Genomic characterization of hepatoid tumors: context matters

Rita T Lawlor; Andrea Mafficini; Concetta Sciammarella; Cinzia Cantù; Borislav C Rusev; Maria L Piredda; Davide Antonello; Sonia Grimaldi; Giada Bonizzato; Nicola Sperandio; Giovanni Marchegiani; Giuseppe Malleo; Antonio Pea; Roberto Salvia; Aldo Mombello; Guido Mazzoleni; Alessia Nottegar; Esther Hanspeter; Giulio Riva; Anna Tomezzoli; Maria Bencivenga; Giovanni de Manzoni; Serena Pedron; Gaetano Paolino; Paola Mattiolo; Lodewijk A Brosens; Nicola Silvestris; Matteo Fassan; Susanna L Cooke; Philip A Beer; Michele Milella; Volkan N Adsay; Liang Cheng; Aldo Scarpa; Claudio Luchini

doi:10.1016/j.humpath.2021.09.006

Genomic characterization of hepatoid tumors: context matters

Rita T Lawlor, Andrea Mafficini, Concetta Sciammarella, Cinzia Cantù, Borislav C Rusev, Maria L Piredda, Davide Antonello, Sonia Grimaldi, Giada Bonizzato, Nicola Sperandio, Giovanni Marchegiani, Giuseppe Malleo, Antonio Pea, Roberto Salvia, Aldo Mombello, Guido Mazzoleni, Alessia Nottegar, Esther Hanspeter, Giulio Riva, Anna TomezzoliMaria Bencivenga, Giovanni de Manzoni, Serena Pedron, Gaetano Paolino, Paola Mattiolo, Lodewijk A Brosens, Nicola Silvestris, Matteo Fassan, Susanna L Cooke, Philip A Beer, Michele Milella, Volkan N Adsay, Liang Cheng, Aldo Scarpa, Claudio Luchini

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Hepatoid tumors (HT) are rare neoplasms morphologically resembling hepatocellular carcinoma, which arise in several organs other than the liver. A comprehensive molecular profile of this group of neoplasms is still lacking. Genomic characterization of 19 HTs from different organs (three colon HTs, four esophagogastric HTs, four biliary HTs, six genitourinary HTs, two lung HTs) was performed using a multigene next-generation sequencing panel. NGS unraveled a composite molecular profile of HT. Their genetic alterations were clearly clustered by tumor site: (i) colorectal HT displayed microsatellite instability, high tumor mutational burden, mutations in ARID1A/B genes and NCOA4-RET gene fusion (2/3 cases); (ii) gastric HT had TP53 mutations (2/4); (iii) biliary HT displayed loss of CDKN2A (3/4) and loss of chromosome 18 (2/4); (iv) genital HT showed gain of chromosome 12 (3/6); (v) lung HT had STK11 somatic mutations (2/2). The only commonly mutated gene occurring in HT of different sites was TP53 (8/19 cases: colon 2, esophagogastric 2, biliary 2, genital 1, lungs 1). This study shows that most genetic alterations of HT were clustered by site, indicating that context matters. The novel potential targets for HT precision oncology are also clustered based on the anatomic origin. This study shed light on the biology of these rare cancers and may have important consequences for treatment decisions and clinical trial selection for HT patients.

Original language	English
Pages (from-to)	30-41
Number of pages	12
Journal	Human Pathology
Volume	118
Early online date	22 Sept 2021
DOIs	https://doi.org/10.1016/j.humpath.2021.09.006
Publication status	Published - Dec 2021

Keywords

Adult
Aged
Aged, 80 and over
Carcinoma/genetics
Digestive System Neoplasms/genetics
Female
Hepatoid
Humans
Lung Neoplasms/genetics
Male
Microsatellite instability
Middle Aged
NGS
RET fusions
STK11
Urogenital Neoplasms/genetics

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10.1016/j.humpath.2021.09.006

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Lawlor, R. T., Mafficini, A., Sciammarella, C., Cantù, C., Rusev, B. C., Piredda, M. L., Antonello, D., Grimaldi, S., Bonizzato, G., Sperandio, N., Marchegiani, G., Malleo, G., Pea, A., Salvia, R., Mombello, A., Mazzoleni, G., Nottegar, A., Hanspeter, E., Riva, G., ... Luchini, C. (2021). Genomic characterization of hepatoid tumors: context matters. Human Pathology, 118, 30-41. https://doi.org/10.1016/j.humpath.2021.09.006

