Measuring ERCC1 protein expression in cancer specimens: Validation of a novel antibody

D. H. Smith; A. M. K. Fiehn; L. Fogh; I. J. Christensen; T. P. Hansen; J. Stenvang; H. J. Nielsen; K. V. Nielsen; J. P. Hasselby; N. Brunner; S. S. Jensen

doi:10.1038/srep04313

Measuring ERCC1 protein expression in cancer specimens: Validation of a novel antibody

D. H. Smith
, A. M. K. Fiehn
, L. Fogh
, I. J. Christensen
, T. P. Hansen
, J. Stenvang
, H. J. Nielsen
, K. V. Nielsen
, J. P. Hasselby
, N. Brunner
, S. S. Jensen

KI, OUH, Forskningsenhed for Patologi (Odense)

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

Abstract

Platinum chemotherapy remains part of standard therapies in the management of a variety of cancers. Severe side effects and a high degree of resistance to platinum drugs have led numerous researchers to search for predictive biomarkers, which could aid in identifying patients that are the most likely to respond to therapy. The ERCC1-ERCC4 endonuclease plays a critical role in the repair of platinum-DNA damage and has widely been studied in relation to sensitivity to platinum chemotherapy. The standard method to evaluate ERCC1 protein expression is through the use of immunohistochemistry with monoclonal antibody 8F1, an antibody that was recently found to bind an unrelated protein. The present study determines the specificity of a novel antibody, monoclonal antibody 4F9, and presents a method to evaluate ERCC1 expression in colorectal tumor specimens. Using relevant cell lines as controls, the specificity of antibody 4F9 was tested by immunoblotting, immunohistochemistry and immunofluorescence. Scoring guidelines to aid in the evaluation of ERCC1 tumor expression were developed and evaluated in archival formalin-fixed paraffin embedded colorectal cancer specimens. Antibody 4F9 was found to be specific by all methods applied and it was possible to evaluate the ERCC1 expression in the majority (85%) of colorectal cancer tumor specimens.

Originalsprog	Engelsk
Artikelnummer	4313
Tidsskrift	Scientific Reports
Vol/bind	4
ISSN	2045-2322
DOI	https://doi.org/10.1038/srep04313
Status	Udgivet - 2014

Bibliografisk note

ISI Document Delivery No.: AC2WC Times Cited: 1 Cited Reference Count: 37 Smith, David Hersi Fiehn, Anne-Marie Kanstrup Fogh, Louise Christensen, Ib Jarle Hansen, Tine Plato Stenvang, Jan Nielsen, Hans Jorgen Nielsen, Kirsten Vang Hasselby, Jane Preuss Brunner, Nils Jensen, Sussie Steen Danish Agency for Science, Technology and Innovation through the Industrial PhD program; Danish Strategic Research Council; Danish Cancer Society; Kathrine og Vigo Skovgaards Foundation This study was supported by the Danish Agency for Science, Technology and Innovation through the Industrial PhD program. Nils Brunner and Hans Jorgen Nielsen were supported by the Danish Strategic Research Council, the Danish Cancer Society, and Kathrine og Vigo Skovgaards Foundation. We would like to thank laboratory technicians Birgitte Jepsen and Signe Lykke Nielsen, as well as research scientists Kathy Kamath, Tatiana Okouneva and Jesper Lohse for their expertise and advice. 1 NATURE PUBLISHING GROUP LONDON SCI REP-UK

