Gauging NOTCH1 Activation in Cancer Using Immunohistochemistry.

Fixed, paraffin-embedded (FPE) tissues are a potentially rich resource for studying the role of NOTCH1 in cancer and other pathologies, but tests that reliably detect activated NOTCH1 (NICD1) in FPE samples have been lacking. Here, we bridge this gap by developing an immunohistochemical (IHC) stain...

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Main Authors: Michael J Kluk, Todd Ashworth, Hongfang Wang, Birgit Knoechel, Emily F Mason, Elizabeth A Morgan, David Dorfman, Geraldine Pinkus, Oliver Weigert, Jason L Hornick, Lucian R Chirieac, Michelle Hirsch, David J Oh, Andrew P South, Irene M Leigh, Celine Pourreyron, Andrew J Cassidy, Daniel J Deangelo, David M Weinstock, Ian E Krop, Deborah Dillon, Jane E Brock, Alexander J F Lazar, Myron Peto, Raymond J Cho, Alexander Stoeck, Brian B Haines, Sriram Sathayanrayanan, Scott Rodig, Jon C Aster
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3688991?pdf=render
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spelling doaj-32604a8825f6402bb5ed46051a8c0b7c2020-11-25T02:19:48ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0186e6730610.1371/journal.pone.0067306Gauging NOTCH1 Activation in Cancer Using Immunohistochemistry.Michael J KlukTodd AshworthHongfang WangBirgit KnoechelEmily F MasonElizabeth A MorganDavid DorfmanGeraldine PinkusOliver WeigertJason L HornickLucian R ChirieacMichelle HirschDavid J OhAndrew P SouthIrene M LeighCeline PourreyronAndrew J CassidyDaniel J DeangeloDavid M WeinstockIan E KropDeborah DillonJane E BrockAlexander J F LazarMyron PetoRaymond J ChoAlexander StoeckBrian B HainesSriram SathayanrayananScott RodigJon C AsterFixed, paraffin-embedded (FPE) tissues are a potentially rich resource for studying the role of NOTCH1 in cancer and other pathologies, but tests that reliably detect activated NOTCH1 (NICD1) in FPE samples have been lacking. Here, we bridge this gap by developing an immunohistochemical (IHC) stain that detects a neoepitope created by the proteolytic cleavage event that activates NOTCH1. Following validation using xenografted cancers and normal tissues with known patterns of NOTCH1 activation, we applied this test to tumors linked to dysregulated Notch signaling by mutational studies. As expected, frequent NICD1 staining was observed in T lymphoblastic leukemia/lymphoma, a tumor in which activating NOTCH1 mutations are common. However, when IHC was used to gauge NOTCH1 activation in other human cancers, several unexpected findings emerged. Among B cell tumors, NICD1 staining was much more frequent in chronic lymphocytic leukemia than would be predicted based on the frequency of NOTCH1 mutations, while mantle cell lymphoma and diffuse large B cell lymphoma showed no evidence of NOTCH1 activation. NICD1 was also detected in 38% of peripheral T cell lymphomas. Of interest, NICD1 staining in chronic lymphocytic leukemia cells and in angioimmunoblastic lymphoma was consistently more pronounced in lymph nodes than in surrounding soft tissues, implicating factors in the nodal microenvironment in NOTCH1 activation in these diseases. Among carcinomas, diffuse strong NICD1 staining was observed in 3.8% of cases of triple negative breast cancer (3 of 78 tumors), but was absent from 151 non-small cell lung carcinomas and 147 ovarian carcinomas. Frequent staining of normal endothelium was also observed; in line with this observation, strong NICD1 staining was also seen in 77% of angiosarcomas. These findings complement insights from genomic sequencing studies and suggest that IHC staining is a valuable experimental tool that may be useful in selection of patients for clinical trials.http://europepmc.org/articles/PMC3688991?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Michael J Kluk
Todd Ashworth
Hongfang Wang
Birgit Knoechel
Emily F Mason
Elizabeth A Morgan
David Dorfman
Geraldine Pinkus
Oliver Weigert
Jason L Hornick
Lucian R Chirieac
Michelle Hirsch
David J Oh
Andrew P South
Irene M Leigh
Celine Pourreyron
Andrew J Cassidy
Daniel J Deangelo
David M Weinstock
Ian E Krop
Deborah Dillon
Jane E Brock
Alexander J F Lazar
Myron Peto
Raymond J Cho
Alexander Stoeck
Brian B Haines
Sriram Sathayanrayanan
Scott Rodig
Jon C Aster
spellingShingle Michael J Kluk
Todd Ashworth
Hongfang Wang
Birgit Knoechel
Emily F Mason
Elizabeth A Morgan
David Dorfman
Geraldine Pinkus
Oliver Weigert
Jason L Hornick
Lucian R Chirieac
Michelle Hirsch
David J Oh
Andrew P South
Irene M Leigh
Celine Pourreyron
Andrew J Cassidy
Daniel J Deangelo
David M Weinstock
Ian E Krop
Deborah Dillon
Jane E Brock
Alexander J F Lazar
Myron Peto
Raymond J Cho
Alexander Stoeck
Brian B Haines
Sriram Sathayanrayanan
Scott Rodig
Jon C Aster
Gauging NOTCH1 Activation in Cancer Using Immunohistochemistry.
