Rodolfo Duarte Nascimento, Patrícia Rocha Martins, André de Souza Lisboa, Sheila Jorge Adad, Alexandre Barcelos Morais da Silveira, Débora d'Ávila Reis
Department of Morphology, ICB, Universidade Federal de Minas Gerais, Belo Horizonte, Minas Gerais 31.270-901, Brazil.
Human pathology 2013 FebMegaesophagus is one of the major causes of morbidity in chronic Chagas disease, and extensive denervation, associated with an inflammatory process, is recognized as the key factor for alterations in motility and disease development. Here, we analyzed esophagus samples from necropsied, infected individuals--6 cases with megaesophagus and 6 cases without megaesophagus--for the relative areas of expression of 2 neuromediators, substance P and vasoactive intestinal peptide, which are known to activate or inhibit, respectively, local immune cells. Samples from 6 noninfected individuals were used as controls. Esophageal sections were immunohistochemically stained for protein gene product 9.5, vasoactive intestinal peptide, and substance P, and the relative areas of expression of the latter 2 were calculated. Morphometric analyses revealed increased substance P and decreased vasoactive intestinal peptide relative areas in esophageal sections from patients with megaesophagus. Furthermore, in the group of patients without megaesophagus, the loss of vasoactive intestinal peptide positively correlated with the denervation process. We suggest that an imbalance between vasoactive intestinal peptide and substance P production results in the reestablishment and maintenance of the inflammatory process, leading to denervation and, consequently, promoting the development of megaesophagus. Copyright © 2013 Elsevier Inc. All rights reserved.
Rodolfo Duarte Nascimento, Patrícia Rocha Martins, André de Souza Lisboa, Sheila Jorge Adad, Alexandre Barcelos Morais da Silveira, Débora d'Ávila Reis. An imbalance between substance P and vasoactive intestinal polypeptide might contribute to the immunopathology of megaesophagus after Trypanosoma cruzi infection. Human pathology. 2013 Feb;44(2):269-76
PMID: 22995328
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