Evaluation of [(11)C]NMS-E973 as a PET tracer for in vivo visualisation of HSP90

Heat shock protein 90 is an ATP-dependent molecular chaperone important for folding, maturation and clearance of aberrantly expressed proteins and is abundantly expressed (1-2% of all proteins) in the cytosol of all normal cells. In some tumour cells, however, strong expression of HSP90 is also obse...

Descripción completa

Detalles Bibliográficos
Autores principales: Vermeulen, Koen, Naus, Evelyne, Ahamed, Muneer, Attili, Bala, Siemons, Maxime, Luyten, Kaat, Celen, Sofie, Schymkowitz, Joost, Rousseau, Frederic, Bormans, Guy
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2019
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6376183/
https://www.ncbi.nlm.nih.gov/pubmed/30809293
http://dx.doi.org/10.7150/thno.27213
_version_ 1783395511164731392
author Vermeulen, Koen
Naus, Evelyne
Ahamed, Muneer
Attili, Bala
Siemons, Maxime
Luyten, Kaat
Celen, Sofie
Schymkowitz, Joost
Rousseau, Frederic
Bormans, Guy
author_facet Vermeulen, Koen
Naus, Evelyne
Ahamed, Muneer
Attili, Bala
Siemons, Maxime
Luyten, Kaat
Celen, Sofie
Schymkowitz, Joost
Rousseau, Frederic
Bormans, Guy
author_sort Vermeulen, Koen
collection PubMed
description Heat shock protein 90 is an ATP-dependent molecular chaperone important for folding, maturation and clearance of aberrantly expressed proteins and is abundantly expressed (1-2% of all proteins) in the cytosol of all normal cells. In some tumour cells, however, strong expression of HSP90 is also observed on the cell membrane and in the extracellular matrix and the affinity of tumoural HSP90 for ATP domain inhibitors was reported to increase over 100-fold compared to that of HSP90 in normal cells. Here, we explore [(11)C]NMS-E973 as a PET tracer for in vivo visualisation of HSP90 and as a potential tool for in vivo quantification of occupancy of HSP90 inhibitors. Methods: HSP90 expression was biochemically characterized in a panel of established cell lines including the melanoma line B16.F10. B16.F10 melanoma xenograft tumour tissue was compared to non-malignant mouse tissue. NMS-E973 was tested in vitro for HSP90 inhibitory activity in several tumour cell lines. HSP90-specific binding of [(11)C]NMS-E973 was evaluated in B16.F10 melanoma cells and B16.F10 melanoma, prostate cancer LNCaP and PC3, SKOV-3 xenograft tumour slices and in vivo in a B16.F10 melanoma mouse model. Results: Strong intracellular upregulation and abundant membrane localisation of HSP90 was observed in the different tumour cell lines, in the B16.F10 tumour cell line and in B16.F10 xenograft tumours compared to non-malignant tissue. NMS-E973 showed HSP90-specific inhibition and reduced proliferation of cells. [(11)C]NMS-E973 showed strong binding to B16.F10 melanoma cells, which was inhibited by 200 µM of PU-H71, a non-structurally related HSP90 inhibitor. HSP90-specific binding was observed by in vitro autoradiography of murine B16.F10 melanoma, LNCaP and PC3 prostate cancer and SKOV-3 ovary carcinoma tissue slices. Further, B16.F10 melanoma-inoculated mice were subjected to a µPET study, where the tracer showed fast and persistent tumour uptake. Pretreatment of B16.F10 melanoma mice with PU-H71 or Ganetespib (50 mg/kg) completely blocked tumour accumulation of [(11)C]NMS-E973 and confirmed in vivo HSP90 binding specificity. HSP90-specific binding of [(11)C]NMS-E973 was observed in blood, lungs and spleen of tumour-bearing animals but not in control animals. Conclusion: [(11)C]NMS-E973 is a PET tracer for in vivo visualisation of tumour HSP90 expression and can potentially be used for quantification of HSP90 occupancy. Further translational evaluation of [(11)C]NMS-E973 is warranted.
format Online
Article
Text
id pubmed-6376183
institution National Center for Biotechnology Information
language English
publishDate 2019
publisher Ivyspring International Publisher
record_format MEDLINE/PubMed
