AI Article Synopsis

  • SMARCA4/BRG1 protein-deficient lung adenocarcinomas and thoracic sarcomas lack clear histological features, making current diagnostic classifications often inadequate and leading to misdiagnosis as non-small cell carcinoma-not otherwise specified (NSCC-NOS).
  • The study tests lung biopsies for BRG1 protein deficiency and evaluates these tumors using immunohistochemistry, identifying nine cases with this deficiency, including six lung adenocarcinomas and three thoracic sarcomas.
  • The findings indicate that traditional morphology-based diagnosis is insufficient, prompting the need for a new diagnostic pathway to better identify and research these tumors for potential biomarkers and treatment options.

Article Abstract

Background: SMARCA4/BRG1 protein-deficient lung adenocarcinomas and thoracic sarcoma are recently described entities that lack distinctive histological features, transcription termination factor 1 (TTF1) reactivity, and actionable driver mutations. The current diagnostic path for small lung biopsies as recommended by the World Health Organization (WHO, 2015) is likely to categorize these as non- small cell carcinoma-not otherwise specified (NSCC-NOS). The present study attempts to define the subtle but distinctive clinicopathologic features of SMARCA4/BRG1 protein-deficient thoracic tumors; highlight their unique biology; and addresses the unmet need to segregate these using a new, tissue-proficient diagnostic pathway.

Methods: All lung biopsies and those from metastatic sites in patients with suspected advanced lung cancer and classified as NSCC-NOS as per WHO (2015) guidelines were subjected to BRG1 testing by immunohistochemistry. SMARCA4/BRG1 protein-deficient thoracic tumors were evaluated by an extended immunohistochemistry panel. Predictive biomarker and programmed death-ligand 1 testing was conducted in all cases.

Results: Of 110 cases, nine were found to be SMARCA4/BRG1 protein-deficient; six were identified as SMARCA4/BRG1 protein-deficient lung adenocarcinomas, and three were SMARCA4/BRG1 protein-deficient thoracic sarcomas. The histology ranged from poorly differentiated to undifferentiated to rhabdoid. None of the cases showed significant expression of TTF1 or p40, and no actionable mutation was identified.

Conclusions: It is difficult to separate BRG1-deficient lung adenocarcinomas and thoracic sarcomas based on morphology alone. We propose a diagnostic pathway for small biopsies of thoracic tumors to segregate these distinct entities so that they can be studied more efficaciously for new biomarkers and therapeutic options.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8476316PMC
http://dx.doi.org/10.4132/jptm.2021.05.11DOI Listing

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