RANK and RANK ligand expression in primary human osteosarcoma

RANK and RANK ligand expression in primary human osteosarcoma

Receptor activator of nuclear factor kappa-B ligand (RANKL) is an essential mediator of osteoclast formation, function and survival. In patients with solid tumor metastasis to the bone, targeting the bone microenvironment by inhibition of RANKL using denosumab, a fully human monoclonal antibody (mAb...

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Main Authors: Daniel Branstetter, Kathy Rohrbach, Li-Ya Huang, Rosalia Soriano, Mark Tometsko, Michelle Blake, Allison P. Jacob, William C. Dougall
Format: Article
Language:English
Published: Elsevier 2015-09-01
Series:Journal of Bone Oncology
Subjects:
RANK
RANKL
Human osteosarcoma
Antibodies
Protein expression
Immunohistochemistry
Online Access:http://www.sciencedirect.com/science/article/pii/S2212137415300063
id doaj-18f9632d263c4179a834da9db4832412
record_format Article
spelling doaj-18f9632d263c4179a834da9db48324122020-11-24T23:04:55ZengElsevierJournal of Bone Oncology2212-13742015-09-0143596810.1016/j.jbo.2015.06.002RANK and RANK ligand expression in primary human osteosarcomaDaniel Branstetter0Kathy Rohrbach1Li-Ya Huang2Rosalia Soriano3Mark Tometsko4Michelle Blake5Allison P. Jacob6William C. Dougall7Department of Pathology, Amgen Inc., Seattle, WA, USADepartment of Pathology, Amgen Inc., Seattle, WA, USADepartment of Pathology, Amgen Inc., Seattle, WA, USADepartment of Pathology, Amgen Inc., Seattle, WA, USATherapeutic Innovation Unit, Amgen Inc., Seattle, WA, USADepartment of Hematology/Oncology Research, Amgen Inc., Seattle, WA, USATherapeutic Innovation Unit, Amgen Inc., Seattle, WA, USATherapeutic Innovation Unit, Amgen Inc., Seattle, WA, USAReceptor activator of nuclear factor kappa-B ligand (RANKL) is an essential mediator of osteoclast formation, function and survival. In patients with solid tumor metastasis to the bone, targeting the bone microenvironment by inhibition of RANKL using denosumab, a fully human monoclonal antibody (mAb) specific to RANKL, has been demonstrated to prevent tumor-induced osteolysis and subsequent skeletal complications. Recently, a prominent functional role for the RANKL pathway has emerged in the primary bone tumor giant cell tumor of bone (GCTB). Expression of both RANKL and RANK is extremely high in GCTB tumors and denosumab treatment was associated with tumor regression and reduced tumor-associated bone lysis in GCTB patients. In order to address the potential role of the RANKL pathway in another primary bone tumor, this study assessed human RANKL and RANK expression in human primary osteosarcoma (OS) using specific mAbs, validated and optimized for immunohistochemistry (IHC) or flow cytometry. Our results demonstrate RANKL expression was observed in the tumor element in 68% of human OS using IHC. However, the staining intensity was relatively low and only 37% (29/79) of samples exhibited≥10% RANKL positive tumor cells. RANK expression was not observed in OS tumor cells. In contrast, RANK expression was clearly observed in other cells within OS samples, including the myeloid osteoclast precursor compartment, osteoclasts and in giant osteoclast cells. The intensity and frequency of RANKL and RANK staining in OS samples were substantially less than that observed in GCTB samples. The observation that RANKL is expressed in OS cells themselves suggests that these tumors may mediate an osteoclastic response, and anti-RANKL therapy may potentially be protective against bone pathologies in OS. However, the absence of RANK expression in primary human OS cells suggests that any autocrine RANKL/RANK signaling in human OS tumor cells is not operative, and anti-RANKL therapy would not directly affect the tumor.http://www.sciencedirect.com/science/article/pii/S2212137415300063RANKRANKLHuman osteosarcomaAntibodiesProtein expressionImmunohistochemistry
collection DOAJ
language English
format Article
sources DOAJ
author Daniel Branstetter
Kathy Rohrbach
Li-Ya Huang
Rosalia Soriano
Mark Tometsko
Michelle Blake
Allison P. Jacob
William C. Dougall
spellingShingle Daniel Branstetter
Kathy Rohrbach
Li-Ya Huang
Rosalia Soriano
Mark Tometsko
Michelle Blake
Allison P. Jacob
William C. Dougall
RANK and RANK ligand expression in primary human osteosarcoma
Journal of Bone Oncology
RANK
RANKL
Human osteosarcoma
Antibodies
Protein expression
Immunohistochemistry
author_facet Daniel Branstetter
Kathy Rohrbach
Li-Ya Huang
Rosalia Soriano
Mark Tometsko
Michelle Blake
Allison P. Jacob
William C. Dougall
author_sort Daniel Branstetter
title RANK and RANK ligand expression in primary human osteosarcoma
title_short RANK and RANK ligand expression in primary human osteosarcoma
title_full RANK and RANK ligand expression in primary human osteosarcoma
title_fullStr RANK and RANK ligand expression in primary human osteosarcoma
title_full_unstemmed RANK and RANK ligand expression in primary human osteosarcoma
title_sort rank and rank ligand expression in primary human osteosarcoma
publisher Elsevier
series Journal of Bone Oncology
issn 2212-1374
publishDate 2015-09-01
description Receptor activator of nuclear factor kappa-B ligand (RANKL) is an essential mediator of osteoclast formation, function and survival. In patients with solid tumor metastasis to the bone, targeting the bone microenvironment by inhibition of RANKL using denosumab, a fully human monoclonal antibody (mAb) specific to RANKL, has been demonstrated to prevent tumor-induced osteolysis and subsequent skeletal complications. Recently, a prominent functional role for the RANKL pathway has emerged in the primary bone tumor giant cell tumor of bone (GCTB). Expression of both RANKL and RANK is extremely high in GCTB tumors and denosumab treatment was associated with tumor regression and reduced tumor-associated bone lysis in GCTB patients. In order to address the potential role of the RANKL pathway in another primary bone tumor, this study assessed human RANKL and RANK expression in human primary osteosarcoma (OS) using specific mAbs, validated and optimized for immunohistochemistry (IHC) or flow cytometry. Our results demonstrate RANKL expression was observed in the tumor element in 68% of human OS using IHC. However, the staining intensity was relatively low and only 37% (29/79) of samples exhibited≥10% RANKL positive tumor cells. RANK expression was not observed in OS tumor cells. In contrast, RANK expression was clearly observed in other cells within OS samples, including the myeloid osteoclast precursor compartment, osteoclasts and in giant osteoclast cells. The intensity and frequency of RANKL and RANK staining in OS samples were substantially less than that observed in GCTB samples. The observation that RANKL is expressed in OS cells themselves suggests that these tumors may mediate an osteoclastic response, and anti-RANKL therapy may potentially be protective against bone pathologies in OS. However, the absence of RANK expression in primary human OS cells suggests that any autocrine RANKL/RANK signaling in human OS tumor cells is not operative, and anti-RANKL therapy would not directly affect the tumor.
topic RANK
RANKL
Human osteosarcoma
Antibodies
Protein expression
Immunohistochemistry
url http://www.sciencedirect.com/science/article/pii/S2212137415300063
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AT marktometsko rankandrankligandexpressioninprimaryhumanosteosarcoma
AT michelleblake rankandrankligandexpressioninprimaryhumanosteosarcoma
AT allisonpjacob rankandrankligandexpressioninprimaryhumanosteosarcoma
AT williamcdougall rankandrankligandexpressioninprimaryhumanosteosarcoma
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