Nucl Med Mol Imaging.  2022 Aug;56(4):188-195. 10.1007/s13139-022-00754-6.

Interval Changes in PSMA PET/CT During Radium‑223 Therapy for Metastatic Bone Disease from Castration‑Resistant Prostate Cancer

Affiliations
  • 1Division of Nuclear Medicine, Jewish General Hospital, 3755 Cote St Catherine Rd, G19, Montreal, QC H3T1E2, Canada
  • 2Dept of Urology, Skåne University, Jan Waldenströms gata 5, 205 02 Malmö, SE, Sweden
  • 3Dept of Translational Medicine, Lund University, Scheelevägen 27, 223 70 Lund, SE, Sweden
  • 4Division of Hematology, Jewish General Hospital, 3755 Cote St Catherine Rd, Montreal, QC H3T1E2, Canada
  • 5Division of Medical Oncology, Jewish General Hospital, 3755 Cote St Catherine Rd, Montreal, QC H3T1E2, Canada

Abstract

Background
Radium-223, an alpha-emitting therapeutic radiopharmaceutical, prolongs overall survival (OS) in patients with symptomatic bone-predominant metastatic castration-resistant prostate cancer (mCRPC). PSMA PET/CT is a molecular imaging tool for whole-body imaging of prostate cancer and may inform on the mechanisms of radium-223 activity and treatment resistance in mCRPC patients.
Methods
In an open-label, single-arm, prospective trial, we enrolled patients with bone-predominant mCRPC to undergo baseline PSMA PET/CT, 6 cycles of radium-223, and post-therapy PSMA PET/CT. We assessed the relationship between multiple parameters of interval change on PSMA PET/CT on aPROMISE PSMA automated analysis and a human reader, and laboratory measurements.
Results
Fourteen patients were enrolled and 9 patients completed both protocol-defined PSMA PET/CT. Of the 9 evaluable patients, 1 (11%) had a complete response and 8 (89%) had PSMA PET progressive disease. All patients showed decreases in PSMA uptake in some disease sites evident on the baseline scan. The change in overall burden of disease on PSMA PET was more strongly correlated with changes in PSA (ρ = 0.95) than ALP (ρ = 0.62). Progression in bone was a common finding on post-treatment PSMA PET/CT.
Conclusion
PSMA PET was able to assess response in individual lesions during radium-223 therapy in mCRPC patients. PSMA PET responses in previously established disease sites were universal, but most patients also showed overall PSMA PET progression during 6 cycles of radium-223. Given high correlation with changes in PSA, PSMA PET may be of limited value in follow-up during or after radium-223 in bone-predominant mCRPC.

Keyword

Prostate cancer; Radium-223; PSMA PET/CT
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