Initial surveillance in men with marker negative clinical stage IIA non-seminomatous germ cell tumours
Permanent link
https://hdl.handle.net/10037/35281Date
2024-01-31Type
Journal articleTidsskriftartikkel
Peer reviewed
Author
Gerdtsson, Axel; Negaard, Helene Francisca Stigter; Almås, Bjarte; Bergdahl, Anna Grenabo; Cohn-Cedermark, Gabriella; Glimelius, Ingrid; Halvorsen, Dag; Haugnes, Hege Sagstuen; Hedlund, Annika; Hellström, Martin; Holmberg, Göran; Karlsdottir, Åsa; Kjellman, Anders; Larsen, Signe Melsen; Thor, Anna; Wahlqvist, Rolf; Ståhl, Olof; Tandstad, TorgrimAbstract
Patients and methods - Observational prospective population-based study of patients diagnosed 2008–2019 with CS IIA Mk− NSGCT in the Swedish and Norwegian Testicular Cancer Group (SWENOTECA) registry. Patients were managed with surveillance, with CT scans, and tumour markers every sixth week for a maximum of 18 weeks. Patients with radiological regression were treated as CS I, if progression with chemotherapy, and remaining CS IIA Mk− disease with RPLND. The end-point was the number and percentage of patients down-staged to CS I on surveillance and rate of RPLND histopathology presented as benign, teratoma, or viable cancer.
Results - Overall, 126 patients with CS IIA Mk− NSGCT were included but 41 received therapy upfront. After surveillance for a median (range) of 6 (6–18) weeks, 23/85 (27%) patients were in true CS I and four (5%) progressed. Of the remaining 58 patients with lasting CS IIA Mk− NSGCT, 16 received chemotherapy and 42 underwent RPLND. The RPLND histopathology revealed benign lymph nodes in 11 (26%), teratoma in two (6%), and viable cancer in 29 (70%) patients.
Conclusions - Surveillance with repeated CT scans can identify patients in true CS I, thus avoiding overtreatment. The RPLND histopathology in patients with CS IIA Mk− NSGCT had a high rate of cancer and a low rate of teratoma.