元的潜力,这些成熟神经元整合在先前存在的神经回路中。它们仅限于大脑较小的啮齿动物的古皮层,而延伸到大脑高度回旋、大脑较大的物种的广泛扩展的新皮层。目前的假设是,这些非新产生的“未成熟”神经元群体可能代表了哺乳动物物种的发育可塑性细胞库,其特征是干细胞驱动的成年神经发生减少。这表明,在大脑进化过程中共存的各种形式的可塑性之间可能存在权衡。这种平衡对于维持大脑区域的“可塑性库”可能是必要的,这些区域在特定物种的社会生态适应中具有不同的作用,如新皮层和嗅觉结构。
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来源期刊
Brain Structure & Function
Brain Structure & Function 医学-解剖学与形态学
CiteScore
6.00
自引率
6.50%
发文量
168
审稿时长
8 months
期刊介绍: Brain Structure & Function publishes research that provides insight into brain structure−function relationships. Studies published here integrate data spanning from molecular, cellular, developmental, and systems architecture to the neuroanatomy of behavior and cognitive functions. Manuscripts with focus on the spinal cord or the peripheral nervous system are not accepted for publication. Manuscripts with focus on diseases, animal models of diseases, or disease-related mechanisms are only considered for publication, if the findings provide novel insight into the organization and mechanisms of normal brain structure and function.
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