The “Brescia panel” (Claudin‐4 and BRCA‐associated protein 1) in the differential diagnosis of mesotheliomas with epithelioid features versus metastatic carcinomas

Bernardi, Livia; Bizzarro, Tommaso; Pironi, Flavio; Szymczuk, S; Buda, Raffaella; Fabbri, Enrica; Claudio, Giovanni Di; Rossi, Giulio

doi:10.1002/cncy.22368

Cited by 19 publications

(37 citation statements)

References 31 publications

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“…In order to maximize the diagnostic sensitivity and specificity of immunohistochemical markers, Bernardi et al [ 93 ] demonstrated that the coordinated use of two mesothelial negative biomarkers, namely claudin 4 and BAP1, had the best performance in differential diagnosis between epithelioid or biphasic mesothelioma and metastatic carcinomas. The expression of claudin-4 alone excluded MPM and double negativity was evident in all MPM.…”

Section: Unusual Morphologic and Immunohistochemical Featuresmentioning

confidence: 99%

“…This study summarized previous experiences singly investigating claudin-4 and BAP1 [ 94 , 95 , 96 , 97 , 98 ], and was performed on cell blocks and the corresponding pleural biopsies. In a practical algorithm [ 93 ], BAP1 and claudin-4 seems to represent the best panel for differentiating MPM with epithelioid features and metastatic carcinoma either on cytology or biopsy. More recently, cytoplasmic loss of methylthioadenosine phosphorylase (MTAP) has emerged as a specific marker of malignancy in mesothelial proliferations [ 99 , 100 , 101 ].…”

Section: Unusual Morphologic and Immunohistochemical Featuresmentioning

confidence: 99%

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When the Diagnosis of Mesothelioma Challenges Textbooks and Guidelines

Rossi

Davoli

Poletti

et al. 2021

JCM

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The diagnosis of malignant mesothelioma (MPM) does not pose difficulties when presenting with usual clinico-radiologic features and morphology. Pathology textbooks and national/international guidelines generally describe the findings of classic MPM, underlining common clinical presentation, the gold standard of sampling techniques, usual morphologic variants, immunohistochemical results of several positive and negative primary antibodies in the differential diagnosis, and the role of novel molecular markers. Nevertheless, MPM often does not follow the golden rules in routine practice, while the literature generally does not sufficiently emphasize unusual features of its manifestation. This gap may potentially create problems for patients in sustaining a difficult diagnosis of MPM in clinical practice and during legal disputes. Indeed, the guidelines accidentally tend to favor the job of lawyers and pathologists defending asbestos-producing industries against patients suffering from MPM characterized by uncommon features. The current review is aimed at underlining the wide spectrum of clinical and radiological presentation of MPM, the possibility to consistently use cytology for diagnostic intent, the aberrant immunohistochemical expression using so-called specific negative and positive primary antibodies, and finally proposing some alternative and more unbiased approaches to the diagnosis of MPM.

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Section: Unusual Morphologic and Immunohistochemical Featuresmentioning

confidence: 99%

Section: Unusual Morphologic and Immunohistochemical Featuresmentioning

confidence: 99%

When the Diagnosis of Mesothelioma Challenges Textbooks and Guidelines

Rossi

Davoli

Poletti

et al. 2021

JCM

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“…Additional ancillary tests may then be employed as necessary. Further studies are expected to validate this promising approach [14,48].…”

Section: Mesothelial Proliferationsmentioning

confidence: 99%

The International System for Reporting Serous Fluid Cytopathology: How to Incorporate Molecular Data in Cytopathology Reports

Pinto

Chandra

Schmitt

2021

JMP

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Serous effusion cytology is widely employed in the initial evaluation of the etiology of effusions with a high diagnostic sensitivity. To standardize practices, The International System for Reporting Serous Fluid Cytology (TIS) was developed following best international practices, the most up-to-date literature, and expert consensus. In the context of this system, ancillary techniques play an important role. Besides defining basic principles in laboratory specimen handling, adequacy criteria, and a standardized reporting terminology with five diagnostic categories, TIS provides an actionable framework for using immunohistochemical and molecular testing in effusion samples, namely, in atypical, suspicious of malignant samples. For diagnostic purposes, these tests may be employed to distinguish between a primary and secondary neoplasm, to confirm a diagnosis of malignant mesothelioma vs. reactive mesothelial hyperplasia, and to correctly classify and determine the primary location of a metastasis. Theranostic molecular tests may also be used for these samples to evaluate potential therapeutic targets. Pathologists play a central role in guiding this process by determining adequacy and selecting appropriate ancillary tests. The activity in this area of research should increase in the near future as new therapeutic targets are discovered and new drugs enter the clinical practice.

