| Literature DB >> 28063977 |
Raphaela da Cunha Franceschi1, Patrícia Nardin2, Clivia Valle Machado1, Lucas Silva Tortorelli2, Malcon Andrei Martinez-Pereira3, Caroline Zanotto2, Carlos-Alberto Gonçalves4, Denise Maria Zancan1.
Abstract
Lipopolysaccharide (LPS) is used to induce inflammation and promotes nervous system activation. Different regions of the brain present heterogeneous glial responses; thus, in order to verify whether systemic LPS-induced inflammation affects the enteric glia differently across the intestinal segments, we evaluated the expressions of two glial activity markers, GFAP and S100B protein, in different intestine segments, at 1h, 24h and 7days after acute systemic LPS administration (0.25 or 2.5mgkg-1) in rats. Histological inflammatory analysis indicated that the cecum was most affected when compared to the duodenum and proximal colon at the highest doses of LPS. LPS induced an increased S100B content after 24h in all three regions, which decreased at 7days after the highest dose in all regions. Moreover, at 24h, this dose of LPS increased ex-vivo S100B secretion only in the cecum. The highest dose of LPS also increased GFAP in all regions at 24h, but earlier in the cecum, where LPS-induced enteric S100B and GFAP alterations were dependent on dose, time and intestine region. No associated changes in serum S100B were observed. Our results indicate heterogeneous enteric glial responses to inflammatory insult, as observed in distinct brain areas.Entities:
Keywords: Enteric glia cell; GFAP; Inflammation; LPS; S100B
Mesh:
Substances:
Year: 2017 PMID: 28063977 DOI: 10.1016/j.neures.2016.12.005
Source DB: PubMed Journal: Neurosci Res ISSN: 0168-0102 Impact factor: 3.304