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Abstract

There is a strong evidence base available to guide management, with relatively uniform practice at major centres internationally. Some aspects of management are peculiar to this malignancy. These include:

• the strong reliance on serum tumour markers for management,^3,4

• the use of surveillance in patients with Stage I disease, with anticipated cure by salvage therapy in those who relapse,⁵

• the expectation of cure of metastatic disease with a brief, intensive course of chemotherapy,⁶ and

• the use of surgery to resect residual masses at metastatic sites after chemotherapy.⁷

Because of the potential for cure, the multidisciplinary nature of management and the availability of high quality evidence to guide practice, the management of testicular cancer is expected to provide an excellent assessment of the quality of cancer management in a community. However, there are no comprehensive data on the management of testicular cancer in the community in Australia.

In January 1996, after approval by the Ethics Committee of the Anti-Cancer Council of Victoria, the questionnaire was sent to the treating doctors of all patients with testicular cancer in 1988-1993 identified in the cancer registry. Questionnaires were subsequently sent to other doctors identified as participants in the patients' care. Neither the doctors' nor the patients' names were identified to third parties. At the end of the survey, the data were entered into a database and a de-identified file was used for analysis.

Classification of testicular cancer

Analysis

Quality of care

Questionnaires were sent to the treating doctor for all 667 eligible patients, and replies were received for 633 (94.9% response rate).

Patient characteristics

Location of care

Initial investigation

An abdominal CT scan or lymphangiogram was not performed in 26 patients (4.1%), and a chest CT scan or chest x-ray was not performed in 33 (5.2%). Serum tumour markers were not measured at diagnosis in 16 patients (2.5%) and were recorded as "don't know" in 44 (7.0%).  

Management

There was considerable variation in the follow-up of patients on surveillance, which was inadequate for many patients according to our criteria. For patients with seminoma, investigations during the first year of surveillance did not include an abdominal CT scan in 12 (36%), did not include a chest x-ray or chest CT scan in 17 (55%), and included fewer than four serum tumour marker measurements in 25 (76%). Similarly, for patients with non-seminoma, no abdominal CT scan was performed in the first year in 6 (6%), no chest imaging in 31 (30%), and fewer than four measurements of serum marker levels in 26 (26%).

Three of the 33 patients with seminoma managed with surveillance relapsed, and one of these patients died. Twenty-seven of 102 patients with Stage I non-seminoma managed with surveillance relapsed (one of whom died), with a median time to relapse of nine months. Overall relative survival for these 102 patients was 99%.  

Survival

The relative survival according to tumour type and stage is shown in Box 4. The relative survival at five years for patients with seminoma (all stages) was 99% (95% CI, 98%-100%). For patients with non-seminoma, relative survival at five years was Stage I, 98% (95% CI, 97%-100%); Stage II, 92% (95% CI, 84%-100%); Stage III, 69% (95% CI, 56%-82%). The overall relative survival for Stage II and III patients was 84% (95% CI, 76%-91%).  

Quality of care

Studies in Scotland,¹⁰ Norway¹¹ and New York¹² have indicated higher survival proportions for patients treated in centres treating a greater number of cases of testicular cancer compared with patients treated in a "community" setting. A recently published clinical trial performed in 49 European centres found the relative risk of death was 1.85 (95% CI, 1.16-3.03) for patients with metastatic poor-prognosis non-seminoma treated at centres entering fewer than five patients on the study compared with those treated at centres entering a greater number.¹³ We found that management in Australia has been dispersed increasingly to many individual clinicians and hospitals. In this series, testicular cancer was managed in 93 centres; 71 of these centres treated fewer than two patients per year, and 86 fewer than five per year. Yet, we did not find a significant difference in survival between these centres and ones that treated more patients.

Our results show a pleasing 95% relative survival of testicular cancer patients when compared with a matched cohort from the same population. Survival in other reported series includes a 95.7% relative survival in the United States Surveillance, Epidemiology and End Results (SEER) review for a similar time period,¹⁴ and a 99% cancer-related survival in a community survey in southern Norway.¹¹ The stage at diagnosis and survival outcomes in the SEER review are very similar to ours. The 69% relative survival at five years for Stage III non-seminoma is lower than expected. However, it is difficult to compare this figure with published results, as not all details of prognostic factors⁴ are available.

The 7.5% per year increase in incidence over the six-year period of the survey is consistent with a continuation of the threefold increase in Victoria between 1950 and 1980.¹⁵ Similar dramatic increases in incidence have been reported in other Western countries,¹ but the cause remains uncertain.¹⁶

Survival figures alone are an inadequate assessment of treatment. The aim of management is to achieve cure with the least morbidity. Patients who are initially managed poorly may be cured by salvage therapy, but at the price of greater toxicity. The resulting morbidity may be severe and potentially includes infertility, sexual dysfunction, and an increased risk of secondary malignancy.

Our survey identified a number of problems. There was a wide variation in patterns of practice, particularly in patients with early-stage disease and those undergoing surveillance. Thirty-two per cent of patients failed to complete five simple measures of quality of care. More complex measures of quality of care, such as the extent of disease at relapse after initial surveillance or the quality and type of radiation therapy and chemotherapy, were not assessed in this survey.

Surveillance after orchidectomy of Stage I seminoma, as an alternative to radiation therapy, was initially described in 1988,¹⁷ but we did not consider it to be accepted management during the period of the survey. Thus, we were surprised by the number of Stage I seminoma patients managed by surveillance. These patients were managed at multiple centres and there is no evidence that they were entered into a clinical trial.

We were particularly concerned about inappropriate schedules for follow-up when surveillance was initiated. Published results of surveillance programs have emphasised the need for strict and frequent follow-up and investigation to ensure that any relapse is detected at an early stage.¹⁸ There are no published data to indicate less rigorous programs of surveillance maintain the same proportion of cure. Many patients with Stage I disease were also lost to follow-up or refused therapy. Young men are often not well motivated to continue regular and extensive follow-up. Therefore, it is essential to ensure such patients are fully informed about the options for therapy and the potential risk of unnecessary morbidity and mortality if an appropriate program of management is not followed.

We believe the development and implementation of management guidelines for testicular cancer in our community may help to reduce the problems we identified.

References

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Authors' details

Geelong Hospital, Geelong, VIC.
Greg J Neerhut, MB BS, FRACS(Urol), Urologist.

Alfred Hospital, Melbourne, VIC.
Max A Schwarz, MB BS(Hons), FRACP, Head, Medical Oncology Unit;
Ross M Snow, MB BS, FRACS(Urol), Head, Urology Unit.

Anti-Cancer Council of Victoria, Melbourne, VIC.
Vicky J Thursfield, BSc, GradDip(Applied Stats), Information Manager, Cancer Epidemiology Centre;
Graham G Giles, PhD, Director, Victorian Cancer Registry.

Reprints will not be available from the authors.
Correspondence: Associate Professor G C Toner, Head, Medical Oncology, Peter MacCallum Cancer Institute, St Andrew's Place, East Melbourne, VIC 3002.
gtonerATpetermac.unimelb.edu.au

©MJA 2001
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