False positive FDG uptake in melanoma patients treated with talimogene laherparepvec (T-VEC).
Evalyn E A P MulderEmma H A StahlieDaniëlle VerverClara LemstraLukas B BeenAntien L MooyaartTessa BrabanderErik VegtFrederik A VerburgAstrid A M van der VeldtCornelis VerhoefAlexander C J van AkkooiDirk J GrünhagenPublished in: Journal of surgical oncology (2021)
Talimogene laherparepvec (T-VEC) is a genetically modified herpes simplex virus-1-based oncolytic immunotherapy and has been approved for the local treatment of unresectable (stage IIIB/C and IVM1a) cutaneous melanoma. During T-VEC treatment, tumor response is often evaluated using [18F]2-fluoro-2-deoxy- d-glucose(FDG) positron emission tomography/computed tomography (PET/CT). In a Dutch cohort (n = 173), almost one-third of patients developed new-onset FDG uptake in uninjected locoregional lymph nodes during T-VEC. In 36 out of 53 (68%) patients with new nodal FDG uptake, nuclear medicine physicians classified this FDG uptake as "suspected metastases" without clinical or pathological confirmation in the majority of patients. These false positive results indicate that new-onset FDG uptake in locoregional lymph nodes during T-VEC treatment does not necessarily reflect progressive disease, but may be associated with immune infiltration. In current clinical practice, physicians should be aware of the high false positive rate of FDG uptake during treatment with T-VEC in patients with melanoma. Therefore, pathological examination of lymph node lesions with new FDG uptake is recommended to differentiate between progressive disease and immune infiltration after treatment with T-VEC.
Keyphrases
- positron emission tomography
- pet ct
- computed tomography
- lymph node
- pet imaging
- end stage renal disease
- multiple sclerosis
- primary care
- chronic kidney disease
- newly diagnosed
- prognostic factors
- neoadjuvant chemotherapy
- herpes simplex virus
- squamous cell carcinoma
- skin cancer
- adipose tissue
- contrast enhanced
- dual energy
- skeletal muscle
- basal cell carcinoma