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Two populations of neurokinin 1 receptor-expressing projection neurons in lamina I of the rat spinal cord that differ in AMPA receptor subunit composition and density of excitatory synaptic input

机译:大鼠脊髓板层I中两个表达神经激肽1受体的投射神经元种群的AMPA受体亚基组成和兴奋性突触输入密度不同

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摘要

Lamina I of the spinal cord contains many projection neurons that express the neurokinin 1 receptor (NK1r). It has been reported that these cells can undergo long-term potentiation (LTP), which may result from insertion of AMPA-type glutamate receptors (AMPArs) containing GluA1 or GluA4 subunits. We therefore investigated synaptic AMPAr expression on these cells with immunocytochemistry following antigen-retrieval. We also examined their density of glutamatergic input (by analysing AMPAr synaptic puncta and contacts from glutamatergic boutons), and phosphorylation of extracellular signal-regulated kinases (pERKs) following noxious stimulation. Our results indicate that there are two populations of NK1r-expressing projection neurons: large GluA4+/GluA1− cells with a high density of glutamatergic input and small GluA1+/GluA4− cells with a much lower input density. Results from pERK experiments suggested that the two groups may not differ in the types of noxious stimulus that activate them. Glutamatergic synapses on distal dendrites of the large cells were significantly longer than those on proximal dendrites, which presumably compensates for the greater attenuation of distally-generated excitatory postsynaptic currents (EPSCs). Both types of cell received contacts from peptidergic primary afferents, however, on the large cells these appeared to constitute over half of the glutamatergic synapses, and were often associated with elongated AMPAr puncta. This suggests that these afferents, which probably contain substance P, provide a powerful, secure synaptic input to large NK1r-expressing projection neurons. These results demonstrate the importance of GluA4-containing AMPArs in nociceptive transmission and raise the possibility that different forms of LTP in lamina I projection neurons may be related to differential expression of GluA1/GluA4.
机译:脊髓的层I包含许多表达神经激肽1受体(NK1r)的投射神经元。据报道,这些细胞可经历长期增强作用(LTP),这可能是由于插入含有GluA1或GluA4亚基的AMPA型谷氨酸受体(AMPArs)导致的。因此,我们用抗原回收后的免疫细胞化学研究了这些细胞上突触AMPAr的表达。我们还检查了它们的谷氨酸能输入密度(通过分析AMPAr突触点和来自谷氨酸能纽扣的接触),以及有害刺激后细胞外信号调节激酶(pERK)的磷酸化。我们的结果表明存在两种表达NK1r的投射神经元群体:具有高密度谷氨酸能输入的大GluA4 + / GluA1-细胞和具有低得多的输入密度的小型GluA1 + / GluA4-细胞。 pERK实验的结果表明,在激活它们的有害刺激类型上,两组可能没有差异。大细胞远端树突上的谷氨酸能突触明显长于近端树突上的谷氨酸,这可能补偿了远端产生的兴奋性突触后突触电流(EPSC)的更大衰减。两种类型的细胞都接受肽能性初级传入的接触,但是,在大细胞上,它们似乎构成了谷氨酸能突触的一半以上,并且通常与细长的AMPAr点有关。这表明这些可能包含物质P的传入神经为表达大型NK1r的投射神经元提供了强大而安全的突触输入。这些结果证明了含GluA4的AMPAr在伤害性传递中的重要性,并增加了层I投影神经元中不同形式的LTP可能与GluA1 / GluA4差异表达有关的可能性。

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