Abstract
We assessed the external validity of a prediction rule for nonseminomatous testicular cancer patients. The rule was developed to predict the probability of retroperitoneal metastases being benign (only necrosis/fibrosis) after chemotherapy treatment. Patients with a high probability of benign residual masses might be offered surveillance as opposed to patients with a low probability, who should undergo retroperitoneal lymph node dissection (RPLND). We compared the observed histology with the predicted probability in 105 patients with good prognosis germ cell cancer who underwent RPLND between 1995 and 1998. We found that predicted probabilities higher than 5% were in good agreement with the observed frequencies of benign masses. The area under the receiver operating characteristic curve was 0.76, suggesting that the rule could reasonably discriminate between benign masses and tumour. However, nearly all predicted probabilities (n=101) were lower than 70%, which might be considered as the lowest value at which surveillance offers a reasonable alternative to RPLND. Further, 35% of patients currently under surveillance (84 out of 241) had predicted probabilities lower than 70%. In conclusion, the clinical relevance of the prediction rule was limited for the patients who underwent RPLND; use of the rule would change the policy from RPLND to surveillance in only a few. On the other hand, the rule might support selection of patients for RPLND, who currently are under surveillance.
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Main
Computer tomography (CT) often shows small remnants of retroperitoneal masses after chemotherapy for metastatic nonseminomatous testicular cancer (Peckham, 1988). The histology of the residual masses may be benign (entirely necrotic/fibrotic), or may contain tumour elements (mature teratoma or viable cancer cells). Resection of a totally benign mass has no therapeutic value and should preferably not be performed. Most resection policies consider only one prognostic factor to predict the histology of residual masses, that is, mass size after chemotherapy (Jansen et al, 1991; Mead et al, 1992). Masses smaller than or equal to 10 mm are generally not resected, although more aggressive approaches have been proposed (Gelderman et al, 1986; Fosså et al, 1992).
Mass size as a single prognostic factor has limited predictive power to discriminate benign histology from tumour. Some small masses containing tumour are left unresected and larger benign masses are unnecessarily removed. A distinction based on several prognostic factors has the potential to classify masses more accurately as benign or tumour (Donohue et al, 1987; Fosså et al, 1992). Therefore, a clinical prediction rule has been developed that incorporates six well-known prognostic factors, that is, the Residual Histology in Testicular Cancer (ReHiT) prediction rule (Steyerberg et al, 1995). It estimates the probability that a residual mass is completely benign. The predicted probability may support the treating physician in deciding whether a residual mass should be resected or not.
Before any wide use of a prediction rule can be encouraged, its ability to produce accurate predictions for patients from different but plausibly related populations (‘transportability’) needs to be assessed (Justice et al, 1999). The ReHiT prediction rule was developed for good, intermediate, and poor prognosis patients according to the International Germ Cell Consensus Classification (IGCCG, 1997) on the basis of data from patients from six European and US study groups (development population), who were predominantly treated in the 1980s with cisplatin-based chemotherapy. Patients with a good prognosis (56% of all nonseminomas) have an expected 5-year progression-free survival probability of 89% (IGCCG, 1997). In this group, particularly, it is important to minimise the therapeutic burden; any unnecessary treatment such as resection should be avoided. We therefore studied the transportability of the prediction rule to good prognosis patients treated in the 1990s. We were particularly interested in the clinical relevance of the prediction rule, that is, its ability to support decision-making for patients after chemotherapy.
Patients and methods
Patients participated in an EORTC/MRC trial of the genitourinary group (EORTC-30941/MRC-TE20), which compared three cycles of bleomycin, etoposide, cisplatin (3BEP) with four cycles (3BEP–1EP) and the administration of BEP over 5 days with 3 days (de Wit et al, 2001). A total of 812 good prognosis patients were enrolled between March 1995 and April 1998 (Figure 1). The present analysis included only nonseminomas (n=682), which are defined as good prognosis disease when the site of the primary tumour is not mediastinal, no nonpulmonary visceral metastases are present, and the marker levels are good, that is, α-fetoprotein (AFP) and human chorionic gonadotropin (HCG) below 1000 ng ml−1 and lactate dehydrogenase (LDH) below 1.5 × upper limit of the normal value (IGCCG, 1997). Patients with an extragonadal primary site (n=21), patients having no retroperitoneal metastasis (n=182), and patients with elevated markers after chemotherapy (n=68) were excluded from the analysis. Out of the remaining 411 patients, 306 patients with a prechemotherapy retroperitoneal metastasis did not undergo retroperitoneal lymph node dissection (RPLND), either because the CT was considered to be normal following chemotherapy (n=241) or for other reasons (n=65, e.g. uncompleted chemotherapy). This meant that 105 patients were analysed for the relation between the predicted probabilities and the observed histologies (validation population); 241 patients were analysed for the predicted probabilities only. Histological findings at RPLND were classified as benign or tumour. Lesions classified as benign contained only necrotic or fibrotic elements, while tumour contained mature teratoma or viable cancer cells.
