18F-FDG PET predicts survival after pretargeted radioimmunotherapy in patients with progressive metastatic medullary thyroid carcinoma

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• 作者：Pierre-Yves Salaun (1)
  Lo?c Campion (2)
  Catherine Ansquer (3)
  Eric Frampas (4) (5)
  Cédric Mathieu (3)
  Philippe Robin (1)
  Claire Bournaud (6)
  Jean-Philippe Vuillez (7)
  David Taieb (8)
  Caroline Rousseau (5) (9)
  Delphine Drui (10)
  Eric Mirallié (11)
  Fran?oise Borson-Chazot (12)
  David M. Goldenberg (13) (14)
  Jean-Fran?ois Chatal (15)
  Jacques Barbet (15) (5)
  Fran?oise Kraeber-Bodéré (16) (3) (5) (9)
  
• 关键词：Surrogate marker ; Radioimmunotherapy ; Medullary thyroid carcinoma ; CEA ; Calcitonin ; Doubling time ; FDG PET ; Survival
• 刊名：European Journal of Nuclear Medicine and Molecular Imaging
• 出版年：2014
• 出版时间：August 2014
• 年：2014
• 卷：41
• 期：8
• 页码：1501-1510
• 全文大小：468 KB
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• 作者单位：Pierre-Yves Salaun (1)
  Lo?c Campion (2)
  Catherine Ansquer (3)
  Eric Frampas (4) (5)
  Cédric Mathieu (3)
  Philippe Robin (1)
  Claire Bournaud (6)
  Jean-Philippe Vuillez (7)
  David Taieb (8)
  Caroline Rousseau (5) (9)
  Delphine Drui (10)
  Eric Mirallié (11)
  Fran?oise Borson-Chazot (12)
  David M. Goldenberg (13) (14)
  Jean-Fran?ois Chatal (15)
  Jacques Barbet (15) (5)
  Fran?oise Kraeber-Bodéré (16) (3) (5) (9)
  
  1. Nuclear Medicine Department, University Hospital, Brest, France
  2. Statistical Department, ICO-Gauducheau Cancer Institute, Nantes, France
  3. Nuclear Medicine Department, University Hospital, Nantes, France
  4. Radiology Department, University Hospital, Nantes, France
  5. Nantes-Angers Cancer Research Center, Inserm, U 892, CNRS, UMR 6299, Université de Nantes, Nantes, France
  6. Nuclear Medicine Department, University Hospital, Lyon, France
  7. Nuclear Medicine Department, University Hospital, Grenoble, France
  8. Nuclear Medicine Department, University Hospital, Marseille, France
  9. Nuclear Medicine Department, ICO-René Gauducheau, Nantes, France
  10. Endocrinology Department, University Hospital, Nantes, France
  11. Surgery Department, University Hospital, Nantes, France
  12. Endocrinology Department, University Hospital, Lyon, France
  13. IBC Pharmaceuticals, Inc., and Immunomedics, Inc., Morris Plains, NJ, USA
  14. Garden State Cancer Center, Center for Molecular Medicine and Immunology, Morris Plains, NJ, USA
  15. GIP ARRONAX, Saint-Herblain, France
  16. Nuclear Medicine Department, H?tel Dieu University Hospital, 1 place Ricordeau, 44093, Nantes, France
  
• ISSN：1619-7089

文摘

Purpose PET is a powerful tool for assessing targeted therapy. Since 18F-FDG shows a potential prognostic value in medullary thyroid carcinoma (MTC), this study evaluated 18F-FDG PET alone and combined with morphological and biomarker evaluations as a surrogate marker of overall survival (OS) in patients with progressive metastatic MTC treated with pretargeted anti-CEA radioimmunotherapy (pRAIT) in a phase II clinical trial. Methods Patients underwent PET associated with morphological imaging (CT and MRI) and biomarker evaluations, before and 3 and 6?months, and then every 6?months, after pRAIT for 36?months. A combined evaluation was performed using anatomic, metabolic and biomarker methods. The prognostic value of the PET response was compared with demographic parameters at inclusion including age, sex, RET mutation, time from initial diagnosis, calcitonin and CEA concentrations and doubling times (DT), SUVmax, location of disease and bone marrow involvement, and with response using RECIST, biomarker concentration variation, impact on DT, and combined methods. Results Enrolled in the study were 25 men and 17 women with disease progression. The median OS from pRAIT was 3.7?years (0.2 to 6.5?years) and from MTC diagnosis 10.9?years (1.7 to 31.5?years). After pRAIT, PET/CT showed 1 patient with a complete response, 4 with a partial response and 24 with disease stabilization. The combined evaluation showed 20 responses. For OS from pRAIT, univariate analysis showed the prognostic value of biomarker DT (P--.011) and SUVmax (P--.038) calculated before pRAIT and impact on DT (P--.034), RECIST (P--.009), PET (P--.009), and combined response (P--.004) measured after pRAIT. PET had the highest predictive value with the lowest Akaike information criterion (AIC 74.26) as compared to RECIST (AIC 78.06), biomarker variation (AIC 81.94) and impact on DT (AIC 79.22). No benefit was obtained by combining the methods (AIC 78.75). This result was confirmed by the analysis of OS from MTC diagnosis. Conclusion 18F-FDG PET appeared as the most potent and simplest prognostic method to predict survival in patients with progressive MTC treated with pRAIT. Biomarker DT before pRAIT also appeared as an independent prognostic factor, but no benefit was found by adding morphological and biomarker evaluation to PET assessment.