Radiotherapy versus single-dose carboplatin in adjuvant treatment of stage I seminoma: a randomised trial
Radiotherapy versus single-dose carboplatin in adjuvant treatment of stage I seminoma: a randomised trial
Background:
Adjuvant radiotherapy is effective treatment for stage I seminoma, but is associated with a risk of late non-germ-cell cancer and cardiovascular events. After good results in initial studies with one injection of carboplatin, we undertook a large randomised trial to compare the approaches of radiotherapy with chemotherapy in seminoma treatment.
Methods:
Between 1996 and 2001, 1477 patients from 70 hospitals in 14 countries were randomly assigned to receive radiotherapy (para-aortic strip or dog-leg field; n=904) or one injection of carboplatin (n=573; dose based on the formula 7×[glomerular filtration rate+25] mg), at two trial centres in the UK and Belgium. The primary outcome measure was the relapse-free rate, with the trial powered to exclude absolute differences in 2-year rates of more than 3%. Analysis was by intention to treat and per protocol. This trial has been assigned the International Standard Randomised Controlled Trial Number ISRCTN27163214.
Findings:
885 and 560 patients received radiotherapy and carboplatin, respectively. With a median follow-up of 4 years (IQR 3·0–4·9), relapse-free survival rates for radiotherapy and carboplatin were similar (96·7% [95% CI 95·3–97·7] vs 97·7% [96·0–98·6] at 2 years; 95·9% [94·4–97·1] vs 94·8% [92·5–96·4] at 3 years, respectively; hazard ratio 1·28 [90% CI 0·85–1·93], p=0·32). At 2 years' follow-up, the absolute differences in relapse-free rates (radiotherapy–chemotherapy) were ?1·0% (90% CI ?2·5 to 0·5) by direct comparison of proportions, and 0·9% (?0·5 to 3·0) by a hazard-ratio-based approach. Patients given carboplatin were less lethargic and less likely to take time off work than those given radiotherapy. New, second primary testicular germ-cell tumours were reported in ten patients allocated irradiation (all after para-aortic strip field) and two allocated carboplatin (5-year event rate 1·96% [95% CI 1·0–3·8] vs 0·54% [0·1–2·1], p=0·04). One seminoma-related death occurred after radiotherapy and none after carboplatin.
Interpretation:
This trial has shown the non-inferiority of carboplatin to radiotherapy in the treatment of stage I seminoma. Although the absence of disease-related deaths and preliminary data indicating fewer second primary testicular germ-cell tumours favour carboplatin use, these findings need to be confirmed beyond 4 years' follow-up.
293-300
Oliver, R.T.D.
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Mason, M.D.
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Mead, G.M.
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von der Maase, H.
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Rustin, G.J.S.
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Joffe, J.K.
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de Wit, R.
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Aass, N.
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Graham, J.D.
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Coleman, R.
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Kirk, S.J.
accd28c4-d788-4bb1-89eb-97a497964fee
Stenning, S.P.
322b2b99-e6c5-46e5-a581-acb46357a418
2005
Oliver, R.T.D.
72fd34ac-3d25-469b-8515-05d0bc0c7e25
Mason, M.D.
da85b733-369d-41e1-81a9-061f5b1df4ab
Mead, G.M.
8a97f978-9c66-4a16-bb03-dd83d20b06a0
von der Maase, H.
ca9a43f2-0ff5-425c-8cf6-f219ce5f0706
Rustin, G.J.S.
6e151fa6-93a4-4516-b0dd-4da94ee954ba
Joffe, J.K.
15819685-3779-4513-a264-25ef953ffa7e
de Wit, R.
cf9bc96b-a6f4-4578-bfeb-b2c28596a436
Aass, N.
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Graham, J.D.
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Coleman, R.
c63e5ff2-8275-46af-ba2d-644e49fec534
Kirk, S.J.
accd28c4-d788-4bb1-89eb-97a497964fee
Stenning, S.P.
322b2b99-e6c5-46e5-a581-acb46357a418
Oliver, R.T.D., Mason, M.D., Mead, G.M., von der Maase, H., Rustin, G.J.S., Joffe, J.K., de Wit, R., Aass, N., Graham, J.D., Coleman, R., Kirk, S.J. and Stenning, S.P.
(2005)
Radiotherapy versus single-dose carboplatin in adjuvant treatment of stage I seminoma: a randomised trial.
The Lancet, 366 (9482), .
(doi:10.1016/S0140-6736(05)66984-X).
Abstract
Background:
Adjuvant radiotherapy is effective treatment for stage I seminoma, but is associated with a risk of late non-germ-cell cancer and cardiovascular events. After good results in initial studies with one injection of carboplatin, we undertook a large randomised trial to compare the approaches of radiotherapy with chemotherapy in seminoma treatment.
Methods:
Between 1996 and 2001, 1477 patients from 70 hospitals in 14 countries were randomly assigned to receive radiotherapy (para-aortic strip or dog-leg field; n=904) or one injection of carboplatin (n=573; dose based on the formula 7×[glomerular filtration rate+25] mg), at two trial centres in the UK and Belgium. The primary outcome measure was the relapse-free rate, with the trial powered to exclude absolute differences in 2-year rates of more than 3%. Analysis was by intention to treat and per protocol. This trial has been assigned the International Standard Randomised Controlled Trial Number ISRCTN27163214.
Findings:
885 and 560 patients received radiotherapy and carboplatin, respectively. With a median follow-up of 4 years (IQR 3·0–4·9), relapse-free survival rates for radiotherapy and carboplatin were similar (96·7% [95% CI 95·3–97·7] vs 97·7% [96·0–98·6] at 2 years; 95·9% [94·4–97·1] vs 94·8% [92·5–96·4] at 3 years, respectively; hazard ratio 1·28 [90% CI 0·85–1·93], p=0·32). At 2 years' follow-up, the absolute differences in relapse-free rates (radiotherapy–chemotherapy) were ?1·0% (90% CI ?2·5 to 0·5) by direct comparison of proportions, and 0·9% (?0·5 to 3·0) by a hazard-ratio-based approach. Patients given carboplatin were less lethargic and less likely to take time off work than those given radiotherapy. New, second primary testicular germ-cell tumours were reported in ten patients allocated irradiation (all after para-aortic strip field) and two allocated carboplatin (5-year event rate 1·96% [95% CI 1·0–3·8] vs 0·54% [0·1–2·1], p=0·04). One seminoma-related death occurred after radiotherapy and none after carboplatin.
Interpretation:
This trial has shown the non-inferiority of carboplatin to radiotherapy in the treatment of stage I seminoma. Although the absence of disease-related deaths and preliminary data indicating fewer second primary testicular germ-cell tumours favour carboplatin use, these findings need to be confirmed beyond 4 years' follow-up.
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More information
Published date: 2005
Additional Information:
fast track article
Organisations:
Cancer Sciences
Identifiers
Local EPrints ID: 40711
URI: http://eprints.soton.ac.uk/id/eprint/40711
ISSN: 0140-6736
PURE UUID: bb9c44f3-d6dc-4b82-91ef-f45c8b1bd68a
Catalogue record
Date deposited: 07 Jul 2006
Last modified: 15 Aug 2024 17:11
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Contributors
Author:
R.T.D. Oliver
Author:
M.D. Mason
Author:
G.M. Mead
Author:
H. von der Maase
Author:
G.J.S. Rustin
Author:
J.K. Joffe
Author:
R. de Wit
Author:
N. Aass
Author:
J.D. Graham
Author:
R. Coleman
Author:
S.J. Kirk
Author:
S.P. Stenning
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