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Coexpression of ΔNp63/p40 and TTF1 Within Most of the Same Individual Cells Identifies Life-Threatening NSCLC Featuring Squamous and Glandular Biphenotypic Differentiation: Clinicopathologic Correlations

INTRODUCTION: Double occurrence of TTF1 and ΔNp63/p40 (henceforth, p40) within the same individual cells is exceedingly rare in lung cancer. Little is known on their biological and clinical implications. METHODS: Two index cases immunoreactive for both p40 and TTF1 and nine tumors selected from The...

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Autores principales: Pelosi, Giuseppe, Bulloni, Matteo, Vescio, Martina, Uccella, Silvia, Forest, Fabien, Leone, Giorgia, Barberis, Massimo, Rahal, Daoud, Bossi, Paola, Finzi, Giovanna, Marchiori, Deborah, De Luca, Marco, Sessa, Fausto, Harari, Sergio, Spinelli, Manuela, Viola, Patrizia, Macrì, Paolo, Maria, Stefania, Rizzo, Antonio, Picone, Antonio, Pattini, Linda
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8551500/
https://www.ncbi.nlm.nih.gov/pubmed/34746884
http://dx.doi.org/10.1016/j.jtocrr.2021.100222
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author Pelosi, Giuseppe
Bulloni, Matteo
Vescio, Martina
Uccella, Silvia
Forest, Fabien
Leone, Giorgia
Barberis, Massimo
Rahal, Daoud
Bossi, Paola
Finzi, Giovanna
Marchiori, Deborah
De Luca, Marco
Sessa, Fausto
Harari, Sergio
Spinelli, Manuela
Viola, Patrizia
Macrì, Paolo
Maria, Stefania
Rizzo, Antonio
Picone, Antonio
Pattini, Linda
author_facet Pelosi, Giuseppe
Bulloni, Matteo
Vescio, Martina
Uccella, Silvia
Forest, Fabien
Leone, Giorgia
Barberis, Massimo
Rahal, Daoud
Bossi, Paola
Finzi, Giovanna
Marchiori, Deborah
De Luca, Marco
Sessa, Fausto
Harari, Sergio
Spinelli, Manuela
Viola, Patrizia
Macrì, Paolo
Maria, Stefania
Rizzo, Antonio
Picone, Antonio
Pattini, Linda
author_sort Pelosi, Giuseppe
collection PubMed
description INTRODUCTION: Double occurrence of TTF1 and ΔNp63/p40 (henceforth, p40) within the same individual cells is exceedingly rare in lung cancer. Little is known on their biological and clinical implications. METHODS: Two index cases immunoreactive for both p40 and TTF1 and nine tumors selected from The Cancer Genome Atlas (TCGA) according to the mRNA levels of the two relevant genes entered the study. RESULTS: The two index cases were peripherally located, poorly differentiated, and behaviorally unfavorable carcinomas, which shared widespread p40 and TTF1 decoration within the same individual tumor cells. They also retained SMARCA2 and SMARCA4 expression, while variably stained for p53, cytokeratin 5, and programmed death-ligand 1. A subset of basal cells p40+/TTF1+ could be found in normal distal airways. Biphenotypic glandular and squamous differentiation was unveiled by electron microscopy, along with EGFR, RAD51B, CCND3, or NF1 mutations and IGF1R, MYC, CCND1, or CDK2 copy number variations on next-generation sequencing analysis. The nine tumors from TCGA (0.88% of 1018 tumors) shared the same poor prognosis, clinical presentation, and challenging histology and had activated pathways of enhanced angiogenesis and epithelial-mesenchymal transition. Mutation and copy number variation profiles did not differ from the other TCGA tumors. CONCLUSIONS: Double p40+/TTF1+ lung carcinomas are aggressive and likely underrecognized non–small cell carcinomas, whose origin could reside in double-positive distal airway stem-like basal cells through either de novo-basal-like or differentiating cell mechanisms according to a model of epithelial renewal.
