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首页> 外文期刊>The Journal of Comparative Neurology >Neurochemical characterization of insulin receptor-expressing primary sensory neurons in wild-type and vanilloid type 1 transient receptor potential receptor knockout mice.
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Neurochemical characterization of insulin receptor-expressing primary sensory neurons in wild-type and vanilloid type 1 transient receptor potential receptor knockout mice.

机译:在野生型和类香草素1型瞬时受体电位受体基因敲除小鼠中表达胰岛素受体的初级感觉神经元的神经化学表征。

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The insulin receptor (IR) is expressed by a subpopulation of primary sensory neurons (PSN), including a proportion of cells expressing the nociceptive transducer vanilloid type 1 transient receptor potential receptor (TRPV1). Recent data suggest functional links between the IR and other receptors, including TRPV1, which could be involved in the development of PSN malfunctions in pathological insulin secretion. Here we used combined immunohistochemical labelling on sections from L4-5 dorsal root ganglia of wild-type (WT) and TRPV1 knockout (KO) mice to examine the neurochemical properties of IR-expressing PSN and the possible effect of deletion of TRPV1 on those characteristics. We found that antibodies raised against the high-molecular-weight neurofilament (NF-200) and the neurofilament protein peripherin distinguished between small and large neurons. We also found that the IR was expressed predominantly by the small peripherin-immunopositive cells both in the WT and in the KO animals. IR expression, however, did not show any preference between the major subpopulations of the small cells, the calcitonin gene-related peptide (CGRP)-expressing and Bandeiraea simplicifolia isolectin B4 (IB4)-binding neurons, either in the WT or in the KO mice. Nevertheless, a significant proportion of the IR-expressing cells also expressed TRPV1. Comparison of the staining pattern of these markers showed no difference between WT and KO animals. These findings indicate that the majority of the IR-expressing PSN are small neurons, which are considered as nociceptive cells. Furthermore, these data show that deletion of the TRPV1 gene does not induce any additional changes in neurochemical phenotype of nociceptive PSN.
机译:胰岛素受体(IR)由初级感觉神经元(PSN)的亚群表达,包括一部分表达伤害性感受器1型瞬态受体电位受体(TRPV1)的细胞。最新数据表明,IR和其他受体(包括TRPV1)之间的功能联系可能与病理性胰岛素分泌中PSN功能障碍的发展有关。在这里,我们对野生型(WT)和TRPV1基因敲除(KO)小鼠的L4-5背根神经节的切片进行了免疫组化标记,以检测表达IR的PSN的神经化学特性以及删除TRPV1对这些特征的可能影响。我们发现针对高分子量神经丝(NF-200)和神经丝蛋白周围蛋白产生的抗体可区分大小神经元。我们还发现,IR主要由野生型和KO动物中的小外周蛋白免疫阳性细胞表达。然而,无论是野生型还是野生型,在小细胞的主要亚群,降钙素基因相关肽(CGRP)表达和辛氏白带菌isolectin B4(IB4)结合神经元之间,IR表达都没有表现出任何偏好。老鼠。然而,很大比例的表达IR的细胞也表达了TRPV1。这些标记物的染色模式的比较显示野生型和KO型动物之间没有差异。这些发现表明大多数表达IR的PSN是小神经元,被认为是伤害性细胞。此外,这些数据表明,TRPV1基因的缺失不会引起伤害性PSN的神经化学表型的任何其他变化。

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