RESUMO
BACKGROUND: Helicobacter pylori has been linked to several diseases such as chronic urticaria, gastritis, and type 1 gastric neuroendocrine tumors (type 1 gNET). Although these diseases seem to have different mechanisms, their relationship with H. pylori suggests a common inflammatory pathway. OBJECTIVE: To identify potential cross-reactive antigens between H. pylori and humans involved in chronic urticaria and type 1 gNET. METHODS: Alignment was carried out among human proteins associated with urticaria (9 proteins), type 1 gNET (32 proteins), and H. pylori proteome. We performed pairwise alignment among the human and H. pylori antigens with PSI-BLAST. Modeling based on homology was done with the Swiss model server and epitope prediction with the Ellipro server. Epitopes were located on a 3D model using PYMOL software. RESULTS: The highest conserved sequence was found between the human HSP 60 antigen and the H. pylori chaperonin GroEL with an identity of 54% and a cover of 92%, followed by the alpha and gamma enolases and two H. pylori phosphopyruvate hydratase, both with an identity and cover of 48% and 96%, respectively. The H/K ATPase (Chain A) showed high identity with two H. pylori proteins (35.21% with both P-type ATPase), but with low cover (only 6%). We observed eight linear and three discontinuous epitopes for human HSP 60 and three lineal and one discontinuous epitope for both alpha-enolase and gamma enolase, high conserved with H. pylori sequences. CONCLUSION: Some type 1 gNET antigens shared potential cross-reactive epitopes with H. pylori proteins, suggesting that molecular mimicry could be a mechanism that explains the relationship between the infection and this disease. Studies evaluating the functional impact of this relationship are needed.
Assuntos
Urticária Crônica , Infecções por Helicobacter , Helicobacter pylori , Tumores Neuroendócrinos , Urticária , Humanos , Epitopos , Infecções por Helicobacter/complicaçõesRESUMO
Introducción. Los tumores neuroendocrinos de páncreas son relativamente raros y heterogéneos. Sin embargo, su incidencia se ha incrementado a nivel mundial, y los avances en el diagnóstico y el tratamiento han mejorado la supervivencia. Tienen un pronóstico más favorable que el adenocarcinoma de páncreas, pero el reconocimiento y el abordaje diagnóstico son complejos y requieren un equipo humano multidisciplinario entrenado. Objetivo. Actualizar al médico en el abordaje clínico, patológico, imaginológico y genético, y en la evaluación hormonal basada en la evidencia disponible, brindando herramientas y recomendaciones específicas para las diferentes circunstancias clínicas. Conclusión. La incidencia de los tumores neuroendocrinos de páncreas en los últimos 40 años ha aumentado en más del 600 %, y corresponden a la segunda neoplasia pancreática con gran mortalidad. Actualmente, disponemos de múltiples biomarcadores para caracterizarlos y plantear un tratamiento más personalizado
Background: Pancreatic Neuroendocrine Tumors (nNET) are rare and heterogeneous. However, the incidence has increased worldwide, and the newer diagnostic methods and treatment have improved survival. They have a more favorable prognosis than pancreatic adenocarcinoma, but recognition and overall diagnostic methods are complex and require a trained multidisciplinary team. Aim: To update the clinical, pathological, imaging, genetic and hormonal evaluation based on the available evidence. To provide tools and recommendations for different clinical scenarios. Coclusions: The incidence of pNET in the last 40 years has increased by more than 600% and corresponds to the second pancreatic neoplasia with a high mortality rate