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Correlation of neuronal size and peptide immunoreactivity in the guinea-pig trigeminal ganglion
Authors:W Kummer  Prof Dr Ch Heym
Institution:(1) Anatomisches Institut der Universität, Heidelberg, Bundesrepublik Deutschland;(2) Anatomisches Institut I der Universität, Im Neuenheimer Feld 307, D-6900 Heidelberg, Germany
Abstract:Summary Frequency and size of guinea-pig trigeminal neurones immunoreactive with antisera to agr-neo-endorphin(agr-neo-END), dynorphin A-(DYN), vasoactive intestinal polypeptide-(VIP), somatostatin-(SOM), and substance P-(SP) are reported. Co-localisation of the various peptides to the same ganglion cells was investigated immunocytochemically in consecutive 7-mgrm thick paraffin sections. According to their size, all peptide-immunoreactive neurones belong to the class of ldquosmallrdquo ganglion cells. Within this cell group, SP-immunoreactive neurones appear to be the largest, followed by SOM-, VIP-, agr-neo-END- and DYN-immunoreactive ganglion cells. The observed differences in size are statistically significant with the exception of that between agr-neo-END and DYN. This finding correlates well with the observed co-occurrence of the two immunoreactive peptides. All agr-neo-END-immunoreactive perikarya are also reactive to VIP antisera. These neurones are significantly smaller than those containing VIP-immunoreactivity exclusively. Ganglion cells displaying co-existence of agr-neoEND- and SP-immunoreactivity or VIP- and SP-immunoreactivity are found too infrequently to allow morphometric analysis. Some non-immunoreactive ganglion cells are shown to be approached by dense baskets of VIP-, agr-neo-END- or SP-immunoreactive varicose fibres, indicating the presence of intraganglionic modulation sites. The combination of immunohistochemistry and morphometry presented in this study allows the differentiation of diverse populations of primary afferent neurones exhibiting peptide immunoreactivity, most likely reflecting their involvement in different central and peripheral reflex arcs and sensory modalities.
Keywords:Opioid peptides  Somatostatin  Substance P  Vasoactive intestinal polypeptide  Trigeminal ganglion  Guinea pig
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