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Synthesis of a benzoxazinthione derivative of tanaproget and pharmacological evaluation for PET imaging of PR expression.
Allott, Louis; Miranda, Cecilia; Hayes, Angela; Raynaud, Florence; Cawthorne, Christopher; Smith, Graham.
Affiliation
  • Allott L; Division of Radiotherapy and Imaging, The Institute of Cancer Research, 123 Old Brompton Road, London, UK.
  • Miranda C; PET Research Centre, University of Hull, Cottingham Road, Hull, Yorkshire, HU6 7RX, UK.
  • Hayes A; Cancer Therapeutics, The Institute of Cancer Research, 123 Old Brompton Road, London, UK.
  • Raynaud F; Cancer Therapeutics, The Institute of Cancer Research, 123 Old Brompton Road, London, UK.
  • Cawthorne C; PET Research Centre, University of Hull, Cottingham Road, Hull, Yorkshire, HU6 7RX, UK. Christopher.cawthorne@kuleuven.be.
  • Smith G; Nuclear Medicine and Molecular Imaging, Department of Imaging and Pathology/MoSAIC- Molecular Small Animal Imaging Centre, Katholieke Universiteit Leuven, Leuven, Belgium. Christopher.cawthorne@kuleuven.be.
EJNMMI Radiopharm Chem ; 4(1): 1, 2019 Jan 10.
Article in En | MEDLINE | ID: mdl-31659497
BACKGROUND: The histological evaluation of estrogen receptor (ER) and progesterone receptor (PR) expression in breast cancer lesions from biopsy tissue can stratify patients to receive endocrine therapy. Furthermore, PR expression can predict response to selective estrogen receptor modulators (SERMs). Current immunohistochemical approaches to PR detection are limited by sampling error associated with biopsy and lack of standardised protocols; positron emission tomography (PET) using receptor targeted radiopharmaceuticals to provide quantitative, whole-body imaging may overcome these limitations. PR expression has been successfully imaged with PET in the clinical setting, however investigation into new radioligands with improved pharmacokinetics and metabolic stability is desirable. RESULTS: We report the synthesis of a focused library of non-steroidal PR ligands evaluated for use as PET radioligands. A lead candidate ([18F]2) with low nanomolar activity was selected and radiolabelled with a radiochemical yield of 2.29 ± 2.31% (decay-corrected), radiochemical purity (RCP) > 95% and a molar activity of 2.5 ± 1.6 GBq/µmol. Cell uptake studies showed a significant and specific accumulation of [18F]2 in T47D (PR++) breast cancer cell compared to MDA-MB-231 (PR-) control; however, in vivo evaluation was confounded by rapid defluorination of the radioligand. In vitro metabolite analysis of 2 in MLM confirmed defluorination and oxidative metabolism of the thiocarbamate to oxocarbamate moiety by mass spectrometry. CONCLUSIONS: A route to access [18F]2 was developed to allow in vitro and in vivo evaluation, albeit with low radiochemical yield and modest molar activity. [18F]2 demonstrated selective uptake in PR++ T47D cells which could be blocked in a dose dependent manner with progesterone. However, [18F]2 showed poor in vivo metabolic stability with rapid defluorination within the time frame of the imaging protocol.
Key words

Full text: 1 Collection: 01-internacional Database: MEDLINE Type of study: Guideline Language: En Journal: EJNMMI Radiopharm Chem Year: 2019 Document type: Article Country of publication: United kingdom

Full text: 1 Collection: 01-internacional Database: MEDLINE Type of study: Guideline Language: En Journal: EJNMMI Radiopharm Chem Year: 2019 Document type: Article Country of publication: United kingdom