Your search keyword '"PULMONARY surfactant-associated protein A"' showing total 4 results

1. Establishment and validation of nomogram for predicting immuno checkpoint inhibitor related pneumonia

Author

Xiaoqi Li, Fei Lv, Ying Wang, and Zhenguang Du

Subjects

Immune checkpoint inhibitors, Krebs von den Lungen-6 protein, Nomograms, Pneumonia, Pulmonary surfactant-associated protein A, Diseases of the respiratory system, RC705-779

Abstract

Abstract Objective Cancer is one of the main causes of death worldwide. Although immunotherapy brings hope for cancer treatment, it is also accompanied by immune checkpoint inhibitor-related adverse events (irAEs). Immune checkpoint inhibitor pneumonia (CIP) is a potentially fatal adverse event, but there is still a lack of effective markers and prediction models to identify patients at increased risk of CIP. Methods A total of 369 cancer patients treated between 2017 and 2022 with immune checkpoint inhibitors at Shengjing Hospital of China Medical University and Liaoning People's Hospital were recruited for this study. Independent variables were selected by differences and binary logistic regression analysis, and a risk assessment nomogram was constructed for CIP risk. The accuracy and discriminative abilities of the nomogram were evaluated by calibration plots, receiver operating characteristic curves (ROCs) and decision curve analyses (DCAs). Results Binary logistic regression analysis showed that smoking history, acute phase proteins [interleukin (IL-6) and C-reactive protein (CRP)], CD8 + T lymphocyte count and serum alveolar protein [surface protein-A (SP-A) and Krebs Von den Lungen-6 (KL-6)] were significantly associated with CIP risk. A nomogram consisting of these variables was established and validated by different analyses. Conclusions We developed an effective risk nomogram for CIP prediction in immune-checkpoint inhibitor administrated cancer patients, which will further assist early detection of immunotherapy-related adverse events.

Published

2022

2. THE INFLUENCE OF MYCOPLASMA PNEUMONIAE AND RECOMBINANT CARDS TOXIN ON THE HUMAN LUNG EPITHELIAL CELLS: THE EFFECT OF SURFACTANT PROTEIN A ON THE MICROORGANISM PATHOGENICITY IN VITRO

Author

Hlinkina T. V., Kostiuk S. A., Rudenkova T. V., and Poluyan O. S.

Subjects

Mycoplasma pneumoniae, respiratory epithelium, cytokines, pulmonary surfactant-associated protein A, Medicine

Abstract

Background: M. pneumoniae and CARDS toxin interact with respiratory epithelium in the presence of surfactant protein A (SP-A). Objective of the study was to estimate the production of proinflammatory cytokines from human lung epithelial cells activated with M. pneumoniae and CARDS toxin as well as to study the influence of SP-A on M. pneumoniae pathogenicity. Material and Method: SP-A treated and not-treated A549 cells were activated with M. pneumoniae and recombinant CARDS (rCARDS) toxin. TNF-α, IL-6, RANTES and IL-33 were analyzed. Results: Pre-treatment with SP-A enhanced RANTES, TNF-α and IL-6 production and prevented cells from increased release of the allergy associated cytokine IL-33. Conclusion: SP-A regulates the interaction between M. pneumoniae, rCARDS and A549 cells by modulating the cytokine release.

Published

2019

3. Surfactant Protein A and Microbiome Composition in Patients With Atraumatic Intraoral Lesions

Author

Shawn Adibi, Davor Seferovic, Gena D. Tribble, Joseph L. Alcorn, and Walid D. Fakhouri

Subjects

humans, pulmonary surfactant-associated protein a, microbiota, oral ulcer, biomarkers, Dentistry, RK1-715

Abstract

Oral ulcers are lesions that occur due to disruption of epithelial integrity of the mucosa of the oral cavity. Intraoral ulcers are often associated with pain, redness, symptoms of discomfort, and blood hemorrhage. The etiology for many oral ulcers is local trauma, systemic health conditions, or medication; for other ulcers the cause is less clear. This pilot study aims to evaluate the salivary components and microbiome in patients with atraumatic pre-ulcerous and ulcerous oral lesions compared to control individuals, while considering three common risk factors for atraumatic ulcers, smoking, stress, and gender. This study uses matched age, sex, and ethnicity samples from healthy otherwise and oral lesion patients to investigate the changes in salivary surfactant protein A (SP-A) and examines the prevalence and diversity of the salivary oral microflora. The goal is to determine if there are factors in saliva that have the potential to be used as biomarkers for risk of developing atraumatic oral ulcers. Our data show that the average level of SP-A is significantly reduced in female smokers compared to non-smoker healthy females. The average level of SP-A in female oral lesion patients is reduced compared to controls. The microbiome composition is significantly affected by smoking and the level of SP-A. Comparing the control participants and oral lesion patients, there are 16 species of bacteria that are significantly different, and all of these bacteria are significantly affected by smoking and SP-A. LEfSe analysis identified five bacteria that may represent potential biomarkers. This preliminary study demonstrates the potential of the oral microbiome to act as a biomarker for oral ulcer risk and infers potential mechanistic links between risk factors and alterations in innate immune mechanisms such as SP-A levels.

Published

2021

4. Surfactant protein A is decreased in the lung of rats with hepatopulmonary syndrome

Author

Lucas Souto Nacif, Wellington Andraus, Márcia Saldanha Kubrusly, Flávia Saldanha Kubrusly, Vera Cristina Bugelli Cainelli Gebara, Andrea Ishizawa, and Luiz Augusto Carneiro D'Albuquerque

Subjects

Hepatopulmonary Syndrome, Pulmonary Surfactant-Associated Protein A, Models, Animal, Rats, Surgery, RD1-811

Abstract

PURPOSE:To evaluate surfactant protein A levels in an hepatopulmonary syndrome rat model. To date, there have been no studies aimed at evaluating surfactant levels in the setting of cirrhosis or hepatopulmonary syndrome.METHODS:A total of 35 rats were divided into control, sham, and experimental HPS groups. We evaluated surfactant protein A levels in rats and the experimental model designed to induce hepatopulmonary syndrome was common bile duct ligation. Statistical analysis was performed using GraphPad Prism Software(r). Differences were considered statistically significant when p

Published

2014