A novel PET probe to selectively image heat shock protein 90α/β isoforms in the brain

Author:

Sakai Takayuki1ORCID,Ikenuma Hiroshi2,Yamada Takashi3,Hattori Saori4,Ogata Aya5,Abe Junichiro4,Imamura Shinichi6,Ichise Masanori7,Tada Mari8,Kakita Akiyoshi8,Koyama Hiroko9,Suzuki Masaaki9,Kato Takashi10,Ito Kengo10,Kimura Yasuyuki4

Affiliation:

1. National Center for Geriatrics and Gerontology, Research Institute, Department of Clinical and Experimental Neuroimaging, Center for Development of Advanced Medicune for Dementia

2. National Center for Geriatrics and Gerontology, Research Institute, Department of Clinical and Experimental Neuroimaging, Center for Development of advanced Medicine for Demetian

3. National Center for Geriatrics and Gerontology, Research Institute, Department of Clinical and Experimental Neuroimaging, Center for Development of Advance Medicine for Dementia

4. National Center for Geriatrics and Gerontology, Research Institute, Department of Clinical and Experimental Neuroimaging, Center for Development of Advanced Medicine for Dementia

5. Gifu University of Medical Science: Gifu Iryo Kagaku Daigaku

6. National Center for Geriatrics and Gerontology, Research Institute, Department of Clinical and Experimental Neuroimaging, Center for Development of Advanced Medicine for Dementia

7. National Center for Geriatrics and Gerontology, Research Institute, Department of Clinical and Experimental Neuroimaging, Center for Development of Advanced medicinefor Dementia

8. Niigata University: Niigata Daigaku

9. Gifu University: Gifu Daigaku

10. National Center for Geriatrics and Gerontology, Research Institute, Department of Clinical and Experimental Neuroimaging, Center for Development of Advanced Medicine for Dementia

Abstract

Abstract Background Heat shock proteins (HSPs), ubiquitously found proteins called molecular chaperones in the brain, play important functional roles in the neuropathological processes of Alzheimer’s disease and Lewy body disease. Of many HSP subtypes, HSP90 has been shown to play a central role in the process. Many studies have shown that drugs that inhibit HSP90 activity have beneficial effects in the neurodegenerative diseases. Therefore, HSP90 PET imaging ligand, an in vivo biomarker of HSP90, can be used effectively to study HSP90 in neurodegenerative diseases. Among four HSP90 isoforms, two cytosolic isoforms (HSP90α and HSP90β) thought to be involved in the structural homeostasis of the proteins related to the neurodegenerative diseases. Currently, no useful PET imaging ligands selectively targeting the two cytosolic isoforms of HSP90 have been available yet. Results In this study, we developed a novel PET imaging ligand, [11C]NCGG801, selectively targeting HSP90α and HSP90β by radiolabeling BIIB021, an inhibitor with a high affinity for and selectivity to HSP90α and HSP90β. [11C]NCGG801 was synthesized with a high yield, molar activity and radiochemical purity. [11C]NCGG801 showed a high binding affinity for rat brain homogenate as well as human recombinant HSP90α and HSP90β proteins. This radioligand was well taken up into the rat brain (SUV 1.4) and showed clear specific binding in PET imaging of healthy rats and autoradiography of healthy rat and human brain sections. Conclusions Our data suggested that [11C]NCGG801 has a potential to be a new imaging biomarker of HSP90α/β in the brain. Further studies appear warranted to evaluate [11C]NCGG801 in humans.

Publisher

Research Square Platform LLC

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