Your search keyword '"Mendes CCH"' showing total 4 results

1. Th22 cytokines and yellow fever: Possible implications for the immunopathogenesis of human liver infection.

Author

Mendes CCH, de Sousa JR, Olímpio FA, Falcão LFM, Carvalho MLG, da Costa Lopes J, Martins Filho AJ, do Socorro Cabral Miranda V, Dos Santos LC, da Silva Vilacoert FS, Galúcio VCA, do Socorro da Silva Azevedo R, Martins LC, Duarte MIS, da Costa Vasconcelos PF, and Quaresma JAS

Subjects

Cytokines, Humans, Yellow fever virus, Communicable Diseases, Flavivirus, Liver Diseases, Yellow Fever pathology

Abstract

Yellow fever (YF) is an infectious disease considered a public health problem in tropical and subtropical areas. YF has many pathophysiological events that are correlated with the host immune response. In this study, the in situ Th22 cytokine profile was evaluated. Liver tissue samples were collected from 21 YFV-positive patients who died of the disease and five flavivirus-negative controls who died of other causes and whose hepatic parenchyma architecture was preserved. Immunohistochemical (IHC) analysis of tissues in the hepatic parenchyma of YF cases showed significantly higher expression of interleukin (IL)-22, IL-13, tumour necrosis factor-alpha, and FGF basic (FGF b) in YFV-positive cases than that in flavivirus-negative controls. These results indicate that the response of Th22 cytokines emerges as an alternative for a better understanding of adaptive immunity in the hepatic parenchyma, highlighting the role of cytokines in the repair and suppressive responses in the immunopathogenesis of YFV infection., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2022

2. Role of Th17 Cytokines in the Liver's Immune Response during Fatal Yellow Fever: Triggering Cell Damage Mechanisms.

Author

Carvalho MLG, Falcão LFM, Lopes JDC, Mendes CCH, Olímpio FA, Miranda VDSC, Santos LCD, de Moraes DDP, Bertonsin Filho MV, da Costa LD, da Silva Azevedo RDS, Cruz ACR, Galúcio VCA, Martins LC, Duarte MIS, Martins Filho AJ, Sousa JR, Vasconcelos PFDC, and Quaresma JAS

Subjects

Cytokines, Humans, Immunity, Liver pathology, Th17 Cells pathology, Yellow Fever pathology

Abstract

Yellow fever (YF) is an infectious and acute viral haemorrhagic disease that triggers a cascade of host immune responses. We investigated the Th17 cytokine profile in the liver tissue of patients with fatal YF. Liver tissue samples were collected from 26 deceased patients, including 21 YF-positive and 5 flavivirus-negative patients, with preserved hepatic parenchyma architecture, who died of other causes. Histopathological and immunohistochemical analysis were performed on the liver samples to evaluate the Th17 profiles (ROR-γ, STAT3, IL-6, TGF-β, IL-17A, and IL-23). Substantial differences were found in the expression levels of these markers between the patients with fatal YF and controls. A predominant expression of Th17 cytokine markers was observed in the midzonal region of the YF cases, the most affected area in the liver acinus, compared with the controls. Histopathological changes in the hepatic parenchyma revealed cellular damage characterised mainly by the presence of inflammatory cell infiltrates, Councilman bodies (apoptotic cells), micro/macrovesicular steatosis, and lytic and coagulative necrosis. Hence, Th17 cytokines play a pivotal role in the immunopathogenesis of YF and contribute markedly to triggering cell damage in patients with fatal disease outcomes.

Published

2022

3. Factors Involved in the Apoptotic Cell Death Mechanism in Yellow Fever Hepatitis.

Author

da Costa Lopes J, Falcão LFM, Martins Filho AJ, Carvalho MLG, Mendes CCH, Olímpio FA, do Socorro Cabral Miranda V, Dos Santos LC, Chiang JO, Cruz ACR, Galúcio VCA, do Socorro da Silva Azevedo R, Martins LC, Duarte MIS, de Sousa JR, da Costa Vasconcelos PF, and Quaresma JAS

Subjects

Apoptosis, Humans, Yellow fever virus, Epidemics, Hepatitis, Hepatitis A epidemiology, Yellow Fever

Abstract

Yellow fever (YF), a non-contagious infectious disease, is endemic or enzootic to the tropical regions of the Americas and Africa. Periodic outbreaks or epidemics have a significant impact on public health. Programmed cell death, or apoptosis, is generally characterised by distinct morphological changes and energy-dependent biochemical pathways. In this study, we performed immunohistochemistry analysis to identify and quantify proteases and protein targets involved in the cascade that triggers apoptosis in YF virus (YFV)-infected human hepatocytes. Liver tissue samples were collected from 26 individuals, among whom 21 were diagnosed as YF-positive, and five were flavivirus-negative and died due to other causes. The histopathological alterations in YFV-positive cases were characterised by the presence of apoptotic bodies, steatosis, cellular swelling, and extensive necrosis and haemorrhage in the hepatic lobules. Additionally, we observed an abundance of inflammatory infiltrates in the portal tract. The expression of various apoptotic markers in the hepatic parenchyma, including CASPASE 3, CASPASE 8, BAX, FAS, FASL, GRANZYME B, and SURVIVIN, differed between YFV-positive cases and controls. Collectively, this study confirmed the complexity of YFV infection-induced apoptosis in situ. However, our data suggest that apoptosis in liver parenchyma lesions may significantly contribute to the pathogenesis of fatal YF in humans.

Published

2022

4. Endothelium Activation during Severe Yellow Fever Triggers an Intense Cytokine-Mediated Inflammatory Response in the Liver Parenchyma.

Author

Olímpio FA, Falcão LFM, Carvalho MLG, da Costa Lopes J, Mendes CCH, Filho AJM, da Silva CAM, Miranda VDSC, Santos LCD, da Silva Vilacoert FS, Cruz ACR, Galúcio VCA, da Silva Azevedo RDS, Martins LC, Duarte MIS, de Sousa JR, da Costa Vasconcelos PF, and Quaresma JAS

Abstract

Yellow fever (YF) is a pansystemic disease caused by the yellow fever virus (YFV), the prototype species of the family Flaviviridae and genus Flavivirus , and has a highly complex host-pathogen relationship, in which endothelial dysfunction reflects viral disease tropism. In this study, the in situ endothelial response was evaluated. Liver tissue samples were collected from 21 YFV-positive patients who died due to the disease and five flavivirus-negative controls who died of other causes and whose hepatic parenchyma architecture was preserved. Immunohistochemical analysis of tissues in the hepatic parenchyma of YF cases showed significantly higher expression of E-selectin, P-selectin, intercellular adhesion molecule-1, vascular cell adhesion molecule-1, and very late antigen-4 in YFV-positive cases than in flavivirus-negative controls. These results indicate that endothelium activation aggravates the inflammatory response by inducing the expression of adhesion molecules that contribute to the rolling, recruitment, migration, and construction of the inflammatory process in the hepatic parenchyma in fatal YF cases.

Published

2022