<HashMap><database>biostudies-literature</database><scores/><additional><submitter>Chapel DB</submitter><funding>NIBIB NIH HHS</funding><funding>U.S. Department of Health &amp;amp; Human Services | NIH | National Cancer Institute</funding><funding>U.S. Department of Defense</funding><funding>NCI NIH HHS</funding><funding>Ovarian Cancer Research Fund Alliance</funding><pagination>1383-1397</pagination><full_dataset_link>https://www.ebi.ac.uk/biostudies/studies/S-EPMC9529776</full_dataset_link><repository>biostudies-literature</repository><omics_type>Unknown</omics_type><volume>35(10)</volume><pubmed_abstract>BAP1 and MTAP immunostains play an important role in diagnosis of mesothelioma, but additional markers are needed to increase sensitivity. We analyzed 84 pleural mesotheliomas (51 epithelioid, 27 biphasic, 6 sarcomatoid) by a hybrid-capture next-generation sequencing (NGS) panel including complete coverage of coding and splicing regions for BAP1, CDKN2A/MTAP, NF2, and TP53 and correlated molecular findings with diagnostic immunostains for BAP1, MTAP, Merlin, and p53, respectively. Fifty-seven reactive mesothelial proliferations served as benign comparators. Loss of BAP1, MTAP, and Merlin protein expression were, respectively, 54%, 46%, and 52% sensitive and 100% specific for mesothelioma. Two-marker immunopanels of BAP1 + MTAP, BAP1 + Merlin, and MTAP + Merlin were 79%, 85%, and 71% sensitive for mesothelioma, while a three-marker immunopanel of BAP1 + MTAP + Merlin was 90% sensitive. Diffuse (mutant-pattern) p53 immunostaining was seen in only 6 (7%) tumors but represented the only immunohistochemical abnormality in 2 cases. Null-pattern p53 was not specific for malignancy. An immunopanel of BAP1 + MTAP + Merlin + p53 was 93% sensitive for mesothelioma, and panel NGS detected a pathogenic alteration in BAP1, MTAP, NF2, and/or TP53 in 95%. Together, 83 (99%) of 84 tumors showed a diagnostic alteration by either immunohistochemistry or panel NGS. Adding Merlin to the standard BAP1 + MTAP immunopanel increases sensitivity for mesothelioma without sacrificing specificity. p53 immunohistochemistry and panel NGS with complete coverage of BAP1, CDKN2A/MTAP, TP53, and NF2 may be useful in diagnostically challenging cases.</pubmed_abstract><journal>Modern pathology : an official journal of the United States and Canadian Academy of Pathology, Inc</journal><pubmed_title>Clinical and molecular validation of BAP1, MTAP, P53, and Merlin immunohistochemistry in diagnosis of pleural mesothelioma.</pubmed_title><pmcid>PMC9529776</pmcid><funding_grant_id>W81XWH-17-1-0373</funding_grant_id><funding_grant_id>RO1 CA120528-12</funding_grant_id><funding_grant_id>650320</funding_grant_id><funding_grant_id>R01 CA120528</funding_grant_id><funding_grant_id>R01 EB025964</funding_grant_id><pubmed_authors>Bueno R</pubmed_authors><pubmed_authors>Sholl LM</pubmed_authors><pubmed_authors>Barlow J</pubmed_authors><pubmed_authors>Chapel DB</pubmed_authors><pubmed_authors>Hornick JL</pubmed_authors></additional><is_claimable>false</is_claimable><name>Clinical and molecular validation of BAP1, MTAP, P53, and Merlin immunohistochemistry in diagnosis of pleural mesothelioma.</name><description>BAP1 and MTAP immunostains play an important role in diagnosis of mesothelioma, but additional markers are needed to increase sensitivity. We analyzed 84 pleural mesotheliomas (51 epithelioid, 27 biphasic, 6 sarcomatoid) by a hybrid-capture next-generation sequencing (NGS) panel including complete coverage of coding and splicing regions for BAP1, CDKN2A/MTAP, NF2, and TP53 and correlated molecular findings with diagnostic immunostains for BAP1, MTAP, Merlin, and p53, respectively. Fifty-seven reactive mesothelial proliferations served as benign comparators. Loss of BAP1, MTAP, and Merlin protein expression were, respectively, 54%, 46%, and 52% sensitive and 100% specific for mesothelioma. Two-marker immunopanels of BAP1 + MTAP, BAP1 + Merlin, and MTAP + Merlin were 79%, 85%, and 71% sensitive for mesothelioma, while a three-marker immunopanel of BAP1 + MTAP + Merlin was 90% sensitive. Diffuse (mutant-pattern) p53 immunostaining was seen in only 6 (7%) tumors but represented the only immunohistochemical abnormality in 2 cases. Null-pattern p53 was not specific for malignancy. An immunopanel of BAP1 + MTAP + Merlin + p53 was 93% sensitive for mesothelioma, and panel NGS detected a pathogenic alteration in BAP1, MTAP, NF2, and/or TP53 in 95%. Together, 83 (99%) of 84 tumors showed a diagnostic alteration by either immunohistochemistry or panel NGS. Adding Merlin to the standard BAP1 + MTAP immunopanel increases sensitivity for mesothelioma without sacrificing specificity. p53 immunohistochemistry and panel NGS with complete coverage of BAP1, CDKN2A/MTAP, TP53, and NF2 may be useful in diagnostically challenging cases.</description><dates><release>2022-01-01T00:00:00Z</release><publication>2022 Oct</publication><modification>2026-06-04T04:54:16.232Z</modification><creation>2025-02-19T04:20:26.385Z</creation></dates><accession>S-EPMC9529776</accession><cross_references><pubmed>35459788</pubmed><doi>10.1038/s41379-022-01081-z</doi></cross_references></HashMap>