spelling pubmed-63761832019-02-26 Evaluation of [(11)C]NMS-E973 as a PET tracer for in vivo visualisation of HSP90 Vermeulen, Koen Naus, Evelyne Ahamed, Muneer Attili, Bala Siemons, Maxime Luyten, Kaat Celen, Sofie Schymkowitz, Joost Rousseau, Frederic Bormans, Guy Theranostics Research Paper Heat shock protein 90 is an ATP-dependent molecular chaperone important for folding, maturation and clearance of aberrantly expressed proteins and is abundantly expressed (1-2% of all proteins) in the cytosol of all normal cells. In some tumour cells, however, strong expression of HSP90 is also observed on the cell membrane and in the extracellular matrix and the affinity of tumoural HSP90 for ATP domain inhibitors was reported to increase over 100-fold compared to that of HSP90 in normal cells. Here, we explore [(11)C]NMS-E973 as a PET tracer for in vivo visualisation of HSP90 and as a potential tool for in vivo quantification of occupancy of HSP90 inhibitors. Methods: HSP90 expression was biochemically characterized in a panel of established cell lines including the melanoma line B16.F10. B16.F10 melanoma xenograft tumour tissue was compared to non-malignant mouse tissue. NMS-E973 was tested in vitro for HSP90 inhibitory activity in several tumour cell lines. HSP90-specific binding of [(11)C]NMS-E973 was evaluated in B16.F10 melanoma cells and B16.F10 melanoma, prostate cancer LNCaP and PC3, SKOV-3 xenograft tumour slices and in vivo in a B16.F10 melanoma mouse model. Results: Strong intracellular upregulation and abundant membrane localisation of HSP90 was observed in the different tumour cell lines, in the B16.F10 tumour cell line and in B16.F10 xenograft tumours compared to non-malignant tissue. NMS-E973 showed HSP90-specific inhibition and reduced proliferation of cells. [(11)C]NMS-E973 showed strong binding to B16.F10 melanoma cells, which was inhibited by 200 µM of PU-H71, a non-structurally related HSP90 inhibitor. HSP90-specific binding was observed by in vitro autoradiography of murine B16.F10 melanoma, LNCaP and PC3 prostate cancer and SKOV-3 ovary carcinoma tissue slices. Further, B16.F10 melanoma-inoculated mice were subjected to a µPET study, where the tracer showed fast and persistent tumour uptake. Pretreatment of B16.F10 melanoma mice with PU-H71 or Ganetespib (50 mg/kg) completely blocked tumour accumulation of [(11)C]NMS-E973 and confirmed in vivo HSP90 binding specificity. HSP90-specific binding of [(11)C]NMS-E973 was observed in blood, lungs and spleen of tumour-bearing animals but not in control animals. Conclusion: [(11)C]NMS-E973 is a PET tracer for in vivo visualisation of tumour HSP90 expression and can potentially be used for quantification of HSP90 occupancy. Further translational evaluation of [(11)C]NMS-E973 is warranted. Ivyspring International Publisher 2019-01-01 /pmc/articles/PMC6376183/ /pubmed/30809293 http://dx.doi.org/10.7150/thno.27213 Text en © Ivyspring International Publisher This is an open access article distributed under the terms of the Creative Commons Attribution (CC BY-NC) license (https://creativecommons.org/licenses/by-nc/4.0/). See http://ivyspring.com/terms for full terms and conditions.
spellingShingle Research Paper
Vermeulen, Koen
Naus, Evelyne
Ahamed, Muneer
Attili, Bala
Siemons, Maxime
Luyten, Kaat
Celen, Sofie
Schymkowitz, Joost
Rousseau, Frederic
Bormans, Guy
Evaluation of [(11)C]NMS-E973 as a PET tracer for in vivo visualisation of HSP90
title Evaluation of [(11)C]NMS-E973 as a PET tracer for in vivo visualisation of HSP90
title_full Evaluation of [(11)C]NMS-E973 as a PET tracer for in vivo visualisation of HSP90
title_fullStr Evaluation of [(11)C]NMS-E973 as a PET tracer for in vivo visualisation of HSP90
title_full_unstemmed Evaluation of [(11)C]NMS-E973 as a PET tracer for in vivo visualisation of HSP90
title_short Evaluation of [(11)C]NMS-E973 as a PET tracer for in vivo visualisation of HSP90
title_sort evaluation of [(11)c]nms-e973 as a pet tracer for in vivo visualisation of hsp90
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6376183/
https://www.ncbi.nlm.nih.gov/pubmed/30809293
http://dx.doi.org/10.7150/thno.27213
work_keys_str_mv AT vermeulenkoen evaluationof11cnmse973asapettracerforinvivovisualisationofhsp90
AT nausevelyne evaluationof11cnmse973asapettracerforinvivovisualisationofhsp90
AT ahamedmuneer evaluationof11cnmse973asapettracerforinvivovisualisationofhsp90
AT attilibala evaluationof11cnmse973asapettracerforinvivovisualisationofhsp90
AT siemonsmaxime evaluationof11cnmse973asapettracerforinvivovisualisationofhsp90
AT luytenkaat evaluationof11cnmse973asapettracerforinvivovisualisationofhsp90
AT celensofie evaluationof11cnmse973asapettracerforinvivovisualisationofhsp90
AT schymkowitzjoost evaluationof11cnmse973asapettracerforinvivovisualisationofhsp90
AT rousseaufrederic evaluationof11cnmse973asapettracerforinvivovisualisationofhsp90
AT bormansguy evaluationof11cnmse973asapettracerforinvivovisualisationofhsp90

Ejemplares similares