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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Baiou, Djalil
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机构:Chelsea & Westminster Hosp, Imperial Coll London, Dept Anaesthet Pain Management & Intens Care, London SW10 9NH, England
Baiou, Djalil
Santha, Peter
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机构:Chelsea & Westminster Hosp, Imperial Coll London, Dept Anaesthet Pain Management & Intens Care, London SW10 9NH, England
Santha, Peter
Avelino, Antonio
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机构:Chelsea & Westminster Hosp, Imperial Coll London, Dept Anaesthet Pain Management & Intens Care, London SW10 9NH, England
Avelino, Antonio
Charrua, Ana
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机构:Chelsea & Westminster Hosp, Imperial Coll London, Dept Anaesthet Pain Management & Intens Care, London SW10 9NH, England
Charrua, Ana
Bacskai, Timea
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机构:Chelsea & Westminster Hosp, Imperial Coll London, Dept Anaesthet Pain Management & Intens Care, London SW10 9NH, England
Bacskai, Timea
Matesz, Klara
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机构:Chelsea & Westminster Hosp, Imperial Coll London, Dept Anaesthet Pain Management & Intens Care, London SW10 9NH, England
Matesz, Klara
Cruz, Francisco
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机构:Chelsea & Westminster Hosp, Imperial Coll London, Dept Anaesthet Pain Management & Intens Care, London SW10 9NH, England
Cruz, Francisco
Nagy, Istvan
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机构:Chelsea & Westminster Hosp, Imperial Coll London, Dept Anaesthet Pain Management & Intens Care, London SW10 9NH, England
Nagy, Istvan
机构:
[1] Chelsea & Westminster Hosp, Imperial Coll London, Dept Anaesthet Pain Management & Intens Care, London SW10 9NH, England
[2] Univ Szeged, Fac Med, Dept Physiol, H-6720 Szeged, Hungary
[3] Univ Porto, Inst Histol & Embryol, P-4200 Oporto, Portugal
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 I 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 inummohistochernical labelling on sections from LA-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.