Dokumenter og links

10.1038/srep04313

SDU link

Tjek adgangen til materialet i Syddansk Universitetsbiblioteks søgemaskine

Citationsformater

@article{e7e0e884acb542f185102e6ed981b6a4,

title = "Measuring ERCC1 protein expression in cancer specimens: Validation of a novel antibody",

abstract = "Platinum chemotherapy remains part of standard therapies in the management of a variety of cancers. Severe side effects and a high degree of resistance to platinum drugs have led numerous researchers to search for predictive biomarkers, which could aid in identifying patients that are the most likely to respond to therapy. The ERCC1-ERCC4 endonuclease plays a critical role in the repair of platinum-DNA damage and has widely been studied in relation to sensitivity to platinum chemotherapy. The standard method to evaluate ERCC1 protein expression is through the use of immunohistochemistry with monoclonal antibody 8F1, an antibody that was recently found to bind an unrelated protein. The present study determines the specificity of a novel antibody, monoclonal antibody 4F9, and presents a method to evaluate ERCC1 expression in colorectal tumor specimens. Using relevant cell lines as controls, the specificity of antibody 4F9 was tested by immunoblotting, immunohistochemistry and immunofluorescence. Scoring guidelines to aid in the evaluation of ERCC1 tumor expression were developed and evaluated in archival formalin-fixed paraffin embedded colorectal cancer specimens. Antibody 4F9 was found to be specific by all methods applied and it was possible to evaluate the ERCC1 expression in the majority (85\%) of colorectal cancer tumor specimens.",

keywords = "MESSENGER-RNA LEVELS CELL LUNG-CANCER PLATINUM-BASED CHEMOTHERAPY NUCLEOTIDE EXCISION-REPAIR COLORECTAL-CANCER DNA-REPAIR THYMIDYLATE SYNTHASE FLUOROURACIL CHEMOTHERAPY ENDONUCLEASE ERCC1-XPF GROUP-F",

author = "Smith, \{D. H.\} and Fiehn, \{A. M. K.\} and L. Fogh and Christensen, \{I. J.\} and Hansen, \{T. P.\} and J. Stenvang and Nielsen, \{H. J.\} and Nielsen, \{K. V.\} and Hasselby, \{J. P.\} and N. Brunner and Jensen, \{S. S.\}",

note = "ISI Document Delivery No.: AC2WC Times Cited: 1 Cited Reference Count: 37 Smith, David Hersi Fiehn, Anne-Marie Kanstrup Fogh, Louise Christensen, Ib Jarle Hansen, Tine Plato Stenvang, Jan Nielsen, Hans Jorgen Nielsen, Kirsten Vang Hasselby, Jane Preuss Brunner, Nils Jensen, Sussie Steen Danish Agency for Science, Technology and Innovation through the Industrial PhD program; Danish Strategic Research Council; Danish Cancer Society; Kathrine og Vigo Skovgaards Foundation This study was supported by the Danish Agency for Science, Technology and Innovation through the Industrial PhD program. Nils Brunner and Hans Jorgen Nielsen were supported by the Danish Strategic Research Council, the Danish Cancer Society, and Kathrine og Vigo Skovgaards Foundation. We would like to thank laboratory technicians Birgitte Jepsen and Signe Lykke Nielsen, as well as research scientists Kathy Kamath, Tatiana Okouneva and Jesper Lohse for their expertise and advice. 1 NATURE PUBLISHING GROUP LONDON SCI REP-UK",

year = "2014",

doi = "10.1038/srep04313",

language = "English",

volume = "4",

journal = "Scientific Reports",

issn = "2045-2322",

publisher = "Nature Publishing Group",

}

TY - JOUR

T1 - Measuring ERCC1 protein expression in cancer specimens: Validation of a novel antibody

AU - Smith, D. H.

AU - Fiehn, A. M. K.

AU - Fogh, L.

AU - Christensen, I. J.

AU - Hansen, T. P.

AU - Stenvang, J.

AU - Nielsen, H. J.

AU - Nielsen, K. V.

AU - Hasselby, J. P.

AU - Brunner, N.

AU - Jensen, S. S.

