How can we use positron emission tomography/
computed tomography more accurately for characterization of asbestos-related pleural thickening?

F. Selcuk Simsek; Muharrem Cakmak; Duygu Kuslu; Tansel A. Balci; Erdal In; Ibrahim H. Ozercan; Yavuz Narin

doi:10.5114/aoms/111529

Archives of Medical Science (Mar 2021)

How can we use positron emission tomography/ computed tomography more accurately for characterization of asbestos-related pleural thickening?

F. Selcuk Simsek,
Muharrem Cakmak,
Duygu Kuslu,
Tansel A. Balci,
Erdal In,
Ibrahim H. Ozercan,
Yavuz Narin

Affiliations

F. Selcuk Simsek: Department of Nuclear Medicine, Faculty of Medicine, Pamukkale University, Denizli, Turkey
Muharrem Cakmak: Department of Thoracic Surgery, Faculty of Medicine, Firat University, Elazig, Turkey
Duygu Kuslu: Department of Nuclear Medicine, Antalya Education and Research Hospital, Antalya, Turkey
Tansel A. Balci: Department of Pulmonology, Faculty of Medicine, Firat University, Elazig, Turkey
Erdal In: Department of Pulmonology, Faculty of Medicine, Firat University, Elazig, Turkey
Ibrahim H. Ozercan: Department of Pathology, Faculty of Medicine, Firat University, Elazig, Turkey
Yavuz Narin: Department of Nuclear Medicine, Elazig Medical Park Hospital, Elazig, Turkey

DOI: https://doi.org/10.5114/aoms/111529
Journal volume & issue: Vol. 19, no. 2
pp. 385 – 391

Abstract

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Introduction There is no consensus about the standardized uptake value maximum (SUV max ) cut-off value to characterize pleural thickening worldwide. Sometimes, this causes unnecessary invasive diagnostic procedures. Our first aim is to determine a cut-off value for SUV max . Secondly, we try to answer the following question: If we use this cut-off value together with morphological parameters, can we differentiate benign thickening from malignant pleural mesothelioma (MPM) more accurately? Material and methods Thirty-seven patients who underwent 2-deoxy-2-fluoro-D-glucose ([18F]FDG) positron emission tomography/computed tomography (PET/CT) before pleural biopsy were included the study. All of patients had histopathologically proven primary pleural disease. Their [18F]FDG-PET/CT imaging reports were re-assessed. If a patient’s SUVmax or size of the thickening was not mentioned in the report, we calculated it with their [18F]FDG-PET/CT. Results Age, pleural effusion, size, and SUV max were found to have a relationship with MPM. We found the size > 14 mm, and SUV max > 4.0 as cut-off values for MPM. The sensitivity, specificity, positive predictive value (PPV), and negative predictive value (NPV) for size > 14 mm were found to be 86.4%, 85.2%, 82.6%, 88.5%, respectively. For SUV max > 4.0, sensitivity, specificity, PPV, NPV were 90.9%, 87.0%, 85.1%, 92.2%, respectively. Conclusions If a patient has SUV max > 4.0 and/or size > 14 mm, the risk of MPM is high. These patients should undergo biopsy. If a patient’s SUV max < 4.0, size < 14 mm and does not have pleural effusion, he/she has low risk for MPM. These patients can undergo the follow-up. If a patient’s SUV max < 4, size < 14, and has pleural effusion the MPM risk is approximately 4%. These patients can undergo biopsy/cytology/follow-up. Novel studies are needed for these patients.

Published in Archives of Medical Science

ISSN: 1734-1922 (Print); 1896-9151 (Online)
Publisher: Termedia Publishing House
Country of publisher: Poland
LCC subjects: Medicine
Website: https://www.archivesofmedicalscience.com/

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