Introduction
SARS-CoV-2 (COVID-19) is known to cause severe respiratory infections with occasional accompanying pleural (PE), pericardial (PCE) or peritoneal effusion (PTE). The effect of COVID-19 disease on effusion cytology is not yet known. Therefore, our study aims to examine the cytomorphologic features and work-up of effusion fluid in patients in recovery from COVID-19 infection versus those with active disease.
Materials and Methods
PE (n=15), PCE (n=1), PTE (n=19) samples from hospitalized patients with COVID-19 infection (6/1/2020-12/30/2020) were reviewed. EFs with metastatic carcinoma were excluded. Differential cell count (DCC), cytomorphology, and immunostains of EFs were retrospectively evaluated by a board-certified cytopathologist and compared between patients with active infection (AI, n=22, positive COVID-19 nucleic acid amplification test (NAAT) within 2 months) and recovery phase from COVID-19 (RC, n=13, negative COVID-19 NAAT for >2 months).
Results
Cytology diagnoses were: negative for malignancy (n=30), atypical (n=4), suspicious for malignancy (n=1). AI cases showed more atypical mesothelial cells than RC cases (Table 1, p<0.05), some with enlarged nuclei with prominent nucleoli and occasional multi-nucleation (Figure 1), and some with bizarre nuclei (Table 1, p<0.01). Immunostains were performed more often in AI than RC cases (50.0% vs 7.7%, p<0.05). DCC (available in 28 cases) showed no significant difference amongst AI and RC cases (Figure 1, p>0.05).
Conclusions
Our study found atypical and bizarre mesothelial cells to be present more often in effusions of cases with active COVID-19 infection than in samples from patients in recovery, though DCCs did not show significant difference. Diagnosis of malignancy may be considered in cases with such nuclear atypia, which explains increased immunostain work-up in AI cases. It is important for cytopathologists to consider the patients’ COVID-19 infection status when evaluating effusion cytology cases.
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