A. Gerl et al., ADVANCES IN THE MANAGEMENT OF METASTATIC NONSEMINOMATOUS GERM-CELL TUMORS DURING THE CISPLATIN ERA - A SINGLE-INSTITUTION EXPERIENCE, British Journal of Cancer, 74(8), 1996, pp. 1280-1285
Long-term outcome was reviewed in 266 consecutive patients with metast
atic non-seminomatous germ cell rumours treated at a single institutio
n. The overall 3 year survival was 77%, and 3 year progression free su
rvival was 71%. Multivariate analysis identified the following clinica
l features as independent prognostic factors: the presence of liver. b
one or brain metastasis, serum human chorionic gonadotropin greater th
an or equal to 10000 U 1(-1) and/or alpha-fetoprotein greater than or
equal to 1000 ng ml(-1), a mediastinal mass > 5 cm and the presence of
20 or more lung metastases. Age was not of prognostic significance. P
atients without any of the above poor-risk factors had a 3-year surviv
al of 91% regardless of etoposide- or vinblastine-containing chemother
apy compared with 61% for the remaining patients. However, etoposide-c
ontaining protocols led to significantly improved survival in patients
with at least one poor risk factor. After 612 patient-years of observ
ation no case of secondary leukaemia was observed among 119 surviving
patients who had received etoposide as part of their treatment. With a
median follow-up of 93 months, five patients developed a second germ
cell tumour, two patients nongerm cell malignancies. Fourteen patients
relapsed after a disease-free interval of more than 2 years, and nine
patients died more than 5 years after commencement of treatment under
scoring the need to report long-term results. There is some evidence t
hat cumulative experience translates into improved survival and cure r
ates for patients with poor-risk metastatic disease.