Microglial Engulfment of Multisensory Terminals in the Midbrain Inferior Colliculus During an Early Critical Period

IF 2.3 4区医学 Q3 NEUROSCIENCES

Journal of Comparative Neurology Pub Date : 2025-03-02 DOI:10.1002/cne.70033

Emily R. Moran, Mark L. Gabriele

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Abstract

The lateral cortex of the inferior colliculus (LCIC) receives multisensory input arrays that preferentially target its compartmental organization. Inputs of somatosensory origin end within modular zones, while auditory inputs terminate throughout an encompassing matrix. Such discrete mapping emerges during an early postnatal critical period (birth to postnatal day 12, P12) via a process of segregation. Similar to other primitive brain maps, it appears an initial excess of connections may be pruned through a refinement process. Microglial cells (MGCs) are involved in a variety of systems in the selective removal and degradation of unnecessary contacts. Aberrations in map plasticity during early critical periods have been associated with certain neurodevelopmental conditions, including autism spectrum disorders (ASD). Despite evidence linking multisensory integration deficits with cognitive/behavioral disturbances associated with ASD, mechanisms that govern multimodal network modifications remain poorly understood. Thus, the present study combines novel tract-tracing approaches in living brain preparations and immunocytochemistry in CX3CR1-GFP knock-in mice to determine: (1) if fractalkine signaling (CX3CL1–CX3CR1) influences MGC engulfment of auditory afferents, (2) whether individual MGCs phagocytose endings of multisensory origin (auditory and somatosensory), and (3) whether consumed product is degraded via the MGC's lysosomal pathway. We demonstrate active MGC pruning of auditory endings at peak LCIC stages for projection shaping (P4, P8) that significantly decreases coincident with its critical period closure (P12). While developmentally regulated, auditory engulfment appears fractalkine signaling-independent. We also provide evidence that individual LCIC microglia engulf both auditory and somatosensory terminals that co-localize with the lysosomal marker, CD68. These results suggest a prominent role for microglia in the remodeling of early multisensory midbrain maps.

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早期关键期中脑下丘多感觉终端的小胶质细胞吞噬

下丘外侧皮层（LCIC）接收多感觉输入阵列，优先针对其室状组织。体感来源的输入终止于模块区域，而听觉输入终止于整个包围矩阵。这种离散映射通过分离过程出现在出生后早期关键时期（出生到出生后12天，P12）。与其他原始的大脑图谱类似，它似乎可以通过一个精炼过程来修剪最初多余的连接。小胶质细胞（MGCs）参与多种系统的选择性去除和降解不必要的接触。早期关键时期脑图谱可塑性的异常与某些神经发育疾病有关，包括自闭症谱系障碍（ASD）。尽管有证据表明多感觉统合缺陷与ASD相关的认知/行为障碍有关，但控制多模态网络修改的机制仍然知之甚少。因此，本研究结合了CX3CR1-GFP敲入小鼠活体脑制备和免疫细胞化学的新型通道追踪方法，以确定：(1)fractalkine信号（CX3CL1-CX3CR1）是否影响MGC对听觉传入的吞噬，(2)单个MGC是否吞噬多感觉来源的末梢（听觉和体感），以及(3)消耗的产物是否通过MGC的溶酶体途径被降解。我们发现，在LCIC的峰值阶段，听觉末梢的MGC主动修剪用于投影形成（P4, P8），在其关键期关闭时显著减少（P12）。虽然发育受到调节，但听觉吞噬似乎与fractalkine信号无关。我们还提供证据表明，单个LCIC小胶质细胞吞噬与溶酶体标记CD68共定位的听觉和体感觉终端。这些结果表明，小胶质细胞在早期多感觉中脑图谱的重塑中起着重要作用。

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来源期刊

Journal of Comparative Neurology 医学-动物学

CiteScore

5.80

自引率

8.00%

发文量

158

审稿时长

3-6 weeks

期刊介绍： Established in 1891, JCN is the oldest continually published basic neuroscience journal. Historically, as the name suggests, the journal focused on a comparison among species to uncover the intricacies of how the brain functions. In modern times, this research is called systems neuroscience where animal models are used to mimic core cognitive processes with the ultimate goal of understanding neural circuits and connections that give rise to behavioral patterns and different neural states. Research published in JCN covers all species from invertebrates to humans, and the reports inform the readers about the function and organization of nervous systems in species with an emphasis on the way that species adaptations inform about the function or organization of the nervous systems, rather than on their evolution per se. JCN publishes primary research articles and critical commentaries and review-type articles offering expert insight in to cutting edge research in the field of systems neuroscience; a complete list of contribution types is given in the Author Guidelines. For primary research contributions, only full-length investigative reports are desired; the journal does not accept short communications.