The aim of this systematic review is to provide a comprehensive overview of the existing literature, comparing F-18-fluorodeoxyglucose (FDG) and C-11-methionine (MET) for the imaging of multiple myeloma (MM) with positron emission computed tomography (PET/CT). Relevant studies published from 2013 up to March 2023 were selected by searching Scopus, PubMed, and Web of Science. Selected imaging studies were analyzed using a modified version of the critical Appraisal Skills Programme (CASP). Ten studies encompassing 335 patients were selected. On a patient-based analysis, MET sensitivity ranged between 75.6% and 100%, resulting higher than that measured for FDG (0-100%). MET outperformed FDG for the detection of focal lesions, diffuse bone marrow involvement and mixed patterns. PET-derived parameters resulted higher for MET than for FDG, with a strong correlation with clinical variables (e.g., monoclonal component and beta-2-microglobulin levels, bone marrow infiltration, etc.), although FDG maintained a prognostic impact on outcome prediction. When compared to other tracers or imaging modalities, MET showed stronger correlation and inter-observer agreement than FDG. Although biased by the small cohorts and requiring confirmation through multicenter studies, preliminary findings suggest that MET-PET should be preferred to FDG for PET imaging of MM, or alternatively used as a complementary imaging modality. Some issues, such as tracer availability and the role of MET with respect to other emerging tracers (i.e., Ga-68-pentixafor, F-18-FACBC and F-18-FET), should be the topic of further investigations.

Head-to-head comparison between FDG and 11C-methionine in multiple myeloma: a systematic review / Filippi, Luca; Frantellizzi, Viviana; Bartoletti, Paola; Vincentis, Giuseppe De; Schillaci, Orazio; Evangelista, Laura. - In: DIAGNOSTICS. - ISSN 2075-4418. - 13:12(2023). [10.3390/diagnostics13122009]

Head-to-head comparison between FDG and 11C-methionine in multiple myeloma: a systematic review

Frantellizzi, Viviana
Secondo
;
Vincentis, Giuseppe De;
2023

Abstract

The aim of this systematic review is to provide a comprehensive overview of the existing literature, comparing F-18-fluorodeoxyglucose (FDG) and C-11-methionine (MET) for the imaging of multiple myeloma (MM) with positron emission computed tomography (PET/CT). Relevant studies published from 2013 up to March 2023 were selected by searching Scopus, PubMed, and Web of Science. Selected imaging studies were analyzed using a modified version of the critical Appraisal Skills Programme (CASP). Ten studies encompassing 335 patients were selected. On a patient-based analysis, MET sensitivity ranged between 75.6% and 100%, resulting higher than that measured for FDG (0-100%). MET outperformed FDG for the detection of focal lesions, diffuse bone marrow involvement and mixed patterns. PET-derived parameters resulted higher for MET than for FDG, with a strong correlation with clinical variables (e.g., monoclonal component and beta-2-microglobulin levels, bone marrow infiltration, etc.), although FDG maintained a prognostic impact on outcome prediction. When compared to other tracers or imaging modalities, MET showed stronger correlation and inter-observer agreement than FDG. Although biased by the small cohorts and requiring confirmation through multicenter studies, preliminary findings suggest that MET-PET should be preferred to FDG for PET imaging of MM, or alternatively used as a complementary imaging modality. Some issues, such as tracer availability and the role of MET with respect to other emerging tracers (i.e., Ga-68-pentixafor, F-18-FACBC and F-18-FET), should be the topic of further investigations.
2023
PET/CT; amino-acid; choline; molecular imaging; multiple myeloma
01 Pubblicazione su rivista::01g Articolo di rassegna (Review)
Head-to-head comparison between FDG and 11C-methionine in multiple myeloma: a systematic review / Filippi, Luca; Frantellizzi, Viviana; Bartoletti, Paola; Vincentis, Giuseppe De; Schillaci, Orazio; Evangelista, Laura. - In: DIAGNOSTICS. - ISSN 2075-4418. - 13:12(2023). [10.3390/diagnostics13122009]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/1685155
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