N1 - ISI Document Delivery No.: AC2WC Times Cited: 1 Cited Reference Count: 37 Smith, David Hersi Fiehn, Anne-Marie Kanstrup Fogh, Louise Christensen, Ib Jarle Hansen, Tine Plato Stenvang, Jan Nielsen, Hans Jorgen Nielsen, Kirsten Vang Hasselby, Jane Preuss Brunner, Nils Jensen, Sussie Steen Danish Agency for Science, Technology and Innovation through the Industrial PhD program; Danish Strategic Research Council; Danish Cancer Society; Kathrine og Vigo Skovgaards Foundation This study was supported by the Danish Agency for Science, Technology and Innovation through the Industrial PhD program. Nils Brunner and Hans Jorgen Nielsen were supported by the Danish Strategic Research Council, the Danish Cancer Society, and Kathrine og Vigo Skovgaards Foundation. We would like to thank laboratory technicians Birgitte Jepsen and Signe Lykke Nielsen, as well as research scientists Kathy Kamath, Tatiana Okouneva and Jesper Lohse for their expertise and advice. 1 NATURE PUBLISHING GROUP LONDON SCI REP-UK

PY - 2014

Y1 - 2014

N2 - Platinum chemotherapy remains part of standard therapies in the management of a variety of cancers. Severe side effects and a high degree of resistance to platinum drugs have led numerous researchers to search for predictive biomarkers, which could aid in identifying patients that are the most likely to respond to therapy. The ERCC1-ERCC4 endonuclease plays a critical role in the repair of platinum-DNA damage and has widely been studied in relation to sensitivity to platinum chemotherapy. The standard method to evaluate ERCC1 protein expression is through the use of immunohistochemistry with monoclonal antibody 8F1, an antibody that was recently found to bind an unrelated protein. The present study determines the specificity of a novel antibody, monoclonal antibody 4F9, and presents a method to evaluate ERCC1 expression in colorectal tumor specimens. Using relevant cell lines as controls, the specificity of antibody 4F9 was tested by immunoblotting, immunohistochemistry and immunofluorescence. Scoring guidelines to aid in the evaluation of ERCC1 tumor expression were developed and evaluated in archival formalin-fixed paraffin embedded colorectal cancer specimens. Antibody 4F9 was found to be specific by all methods applied and it was possible to evaluate the ERCC1 expression in the majority (85%) of colorectal cancer tumor specimens.

AB - Platinum chemotherapy remains part of standard therapies in the management of a variety of cancers. Severe side effects and a high degree of resistance to platinum drugs have led numerous researchers to search for predictive biomarkers, which could aid in identifying patients that are the most likely to respond to therapy. The ERCC1-ERCC4 endonuclease plays a critical role in the repair of platinum-DNA damage and has widely been studied in relation to sensitivity to platinum chemotherapy. The standard method to evaluate ERCC1 protein expression is through the use of immunohistochemistry with monoclonal antibody 8F1, an antibody that was recently found to bind an unrelated protein. The present study determines the specificity of a novel antibody, monoclonal antibody 4F9, and presents a method to evaluate ERCC1 expression in colorectal tumor specimens. Using relevant cell lines as controls, the specificity of antibody 4F9 was tested by immunoblotting, immunohistochemistry and immunofluorescence. Scoring guidelines to aid in the evaluation of ERCC1 tumor expression were developed and evaluated in archival formalin-fixed paraffin embedded colorectal cancer specimens. Antibody 4F9 was found to be specific by all methods applied and it was possible to evaluate the ERCC1 expression in the majority (85%) of colorectal cancer tumor specimens.

KW - MESSENGER-RNA LEVELS CELL LUNG-CANCER PLATINUM-BASED CHEMOTHERAPY NUCLEOTIDE EXCISION-REPAIR COLORECTAL-CANCER DNA-REPAIR THYMIDYLATE SYNTHASE FLUOROURACIL CHEMOTHERAPY ENDONUCLEASE ERCC1-XPF GROUP-F

U2 - 10.1038/srep04313

DO - 10.1038/srep04313

M3 - Journal article

C2 - 24603753

SN - 2045-2322

VL - 4

JO - Scientific Reports

JF - Scientific Reports

M1 - 4313

ER -