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Gq信号通路的化学遗传激活以时间和层特异性方式调节皮质神经元的树突发育。

Chemogenetic activation of Gq signaling modulates dendritic development of cortical neurons in a time- and layer-specific manner.

作者信息

Köhler Ina, Rennau Lisa Marie, Rehm Adriana, Große Julia, Gonda Steffen, Räk Andrea, Riedel Christian, Wahle Petra

机构信息

Developmental Neurobiology, Faculty of Biology and Biotechnology, Ruhr University Bochum, Bochum, Germany.

出版信息

Front Cell Neurosci. 2025 Mar 19;19:1524470. doi: 10.3389/fncel.2025.1524470. eCollection 2025.

Abstract

Designer receptors exclusively activated by designer drugs (DREADDs) are established tools for modulating neuronal activity. Calcium-mobilizing DREADD hM3Dq has been widely used to enhance neuronal activity. hM3Dq activates the Gq protein signaling cascade and mimics the action of native Gq protein-coupled receptors such as muscarinic m1 and m3 receptors leading to calcium release from intracellular storages. Depolarization evoked by increased intracellular calcium levels is an important factor for neuronal maturation. Here, we used repetitive activation of biolistically overexpressed hM3Dq to increase the activity of individual neurons differentiating in organotypic slice cultures of rat visual cortex. HM3Dq was activated by 3 μM clozapine-N-oxide (CNO) dissolved in HO. Transfectants expressing hM3Dq mock-stimulated with HO served as batch-internal controls. Pyramidal cells and multipolar interneurons were analyzed after treatment from DIV 5-10, DIV 10-20, and DIV 15-20 to investigate if Gq signaling is involved in dendritic maturation. Results show that hM3Dq activation accelerated the maturation of apical dendrites of L2/3 pyramidal cells in the early, but no longer in the later time windows. In contrast, dendritic dimensions of L5/6 pyramidal cells and interneurons were not altered at DIV 10. These findings suggest a growth-promoting role of activated Gq signaling selectively for early postnatal L2/3 pyramidal cells. Unexpectedly, hM3Dq activation from DIV 10-20 reduced the dendritic complexity of L5/6 pyramidal cells and multipolar interneurons. Together, results suggest a role of Gq signaling for neuronal differentiation and support evidence that it may also limit dendritic growth.

摘要

仅由设计药物激活的设计受体(DREADDs)是调节神经元活动的既定工具。钙动员型DREADD hM3Dq已被广泛用于增强神经元活动。hM3Dq激活Gq蛋白信号级联反应,并模拟天然Gq蛋白偶联受体(如毒蕈碱m1和m3受体)的作用,导致细胞内储存的钙释放。细胞内钙水平升高引起的去极化是神经元成熟的重要因素。在这里,我们使用生物弹道过表达的hM3Dq的重复激活来增加大鼠视觉皮质器官型切片培养中分化的单个神经元的活动。HM3Dq由溶解在HO中的3μM氯氮平 - N - 氧化物(CNO)激活。用HO模拟刺激表达hM3Dq的转染子作为批次内对照。在第5 - 10天、第10 - 20天和第15 - 20天处理后分析锥体细胞和多极中间神经元,以研究Gq信号是否参与树突成熟。结果表明,hM3Dq激活在早期加速了L2/3锥体细胞顶端树突的成熟,但在后期不再如此。相比之下,L5/6锥体细胞和中间神经元的树突尺寸在第10天没有改变。这些发现表明激活的Gq信号对出生后早期的L2/3锥体细胞具有选择性的促生长作用。出乎意料的是,从第10 - 20天激活hM3Dq会降低L5/6锥体细胞和多极中间神经元的树突复杂性。总之,结果表明Gq信号在神经元分化中起作用,并支持其也可能限制树突生长的证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5a8a/11962018/21dc789f1446/fncel-19-1524470-g001.jpg

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