@article{2c0cad0bdb8847069eb45538dbef3057,

title = "Genomic characterization of hepatoid tumors: context matters",

abstract = "Hepatoid tumors (HT) are rare neoplasms morphologically resembling hepatocellular carcinoma, which arise in several organs other than the liver. A comprehensive molecular profile of this group of neoplasms is still lacking. Genomic characterization of 19 HTs from different organs (three colon HTs, four esophagogastric HTs, four biliary HTs, six genitourinary HTs, two lung HTs) was performed using a multigene next-generation sequencing panel. NGS unraveled a composite molecular profile of HT. Their genetic alterations were clearly clustered by tumor site: (i) colorectal HT displayed microsatellite instability, high tumor mutational burden, mutations in ARID1A/B genes and NCOA4-RET gene fusion (2/3 cases); (ii) gastric HT had TP53 mutations (2/4); (iii) biliary HT displayed loss of CDKN2A (3/4) and loss of chromosome 18 (2/4); (iv) genital HT showed gain of chromosome 12 (3/6); (v) lung HT had STK11 somatic mutations (2/2). The only commonly mutated gene occurring in HT of different sites was TP53 (8/19 cases: colon 2, esophagogastric 2, biliary 2, genital 1, lungs 1). This study shows that most genetic alterations of HT were clustered by site, indicating that context matters. The novel potential targets for HT precision oncology are also clustered based on the anatomic origin. This study shed light on the biology of these rare cancers and may have important consequences for treatment decisions and clinical trial selection for HT patients.",

keywords = "Adult, Aged, Aged, 80 and over, Carcinoma/genetics, Digestive System Neoplasms/genetics, Female, Hepatoid, Humans, Lung Neoplasms/genetics, Male, Microsatellite instability, Middle Aged, NGS, RET fusions, STK11, Urogenital Neoplasms/genetics",

author = "Lawlor, {Rita T} and Andrea Mafficini and Concetta Sciammarella and Cinzia Cant{\`u} and Rusev, {Borislav C} and Piredda, {Maria L} and Davide Antonello and Sonia Grimaldi and Giada Bonizzato and Nicola Sperandio and Giovanni Marchegiani and Giuseppe Malleo and Antonio Pea and Roberto Salvia and Aldo Mombello and Guido Mazzoleni and Alessia Nottegar and Esther Hanspeter and Giulio Riva and Anna Tomezzoli and Maria Bencivenga and {de Manzoni}, Giovanni and Serena Pedron and Gaetano Paolino and Paola Mattiolo and Brosens, {Lodewijk A} and Nicola Silvestris and Matteo Fassan and Cooke, {Susanna L} and Beer, {Philip A} and Michele Milella and Adsay, {Volkan N} and Liang Cheng and Aldo Scarpa and Claudio Luchini",

note = "Publisher Copyright: {\textcopyright} 2021 Elsevier Inc.",

year = "2021",

month = dec,

doi = "10.1016/j.humpath.2021.09.006",

language = "English",

volume = "118",

pages = "30--41",

journal = "Human Pathology",

issn = "0046-8177",

publisher = "W.B. Saunders",

}

Lawlor, RT, Mafficini, A, Sciammarella, C, Cantù, C, Rusev, BC, Piredda, ML, Antonello, D, Grimaldi, S, Bonizzato, G, Sperandio, N, Marchegiani, G, Malleo, G, Pea, A, Salvia, R, Mombello, A, Mazzoleni, G, Nottegar, A, Hanspeter, E, Riva, G, Tomezzoli, A, Bencivenga, M, de Manzoni, G, Pedron, S, Paolino, G, Mattiolo, P, Brosens, LA, Silvestris, N, Fassan, M, Cooke, SL, Beer, PA, Milella, M, Adsay, VN, Cheng, L, Scarpa, A & Luchini, C 2021, 'Genomic characterization of hepatoid tumors: context matters', Human Pathology, vol. 118, pp. 30-41. https://doi.org/10.1016/j.humpath.2021.09.006