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spelling pubmed-85515002021-11-04 Coexpression of ΔNp63/p40 and TTF1 Within Most of the Same Individual Cells Identifies Life-Threatening NSCLC Featuring Squamous and Glandular Biphenotypic Differentiation: Clinicopathologic Correlations Pelosi, Giuseppe Bulloni, Matteo Vescio, Martina Uccella, Silvia Forest, Fabien Leone, Giorgia Barberis, Massimo Rahal, Daoud Bossi, Paola Finzi, Giovanna Marchiori, Deborah De Luca, Marco Sessa, Fausto Harari, Sergio Spinelli, Manuela Viola, Patrizia Macrì, Paolo Maria, Stefania Rizzo, Antonio Picone, Antonio Pattini, Linda JTO Clin Res Rep Brief Report INTRODUCTION: Double occurrence of TTF1 and ΔNp63/p40 (henceforth, p40) within the same individual cells is exceedingly rare in lung cancer. Little is known on their biological and clinical implications. METHODS: Two index cases immunoreactive for both p40 and TTF1 and nine tumors selected from The Cancer Genome Atlas (TCGA) according to the mRNA levels of the two relevant genes entered the study. RESULTS: The two index cases were peripherally located, poorly differentiated, and behaviorally unfavorable carcinomas, which shared widespread p40 and TTF1 decoration within the same individual tumor cells. They also retained SMARCA2 and SMARCA4 expression, while variably stained for p53, cytokeratin 5, and programmed death-ligand 1. A subset of basal cells p40+/TTF1+ could be found in normal distal airways. Biphenotypic glandular and squamous differentiation was unveiled by electron microscopy, along with EGFR, RAD51B, CCND3, or NF1 mutations and IGF1R, MYC, CCND1, or CDK2 copy number variations on next-generation sequencing analysis. The nine tumors from TCGA (0.88% of 1018 tumors) shared the same poor prognosis, clinical presentation, and challenging histology and had activated pathways of enhanced angiogenesis and epithelial-mesenchymal transition. Mutation and copy number variation profiles did not differ from the other TCGA tumors. CONCLUSIONS: Double p40+/TTF1+ lung carcinomas are aggressive and likely underrecognized non–small cell carcinomas, whose origin could reside in double-positive distal airway stem-like basal cells through either de novo-basal-like or differentiating cell mechanisms according to a model of epithelial renewal. Elsevier 2021-09-02 /pmc/articles/PMC8551500/ /pubmed/34746884 http://dx.doi.org/10.1016/j.jtocrr.2021.100222 Text en © 2021 THE AUTHORS https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Brief Report
Pelosi, Giuseppe
Bulloni, Matteo
Vescio, Martina
Uccella, Silvia
Forest, Fabien
Leone, Giorgia
Barberis, Massimo
Rahal, Daoud
Bossi, Paola
Finzi, Giovanna
Marchiori, Deborah
De Luca, Marco
Sessa, Fausto
Harari, Sergio
Spinelli, Manuela
Viola, Patrizia
Macrì, Paolo
Maria, Stefania
Rizzo, Antonio
Picone, Antonio
Pattini, Linda
Coexpression of ΔNp63/p40 and TTF1 Within Most of the Same Individual Cells Identifies Life-Threatening NSCLC Featuring Squamous and Glandular Biphenotypic Differentiation: Clinicopathologic Correlations
title Coexpression of ΔNp63/p40 and TTF1 Within Most of the Same Individual Cells Identifies Life-Threatening NSCLC Featuring Squamous and Glandular Biphenotypic Differentiation: Clinicopathologic Correlations
title_full Coexpression of ΔNp63/p40 and TTF1 Within Most of the Same Individual Cells Identifies Life-Threatening NSCLC Featuring Squamous and Glandular Biphenotypic Differentiation: Clinicopathologic Correlations
title_fullStr Coexpression of ΔNp63/p40 and TTF1 Within Most of the Same Individual Cells Identifies Life-Threatening NSCLC Featuring Squamous and Glandular Biphenotypic Differentiation: Clinicopathologic Correlations
title_full_unstemmed Coexpression of ΔNp63/p40 and TTF1 Within Most of the Same Individual Cells Identifies Life-Threatening NSCLC Featuring Squamous and Glandular Biphenotypic Differentiation: Clinicopathologic Correlations
title_short Coexpression of ΔNp63/p40 and TTF1 Within Most of the Same Individual Cells Identifies Life-Threatening NSCLC Featuring Squamous and Glandular Biphenotypic Differentiation: Clinicopathologic Correlations
title_sort coexpression of δnp63/p40 and ttf1 within most of the same individual cells identifies life-threatening nsclc featuring squamous and glandular biphenotypic differentiation: clinicopathologic correlations
topic Brief Report
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8551500/
https://www.ncbi.nlm.nih.gov/pubmed/34746884
http://dx.doi.org/10.1016/j.jtocrr.2021.100222
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