[PDF][PDF] Selective expression of TLQP-21 and other VGF peptides in gastric neuroendocrine cells and modulation by feeding

C Brancia, C Cocco, F D'Amato, B Noli… - Journal of …, 2010 - researchgate.net
C Brancia, C Cocco, F D'Amato, B Noli, F Sanna, R Possenti, A Argiolas, GL Ferri
Journal of endocrinology, 2010researchgate.net
Although vgf gene knockout mice are hypermetabolic, administration of the VGF peptide
TLQP-21 itself increased energy consumption. Agonist–antagonist roles are thus suggested
for different VGF peptides, and the definition of their tissue heterogeneity is mandatory. We
studied the rat stomach using antisera to C-or N-terminal sequences of known or predicted
VGF peptides in immunohistochemistry and ELISA. TLQP (rat VGF556–565) peptide/s were
most abundant (162G11 pmol/g, meanGS. EM) and were brightly immunostained in …
Abstract
Although vgf gene knockout mice are hypermetabolic, administration of the VGF peptide TLQP-21 itself increased energy consumption. Agonist–antagonist roles are thus suggested for different VGF peptides, and the definition of their tissue heterogeneity is mandatory. We studied the rat stomach using antisera to C-or N-terminal sequences of known or predicted VGF peptides in immunohistochemistry and ELISA. TLQP (rat VGF556–565) peptide/s were most abundant (162G11 pmol/g, meanGS. EM) and were brightly immunostained in enterochromaffin-like (ECL) cells and somatostatin cells. A peptide co-eluting with TLQP-21 was revealed in HPLC of gastric and hypothalamic extracts, while the extended TLQP-62 form was restricted to the hypothalamus. Novel PGH (rat VGF422–430) peptide/s were revealed in ghrelin cells, mostly corresponding to low MW forms (0. 8–1. 5 kDa), while VGF C-terminus peptides were confined to neurons. VGF mRNA was present in the above gastric endocrine cell types, and was prominent in chief cells, in parallel with low-intensity staining for further cleaved products from the C-terminal region of VGF (HVLL peptides: VGF605–614). In swine stomach, a comparable profile of VGF peptides was revealed by immunohistochemistry. When fed and fasted rats were studied, a clear-cut, selective decrease on fasting was observed for TLQP peptides only (162G11 vs 74G5. 3 pmol/g, fed versus fasted rats, meanGS. EM, P! 0. 00001). In conclusion, specific VGF peptides appear to be widely represented in different gastric endocrine and other mucosal cell populations. The selective modulation of TLQP peptides suggests their involvement in peripheral neuro-endocrine mechanisms related to feeding responses and/or ECL cell regulation.
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