PLoS ONE
author_facet Michael J Kluk
Todd Ashworth
Hongfang Wang
Birgit Knoechel
Emily F Mason
Elizabeth A Morgan
David Dorfman
Geraldine Pinkus
Oliver Weigert
Jason L Hornick
Lucian R Chirieac
Michelle Hirsch
David J Oh
Andrew P South
Irene M Leigh
Celine Pourreyron
Andrew J Cassidy
Daniel J Deangelo
David M Weinstock
Ian E Krop
Deborah Dillon
Jane E Brock
Alexander J F Lazar
Myron Peto
Raymond J Cho
Alexander Stoeck
Brian B Haines
Sriram Sathayanrayanan
Scott Rodig
Jon C Aster
author_sort Michael J Kluk
title Gauging NOTCH1 Activation in Cancer Using Immunohistochemistry.
title_short Gauging NOTCH1 Activation in Cancer Using Immunohistochemistry.
title_full Gauging NOTCH1 Activation in Cancer Using Immunohistochemistry.
title_fullStr Gauging NOTCH1 Activation in Cancer Using Immunohistochemistry.
title_full_unstemmed Gauging NOTCH1 Activation in Cancer Using Immunohistochemistry.
title_sort gauging notch1 activation in cancer using immunohistochemistry.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Fixed, paraffin-embedded (FPE) tissues are a potentially rich resource for studying the role of NOTCH1 in cancer and other pathologies, but tests that reliably detect activated NOTCH1 (NICD1) in FPE samples have been lacking. Here, we bridge this gap by developing an immunohistochemical (IHC) stain that detects a neoepitope created by the proteolytic cleavage event that activates NOTCH1. Following validation using xenografted cancers and normal tissues with known patterns of NOTCH1 activation, we applied this test to tumors linked to dysregulated Notch signaling by mutational studies. As expected, frequent NICD1 staining was observed in T lymphoblastic leukemia/lymphoma, a tumor in which activating NOTCH1 mutations are common. However, when IHC was used to gauge NOTCH1 activation in other human cancers, several unexpected findings emerged. Among B cell tumors, NICD1 staining was much more frequent in chronic lymphocytic leukemia than would be predicted based on the frequency of NOTCH1 mutations, while mantle cell lymphoma and diffuse large B cell lymphoma showed no evidence of NOTCH1 activation. NICD1 was also detected in 38% of peripheral T cell lymphomas. Of interest, NICD1 staining in chronic lymphocytic leukemia cells and in angioimmunoblastic lymphoma was consistently more pronounced in lymph nodes than in surrounding soft tissues, implicating factors in the nodal microenvironment in NOTCH1 activation in these diseases. Among carcinomas, diffuse strong NICD1 staining was observed in 3.8% of cases of triple negative breast cancer (3 of 78 tumors), but was absent from 151 non-small cell lung carcinomas and 147 ovarian carcinomas. Frequent staining of normal endothelium was also observed; in line with this observation, strong NICD1 staining was also seen in 77% of angiosarcomas. These findings complement insights from genomic sequencing studies and suggest that IHC staining is a valuable experimental tool that may be useful in selection of patients for clinical trials.
url http://europepmc.org/articles/PMC3688991?pdf=render
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