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断奶后发育对内源性 VPAC 调制 theta 爆发刺激诱导 LTP 的影响:与海马 GABA 能系统成熟的联系。

Postweaning Development Influences Endogenous VPAC Modulation of LTP Induced by Theta-Burst Stimulation: A Link to Maturation of the Hippocampal GABAergic System.

机构信息

BioISI-Biosystems & Integrative Sciences Institute, Faculdade de Ciências, Universidade de Lisboa, 1749-016 Lisbon, Portugal.

Unidade de Neurociências, Instituto de Medicina Molecular João Lobo Antunes, Faculdade de Medicina, Universidade de Lisboa, Av. Prof. Egas Moniz, 1649-028 Lisbon, Portugal.

出版信息

Biomolecules. 2024 Mar 20;14(3):379. doi: 10.3390/biom14030379.

Abstract

Long-term potentiation (LTP) induced by theta-burst stimulation (TBS) undergoes postweaning developmental changes partially linked to GABAergic circuit maturation. Endogenous vasoactive intestinal peptide (VIP) acting on its VPAC receptor strongly influences LTP induced by theta-burst stimulation (TBS), an effect dependent on GABAergic transmission. Although VPAC receptor levels are developmentally regulated during embryogenesis, their variation along postweaning development is unknown, as is the VPAC modulation of LTP or its relation to hippocampal GABAergic circuit maturation. As such, we investigated how VPAC modulation of LTP adjusts from weaning to adulthood along with GABAergic circuit maturation. As described, LTP induced by (5 bursts, 4 pulses delivered at 100 Hz) was increasingly greater from weaning to adulthood. The influence of the VPAC receptor antagonist PG 97-269 (100 nM) on TBS-induced LTP was much larger in (3-week-old) than in (6-7-week-old) or (12-week-old) rats. This effect was not associated with a developmental decrease in synaptic VPAC receptor levels. However, an increase in pre and post-synaptic GABAergic synaptic markers suggests an increase in the number of GABAergic synaptic contacts that is more prominent than the one observed in glutamatergic connections during this period. Conversely, endogenous VPAC receptor activation did not significantly influence TBS-induced LTP. VPAC receptor levels enhance pronouncedly during postweaning development, but not at synaptic sites. Given the involvement of VIP interneurons in several aspects of hippocampal-dependent learning, neurodevelopmental disorders, and epilepsy, this could provide important insights into the role of VIP modulation of hippocampal synaptic plasticity during normal and altered brain development potentially contributing to epileptogenesis.

摘要

长时程增强(LTP)由 theta 爆发刺激(TBS)诱导,其经历了与 GABA 能回路成熟相关的出生后发育变化。内源性血管活性肠肽(VIP)通过其 VPAC 受体发挥作用,强烈影响 theta 爆发刺激(TBS)诱导的 LTP,这种作用依赖于 GABA 能传递。尽管 VPAC 受体水平在胚胎发生期间受到发育调控,但它们在出生后的发育过程中的变化以及 VPAC 对 LTP 的调制或其与海马 GABA 能回路成熟的关系尚不清楚。因此,我们研究了 VPAC 对 LTP 的调制如何随着 GABA 能回路成熟从断奶到成年进行调整。如前所述,(5 个爆发,以 100 Hz 的频率传递 4 个脉冲)诱导的 LTP 从断奶到成年逐渐增加。VPAC 受体拮抗剂 PG 97-269(100 nM)对 TBS 诱导的 LTP 的影响在 (3 周龄)大鼠中比在 (6-7 周龄)或 (12 周龄)大鼠中更大。这种效应与突触 VPAC 受体水平的发育性下降无关。然而,前突触和后突触 GABA 能突触标记物的增加表明 GABA 能突触接触的数量增加,这比在此期间观察到的谷氨酸能连接更为明显。相反,内源性 VPAC 受体激活对 TBS 诱导的 LTP 没有显著影响。VPAC 受体水平在出生后发育过程中显著增强,但不在突触部位。鉴于 VIP 中间神经元参与海马依赖性学习、神经发育障碍和癫痫的多个方面,这可能为 VIP 调节海马突触可塑性在正常和改变的大脑发育中的作用提供重要见解,可能有助于癫痫发生。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/07b3/10968312/0aed458fdd00/biomolecules-14-00379-g001.jpg

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