2012
DOI: 10.1002/cncy.21257
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Subclassification of lymphoproliferative disorders in serous effusions

Abstract: BACKGROUND: Rare studies have reported the application of multiple ancillary tests to the diagnosis of lymphoproliferative disorder in serous effusions. In the current study, the authors evaluated the effectiveness of using an algorithm for the triage of serous effusions and the contribution of ancillary studies to achieve a specific subtype of lymphoproliferative disorder. METHODS: Serous effusion samples that had a final diagnosis of lymphoproliferative disorder or suspicious for lymphoma were selected from … Show more

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Cited by 30 publications
(38 citation statements)
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“…Among the negative cases, 6 showed atypical morphologic features and were studied further, similarly to the cases with atypical, but nondiagnostic, findings on FC, yielding a final definitive diagnosis in an additional 29 and 17% of cases, respectively. The study of Tong et al [9] describes an algorithmic approach, including the application of FC and other auxiliary studies [immunohistochemistry, polymerase chain reaction for B- and T-cell clonality, human herpes virus type 8 (HHV8) status, and EBER], to the diagnosis of lymphoproliferative disease in effusion samples based on 10 years of experience. A diagnosis of a lymphoproliferative disease was made in 133 pleural effusions, 30 ascites, and 5 pericardial effusions.…”
Section: Impact Of Fc On Cytologic Diagnosesmentioning
confidence: 99%
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“…Among the negative cases, 6 showed atypical morphologic features and were studied further, similarly to the cases with atypical, but nondiagnostic, findings on FC, yielding a final definitive diagnosis in an additional 29 and 17% of cases, respectively. The study of Tong et al [9] describes an algorithmic approach, including the application of FC and other auxiliary studies [immunohistochemistry, polymerase chain reaction for B- and T-cell clonality, human herpes virus type 8 (HHV8) status, and EBER], to the diagnosis of lymphoproliferative disease in effusion samples based on 10 years of experience. A diagnosis of a lymphoproliferative disease was made in 133 pleural effusions, 30 ascites, and 5 pericardial effusions.…”
Section: Impact Of Fc On Cytologic Diagnosesmentioning
confidence: 99%
“…After consideration of the differential diagnosis, the proper indication should lead to selection of the antibody panel for the FC study. Since the frequency of malignant effusions is significantly higher in patients with known lymphomas than in those without a hematologic malignancy, the history of any such neoplasia, particularly of an indolent lymphoma, is the most important indication for performance of an FC analysis [6,8,9]. However, if the etiology of the microscopically nonneoplastic effusion remains unexplained, and especially if it is recurrent or accompanied by a striking lymphadenopathy, FC should be performed to rule out or prove the presence of an indolent lymphoma.…”
Section: Indication For Fc Of Effusionsmentioning
confidence: 99%
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“…The newer ancillary techniques used by cytologists, like flow cytometry (FC), help validate his/her morphological diagnosis with an immunological validation. The combined use of cytology and FC has been known to provide nearly 100% sensitivity and specificity, alleviating the need for an invasive procedure to obtain a tissue biopsy [1,2,3]. Fine-needle aspiration cytology (FNAC) along with FC has been shown to be a fundamental tool in the diagnosis and classification of non-Hodgkin's lymphoma [4].…”
Section: Introductionmentioning
confidence: 99%