Histological and molecular diversity and heterogeneity of precancerous lesions associated with inflammatory bowel diseases

Xianyong Gui; Xianyong Gui; Martin Köbel; Jose G.P. Ferraz; Marietta Iacucci; Subrata Ghosh; Shuhong Liu; Young Ou; Marco Perizzolo; Robert J. Winkfein; Peter Rambau; Douglas J. Demetrick

doi:10.1136/jclinpath-2019-206247

Histological and molecular diversity and heterogeneity of precancerous lesions associated with inflammatory bowel diseases

Xianyong Gui
, Xianyong Gui
, Martin Köbel
, Jose G.P. Ferraz
, Marietta Iacucci
, Subrata Ghosh
, Shuhong Liu
, Young Ou
, Marco Perizzolo
, Robert J. Winkfein
, Peter Rambau
, Douglas J. Demetrick

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

Abstract

Aims Inflammatory bowel disease (IBD)-associated precancerous lesions may be adenomatous or non-adenomatous with various histomorphologies. We aim to validate the newly proposed classification, to explore the neoplastic nature of the non-adenomatous lesions and to elucidate the molecular mechanisms underlying the different histomorphologies. Methods 44 background precursor lesions identified in 53 cases of surgically resected IBD-associated colorectal and ileal carcinomas were reviewed for the histomorphological features (classified into adenomatous, mucinous, sessile serrated adenoma (SSA)-like, traditional serrated adenoma-like, differentiated, eosinophilic and serrated not otherwise specified (NOS)) and analysed for a key panel of colonic cancer-related molecular markers. Results Approximately 60% of the lesions were adenomatous, of which some had mixed serrated, mucinous or eosinophilic changes. The remaining non-adenomatous lesions, including all other types except SSA-like type, mostly showed mixed features and focal adenomatous dysplasia. KRAS mutation and p53 mutant-type expression were found in about half cases across all types, while PIK3CA mutation only in some of adenomatous and eosinophilic lesions and MLH1/PMS2 loss in a subset of adenomatous, mucinous and eosinophilic but not in differentiated and serrated lesions. SAT-B2 or PTEN loss and IMP3 overexpression were seen in a small subset of lesions. No BRAF, NRAS or EGFR gene mutation was detected in any type. Certain molecular-morphological correlations were demonstrated; however, no single or combined molecular alteration(s) was specific to any particular morphological type. Conclusions IBD-associated precancerous lesions are heterogeneous both histologically and molecularly. True colitis-associated adenomatous lesions are unlikely conventional adenomas. Non-adenomatous lesions without frank cytologic dysplasia should also be regarded as neoplastic.

Original language	English
Pages (from-to)	391-402
Number of pages	12
Journal	Journal of Clinical Pathology
Volume	73
Issue number	7
DOIs	https://doi.org/10.1136/jclinpath-2019-206247
Publication status	Published - 1 Jul 2020
Externally published	Yes

Keywords

colorectal cancer
genetics
gut pathology
inflammatory bowel disease
oncogenes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1136/jclinpath-2019-206247

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Gui, X., Gui, X., Köbel, M., Ferraz, J. G. P., Iacucci, M., Ghosh, S., Liu, S., Ou, Y., Perizzolo, M., Winkfein, R. J., Rambau, P., & Demetrick, D. J. (2020). Histological and molecular diversity and heterogeneity of precancerous lesions associated with inflammatory bowel diseases. Journal of Clinical Pathology, 73(7), 391-402. https://doi.org/10.1136/jclinpath-2019-206247

@article{7170c340c7fe410e8aa1aa43befe324c,

title = "Histological and molecular diversity and heterogeneity of precancerous lesions associated with inflammatory bowel diseases",

abstract = "Aims Inflammatory bowel disease (IBD)-associated precancerous lesions may be adenomatous or non-adenomatous with various histomorphologies. We aim to validate the newly proposed classification, to explore the neoplastic nature of the non-adenomatous lesions and to elucidate the molecular mechanisms underlying the different histomorphologies. Methods 44 background precursor lesions identified in 53 cases of surgically resected IBD-associated colorectal and ileal carcinomas were reviewed for the histomorphological features (classified into adenomatous, mucinous, sessile serrated adenoma (SSA)-like, traditional serrated adenoma-like, differentiated, eosinophilic and serrated not otherwise specified (NOS)) and analysed for a key panel of colonic cancer-related molecular markers. Results Approximately 60\% of the lesions were adenomatous, of which some had mixed serrated, mucinous or eosinophilic changes. The remaining non-adenomatous lesions, including all other types except SSA-like type, mostly showed mixed features and focal adenomatous dysplasia. KRAS mutation and p53 mutant-type expression were found in about half cases across all types, while PIK3CA mutation only in some of adenomatous and eosinophilic lesions and MLH1/PMS2 loss in a subset of adenomatous, mucinous and eosinophilic but not in differentiated and serrated lesions. SAT-B2 or PTEN loss and IMP3 overexpression were seen in a small subset of lesions. No BRAF, NRAS or EGFR gene mutation was detected in any type. Certain molecular-morphological correlations were demonstrated; however, no single or combined molecular alteration(s) was specific to any particular morphological type. Conclusions IBD-associated precancerous lesions are heterogeneous both histologically and molecularly. True colitis-associated adenomatous lesions are unlikely conventional adenomas. Non-adenomatous lesions without frank cytologic dysplasia should also be regarded as neoplastic.",

keywords = "colorectal cancer, genetics, gut pathology, inflammatory bowel disease, oncogenes",

