PARP1 expression in mantle cell lymphoma: the utility of PARP1 immunohistochemistry and its relationship with markers of DNA damage

Mantle cell lymphoma (MCL) is an aggressive disease with poor overall survival, attributable in part to frequent defects of the DNA repair genes. In such malignancies, additional inhibition of the ubiquitous DNA damage repair protein, poly‐ADP ribose polymerase‐1 (PARP1) has shown enhanced cytotoxic...

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Veröffentlicht in:	Hematological oncology 2015-12, Vol.33 (4), p.159-165
Hauptverfasser:	Mahe, Etienne, Akhter, Ariz, Le, Anne, Street, Lelsey, Pournaziri, Payam, Kosari, Farid, Shabani-Rad, Meer-Taher, Stewart, Douglas, Mansoor, Adnan
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Sprache:	eng
Schlagworte:	Adult Aged Aged, 80 and over digital image analysis DNA Damage - genetics Female Humans Immunohistochemistry Ki-67 Ki-67 Antigen Lymphoma, Mantle-Cell - genetics Lymphoma, Mantle-Cell - metabolism Lymphoma, Mantle-Cell - pathology Male mantle cell lymphoma Middle Aged PARP1 PARP1 inhibitors Poly(ADP-ribose) Polymerases - metabolism Tissue Array Analysis tissue microarray whole slide imaging
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creator	Mahe, Etienne Akhter, Ariz Le, Anne Street, Lelsey Pournaziri, Payam Kosari, Farid Shabani-Rad, Meer-Taher Stewart, Douglas Mansoor, Adnan
description	Mantle cell lymphoma (MCL) is an aggressive disease with poor overall survival, attributable in part to frequent defects of the DNA repair genes. In such malignancies, additional inhibition of the ubiquitous DNA damage repair protein, poly‐ADP ribose polymerase‐1 (PARP1) has shown enhanced cytotoxicity (so‐called synthetic lethality). We studied PARP1 expression in a series of clinical cases of MCL, with the secondary aim to ascertain the relationship between PARP1 expression and DNA repair gene expression (namely ATM and p53) by immunohistochemical methods. We also examined the relationship between PARP1 expression and the well‐established prognostic biomarker Ki‐67, in addition to correlating PARP1 expression with the overall survival. From amongst our series of 79 unselected cases of MCL, we detected PARP1 expression in all but two cases with variable intensity. We also noted correlations between PARP1 expression and ATM and p53 expression. As described in previous studies, we identified a significant survival difference on the basis of Ki‐67 and p53 expression. When digital H‐score analysis of PARP1 expression was performed, there was a distinct survival advantage noted in patients with lower levels of expression. When our biomarker data were assessed by Cox regression, furthermore, the dominant effects of p53 and PARP1 expression were highlighted. Our data support the need for further research into the potential utility of PARP1 as a biomarker in MCL and for the potential direction of future PARP1 inhibitor‐targeted therapy studies. Copyright © 2014 John Wiley & Sons, Ltd.
doi_str_mv	10.1002/hon.2160
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When digital H‐score analysis of PARP1 expression was performed, there was a distinct survival advantage noted in patients with lower levels of expression. When our biomarker data were assessed by Cox regression, furthermore, the dominant effects of p53 and PARP1 expression were highlighted. Our data support the need for further research into the potential utility of PARP1 as a biomarker in MCL and for the potential direction of future PARP1 inhibitor‐targeted therapy studies. 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In such malignancies, additional inhibition of the ubiquitous DNA damage repair protein, poly‐ADP ribose polymerase‐1 (PARP1) has shown enhanced cytotoxicity (so‐called synthetic lethality). We studied PARP1 expression in a series of clinical cases of MCL, with the secondary aim to ascertain the relationship between PARP1 expression and DNA repair gene expression (namely ATM and p53) by immunohistochemical methods. We also examined the relationship between PARP1 expression and the well‐established prognostic biomarker Ki‐67, in addition to correlating PARP1 expression with the overall survival. From amongst our series of 79 unselected cases of MCL, we detected PARP1 expression in all but two cases with variable intensity. We also noted correlations between PARP1 expression and ATM and p53 expression. As described in previous studies, we identified a significant survival difference on the basis of Ki‐67 and p53 expression. When digital H‐score analysis of PARP1 expression was performed, there was a distinct survival advantage noted in patients with lower levels of expression. When our biomarker data were assessed by Cox regression, furthermore, the dominant effects of p53 and PARP1 expression were highlighted. Our data support the need for further research into the potential utility of PARP1 as a biomarker in MCL and for the potential direction of future PARP1 inhibitor‐targeted therapy studies. Copyright © 2014 John Wiley & Sons, Ltd.</abstract><cop>England</cop><pub>Blackwell Publishing Ltd</pub><pmid>25143154</pmid><doi>10.1002/hon.2160</doi><tpages>7</tpages></addata></record>
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subjects	Adult Aged Aged, 80 and over digital image analysis DNA Damage - genetics Female Humans Immunohistochemistry Ki-67 Ki-67 Antigen Lymphoma, Mantle-Cell - genetics Lymphoma, Mantle-Cell - metabolism Lymphoma, Mantle-Cell - pathology Male mantle cell lymphoma Middle Aged PARP1 PARP1 inhibitors Poly(ADP-ribose) Polymerases - metabolism Tissue Array Analysis tissue microarray whole slide imaging
title	PARP1 expression in mantle cell lymphoma: the utility of PARP1 immunohistochemistry and its relationship with markers of DNA damage
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