TY - JOUR

T1 - Genomic characterization of hepatoid tumors

T2 - context matters

AU - Lawlor, Rita T

AU - Mafficini, Andrea

AU - Sciammarella, Concetta

AU - Cantù, Cinzia

AU - Rusev, Borislav C

AU - Piredda, Maria L

AU - Antonello, Davide

AU - Grimaldi, Sonia

AU - Bonizzato, Giada

AU - Sperandio, Nicola

AU - Marchegiani, Giovanni

AU - Malleo, Giuseppe

AU - Pea, Antonio

AU - Salvia, Roberto

AU - Mombello, Aldo

AU - Mazzoleni, Guido

AU - Nottegar, Alessia

AU - Hanspeter, Esther

AU - Riva, Giulio

AU - Tomezzoli, Anna

AU - Bencivenga, Maria

AU - de Manzoni, Giovanni

AU - Pedron, Serena

AU - Paolino, Gaetano

AU - Mattiolo, Paola

AU - Brosens, Lodewijk A

AU - Silvestris, Nicola

AU - Fassan, Matteo

AU - Cooke, Susanna L

AU - Beer, Philip A

AU - Milella, Michele

AU - Adsay, Volkan N

AU - Cheng, Liang

AU - Scarpa, Aldo

AU - Luchini, Claudio

PY - 2021/12

Y1 - 2021/12

N2 - Hepatoid tumors (HT) are rare neoplasms morphologically resembling hepatocellular carcinoma, which arise in several organs other than the liver. A comprehensive molecular profile of this group of neoplasms is still lacking. Genomic characterization of 19 HTs from different organs (three colon HTs, four esophagogastric HTs, four biliary HTs, six genitourinary HTs, two lung HTs) was performed using a multigene next-generation sequencing panel. NGS unraveled a composite molecular profile of HT. Their genetic alterations were clearly clustered by tumor site: (i) colorectal HT displayed microsatellite instability, high tumor mutational burden, mutations in ARID1A/B genes and NCOA4-RET gene fusion (2/3 cases); (ii) gastric HT had TP53 mutations (2/4); (iii) biliary HT displayed loss of CDKN2A (3/4) and loss of chromosome 18 (2/4); (iv) genital HT showed gain of chromosome 12 (3/6); (v) lung HT had STK11 somatic mutations (2/2). The only commonly mutated gene occurring in HT of different sites was TP53 (8/19 cases: colon 2, esophagogastric 2, biliary 2, genital 1, lungs 1). This study shows that most genetic alterations of HT were clustered by site, indicating that context matters. The novel potential targets for HT precision oncology are also clustered based on the anatomic origin. This study shed light on the biology of these rare cancers and may have important consequences for treatment decisions and clinical trial selection for HT patients.

AB - Hepatoid tumors (HT) are rare neoplasms morphologically resembling hepatocellular carcinoma, which arise in several organs other than the liver. A comprehensive molecular profile of this group of neoplasms is still lacking. Genomic characterization of 19 HTs from different organs (three colon HTs, four esophagogastric HTs, four biliary HTs, six genitourinary HTs, two lung HTs) was performed using a multigene next-generation sequencing panel. NGS unraveled a composite molecular profile of HT. Their genetic alterations were clearly clustered by tumor site: (i) colorectal HT displayed microsatellite instability, high tumor mutational burden, mutations in ARID1A/B genes and NCOA4-RET gene fusion (2/3 cases); (ii) gastric HT had TP53 mutations (2/4); (iii) biliary HT displayed loss of CDKN2A (3/4) and loss of chromosome 18 (2/4); (iv) genital HT showed gain of chromosome 12 (3/6); (v) lung HT had STK11 somatic mutations (2/2). The only commonly mutated gene occurring in HT of different sites was TP53 (8/19 cases: colon 2, esophagogastric 2, biliary 2, genital 1, lungs 1). This study shows that most genetic alterations of HT were clustered by site, indicating that context matters. The novel potential targets for HT precision oncology are also clustered based on the anatomic origin. This study shed light on the biology of these rare cancers and may have important consequences for treatment decisions and clinical trial selection for HT patients.

KW - Adult

KW - Aged

KW - Aged, 80 and over

KW - Carcinoma/genetics

KW - Digestive System Neoplasms/genetics

KW - Female

KW - Hepatoid

KW - Humans

KW - Lung Neoplasms/genetics

KW - Male

KW - Microsatellite instability

KW - Middle Aged

KW - NGS

KW - RET fusions

KW - STK11

KW - Urogenital Neoplasms/genetics

U2 - 10.1016/j.humpath.2021.09.006

DO - 10.1016/j.humpath.2021.09.006

M3 - Article

C2 - 34562502

SN - 0046-8177

VL - 118

SP - 30

EP - 41

JO - Human Pathology

JF - Human Pathology

ER -

Genomic characterization of hepatoid tumors: context matters

Abstract

Keywords

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