author = "Xianyong Gui and Xianyong Gui and Martin K{\"o}bel and Ferraz, \{Jose G.P.\} and Marietta Iacucci and Subrata Ghosh and Shuhong Liu and Young Ou and Marco Perizzolo and Winkfein, \{Robert J.\} and Peter Rambau and Demetrick, \{Douglas J.\}",

note = "Publisher Copyright: {\textcopyright} Author(s) (or their employer(s)) 2020. No commercial re-use. See rights and permissions. Published by BMJ.",

year = "2020",

month = jul,

day = "1",

doi = "10.1136/jclinpath-2019-206247",

language = "English",

volume = "73",

pages = "391--402",

journal = "Journal of Clinical Pathology",

issn = "0021-9746",

publisher = "BMJ Publishing Group",

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TY - JOUR

T1 - Histological and molecular diversity and heterogeneity of precancerous lesions associated with inflammatory bowel diseases

AU - Gui, Xianyong

AU - Köbel, Martin

AU - Ferraz, Jose G.P.

AU - Iacucci, Marietta

AU - Ghosh, Subrata

AU - Liu, Shuhong

AU - Ou, Young

AU - Perizzolo, Marco

AU - Winkfein, Robert J.

AU - Rambau, Peter

AU - Demetrick, Douglas J.

N1 - Publisher Copyright: © Author(s) (or their employer(s)) 2020. No commercial re-use. See rights and permissions. Published by BMJ.

PY - 2020/7/1

Y1 - 2020/7/1

N2 - Aims Inflammatory bowel disease (IBD)-associated precancerous lesions may be adenomatous or non-adenomatous with various histomorphologies. We aim to validate the newly proposed classification, to explore the neoplastic nature of the non-adenomatous lesions and to elucidate the molecular mechanisms underlying the different histomorphologies. Methods 44 background precursor lesions identified in 53 cases of surgically resected IBD-associated colorectal and ileal carcinomas were reviewed for the histomorphological features (classified into adenomatous, mucinous, sessile serrated adenoma (SSA)-like, traditional serrated adenoma-like, differentiated, eosinophilic and serrated not otherwise specified (NOS)) and analysed for a key panel of colonic cancer-related molecular markers. Results Approximately 60% of the lesions were adenomatous, of which some had mixed serrated, mucinous or eosinophilic changes. The remaining non-adenomatous lesions, including all other types except SSA-like type, mostly showed mixed features and focal adenomatous dysplasia. KRAS mutation and p53 mutant-type expression were found in about half cases across all types, while PIK3CA mutation only in some of adenomatous and eosinophilic lesions and MLH1/PMS2 loss in a subset of adenomatous, mucinous and eosinophilic but not in differentiated and serrated lesions. SAT-B2 or PTEN loss and IMP3 overexpression were seen in a small subset of lesions. No BRAF, NRAS or EGFR gene mutation was detected in any type. Certain molecular-morphological correlations were demonstrated; however, no single or combined molecular alteration(s) was specific to any particular morphological type. Conclusions IBD-associated precancerous lesions are heterogeneous both histologically and molecularly. True colitis-associated adenomatous lesions are unlikely conventional adenomas. Non-adenomatous lesions without frank cytologic dysplasia should also be regarded as neoplastic.

AB - Aims Inflammatory bowel disease (IBD)-associated precancerous lesions may be adenomatous or non-adenomatous with various histomorphologies. We aim to validate the newly proposed classification, to explore the neoplastic nature of the non-adenomatous lesions and to elucidate the molecular mechanisms underlying the different histomorphologies. Methods 44 background precursor lesions identified in 53 cases of surgically resected IBD-associated colorectal and ileal carcinomas were reviewed for the histomorphological features (classified into adenomatous, mucinous, sessile serrated adenoma (SSA)-like, traditional serrated adenoma-like, differentiated, eosinophilic and serrated not otherwise specified (NOS)) and analysed for a key panel of colonic cancer-related molecular markers. Results Approximately 60% of the lesions were adenomatous, of which some had mixed serrated, mucinous or eosinophilic changes. The remaining non-adenomatous lesions, including all other types except SSA-like type, mostly showed mixed features and focal adenomatous dysplasia. KRAS mutation and p53 mutant-type expression were found in about half cases across all types, while PIK3CA mutation only in some of adenomatous and eosinophilic lesions and MLH1/PMS2 loss in a subset of adenomatous, mucinous and eosinophilic but not in differentiated and serrated lesions. SAT-B2 or PTEN loss and IMP3 overexpression were seen in a small subset of lesions. No BRAF, NRAS or EGFR gene mutation was detected in any type. Certain molecular-morphological correlations were demonstrated; however, no single or combined molecular alteration(s) was specific to any particular morphological type. Conclusions IBD-associated precancerous lesions are heterogeneous both histologically and molecularly. True colitis-associated adenomatous lesions are unlikely conventional adenomas. Non-adenomatous lesions without frank cytologic dysplasia should also be regarded as neoplastic.

KW - colorectal cancer

KW - genetics

KW - gut pathology

KW - inflammatory bowel disease

KW - oncogenes

UR - https://www.scopus.com/pages/publications/85076136576

U2 - 10.1136/jclinpath-2019-206247

DO - 10.1136/jclinpath-2019-206247

M3 - Article

C2 - 31801800

AN - SCOPUS:85076136576

SN - 0021-9746

VL - 73

SP - 391

EP - 402

JO - Journal of Clinical Pathology

JF - Journal of Clinical Pathology

IS - 7

ER -

Histological and molecular diversity and heterogeneity of precancerous lesions associated with inflammatory bowel diseases

Abstract

Keywords

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