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“…Although the value of BRCA‐associated protein 1 (BAP1) and Claudin‐4 has been documented by many studies, Bernardi and colleagues were the first to draw attention to these 2 markers through their earlier publications. In this issue of Cancer Cytopathology , they propose the name of Brescia panel for the combination of these 2 markers 1 . The panel presents the opportunity to use only 2 markers, given the high sensitivity and specificity of the panel to differentiate between mesothelioma (BAP1‐negative/Claudin‐4–negative) from metastatic carcinoma (BAP1‐positive/Claudin‐4–positive).…”

mentioning

confidence: 99%

“…In this issue of Cancer Cytopathology, they propose the name of Brescia panel for the combination of these 2 markers. 1 The panel presents the opportunity to use only 2 markers, given the high sensitivity and specificity of the panel to differentiate between mesothelioma (BAP1-negative/Claudin-4-negative) from metastatic carcinoma (BAP1-positive/Claudin-4-positive).…”

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confidence: 99%

The Brescia panel and The International System for Reporting Serous Fluid Cytopathology

Chandra

2020

Cancer Cytopathology

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The distinction between mesothelial proliferations and metastatic adenocarcinoma in serous fluids remains a common and vexing issue. Whereas cytomorphology allows the identification of one cell type (mesothelial) over another (epithelial), this may be challenging when the number of lesional cells is small, when cells are associated with bland nuclear morphology accompanied by degenerative changes, or when unusual tumor subtypes present in serous fluids. For confirmation of the diagnosis, immunochemical panels using 2 epithelial immunostains and 2 mesothelial immunostains are common practice, with the choice of markers depending on availability and the experience of their usage in a particular institution. Although the value of BRCA-associated protein 1 (BAP1) and Claudin-4 has been documented by many studies, Bernardi and colleagues were the first to draw attention to these 2 markers through their earlier publications. In this issue of Cancer Cytopathology, they propose the name of Brescia panel for the combination of these 2 markers. 1 The panel presents the opportunity to use only 2 markers, given the high sensitivity and specificity of the panel to differentiate between mesothelioma (BAP1-negative/Claudin-4-negative) from metastatic carcinoma (BAP1-positive/Claudin-4-positive). Bernardi et al demonstrate compelling evidence through their pilot study for the cytopathology community to consider validating this panel. The pattern of staining, nuclear with BAP1 and membranous with Claudin-4, makes these immunostains easier to interpret compared with cytoplasmic staining, which is sometimes not as well localized. The panel has been applied successfully to cell block and biopsy specimens. Incidentally, both markers are recommended by The International System (TIS) for Reporting Serous Fluid Cytopathology. 2 The system mentions Claudin-4 as a promising marker for the confirmation of metastatic carcinoma and for the exclusion of mesothelioma. BAP1 is also recommended as an immunostain of choice for the diagnosis of mesothelioma. In the absence of BAP1 loss, clinical data should be taken into account and the mesothelial proliferation should be reported as either atypia of undetermined significance or suspicious for malignancy in TIS, similar to what is proposed by the authors. The Brescia panel holds much promise and merits further validation studies using only Claudin-4 and BAP1 instead of larger panels. This would allow more residual diagnostic material to be available for ascertaining the primary sites and for performing molecular testing of malignant cells in serous effusions. FUNDING SUPPORT No specific funding was disclosed. CONFLICT OF INTEREST DISCLOSURES The author made no disclosures.

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The “Brescia panel” (Claudin‐4 and BRCA‐associated protein 1) in the differential diagnosis of mesotheliomas with epithelioid features versus metastatic carcinomas

Cited by 19 publications

References 31 publications

When the Diagnosis of Mesothelioma Challenges Textbooks and Guidelines

When the Diagnosis of Mesothelioma Challenges Textbooks and Guidelines

The International System for Reporting Serous Fluid Cytopathology: How to Incorporate Molecular Data in Cytopathology Reports

The Brescia panel and The International System for Reporting Serous Fluid Cytopathology

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