Selection of 105 patients from the EORTC-30941/MRC-TE20 study for whom the prediction rule could be validated.
The prediction rule was developed in 544 patients and was described in detail before (Steyerberg et al, 1995). The following patient characteristics are needed to calculate the probability of benign histology: the absence/presence of teratoma elements in the primary tumour, determined as teratoma differentiated (TD) or malignant teratoma intermediate (MTI); prechemotherapy levels of the serum markers AFP, HCG and LDH; maximal transversal mass size measured on CT before and after chemotherapy.
The exact formula is:
The variables teratoma-negative, AFPnormal, and HCGnormal are 1 if true and 0 if false. Ln[LDHst] is the natural logarithm of LDH/upper limit of the normal value range, sqrt[postsize] is the square root of postchemotherapy transverse diameter expressed in millimetres, and reduction is the reduction (per 10%) in mass size during chemotherapy: ((presize−postsize)/presize)*10. The probability of benign histology is calculated with the formula: probability=1/(1+e−sumscore).
This complex formula has been transformed into a score chart (Steyerberg et al, 1995) for easy estimation of the predicted probability. The value of each variable corresponds to a number of points and the total number of points corresponds directly to the predicted probability. The formula is also implemented in a spreadsheet, which is available in the public domain (ReHiT spreadsheet, http://www.eur.nl/fgg/mgz/software.html).
Missing predictor values (2% of all required values) were imputed based on the correlation with the other predictor variables (He and Shen, 1997). The statistical performance of the prediction rule was studied with respect to calibration and discrimination. Calibration refers to the agreement between the predicted probabilities and the observed frequencies. Calibration was studied graphically (Harrell, 1997) and tested with the Hosmer–Lemeshow test for external validation (Hosmer and Lemeshow, 1989). Discriminative ability, that is, whether the relative ranking of individual predictions is in the correct order, was determined with the area under the receiver operating characteristic (ROC) curve (ROC area) (Harrell et al, 1982). The ROC area represents the likelihood that a patient with a benign mass has a higher predicted probability of benign histology than a patient with tumour for a random pair of patients with different histological masses.
To classify masses as benign or tumour using the prediction rule, we applied a threshold value of 70% (Steyerberg et al, 1999a). Masses with predicted probabilities higher than 70% were considered benign; masses with probabilities lower than 70% were considered to contain tumour. Using the threshold value, we could study the clinical relevance of the prediction rule for the current population. Clinical relevance was expressed as the proportion of patients, who would receive an alternative treatment, if the prediction rule was applied (i.e. surveillance instead of RPLND).
Calculations were performed with SAS version 6.12 and S-plus version 4.5 software, using the Hmisc and Design library (Harrell, 1997).
Results
Table 1 shows the distributions of patient characteristics in the development population and in the validation population. Merely 26% (27 out of 105) of the patients in the validation population, which only contained patients with good prognosis disease, had totally benign residual masses. The distributions of the prechemotherapy levels of AFP and HCG and of the histology of the primary tumour were similar across the populations. The validation population contained a far greater number of patients in whom LDH level was normal (72% vs 28%), which follows from the definition of good prognosis; LDH level should be less than 1.5 times the upper normal value. The postchemotherapy mass size was larger than 10 mm in 92% of all patients. A very large reduction in mass size during chemotherapy (⩾70%) was seen in only 6% of the validation population.
Figure 2 shows the calibration of the prediction rule. The ideal curve represents equality of predicted probabilities and observed frequencies. More than 80% of all patients had predicted probabilities for benign histology smaller than 50%, which is in agreement with the low proportion of patients who actually had benign masses (26%). The Hosmer–Lemeshow test for external validation indicated a poor fit (P=0.001). This was caused by three out of 22 patients with a benign histology, while predicted probabilities for benign histology were below 5%. The fit was satisfactory, when these three patients were excluded. The ROC area was 0.76 (95% confidence interval: 0.65–0.88), which indicates reasonable discrimination.
Calibration curve of the prediction rule in patients of the EORTC-30941/MRC-TE20 study. Vertical lines at the bottom indicate the distribution of the predicted probabilities; lines upwards represent patients with a benign mass, lines downwards patients with tumour. Triangles indicate the frequency of benign masses grouped per quintile of predicted probabilities. The solid line shows the relation between predicted probabilities and observed frequencies. Ideally, this line equals the dotted line.
At the threshold value of 70%, only four masses (4%) were classified as benign and would have received surveillance, had the rule been applied. Thus, the clinical relevance of the rule was limited. Three of the four masses were indeed completely benign. Of the 101 masses, 77 (76%) considered as tumour actually contained tumour. Some 84 of the 241 masses, which were not resected (35%) had predicted probabilities of benign histology under 70% and would be considered as tumour.
Discussion
This study shows a reasonable statistical performance of the ReHiT prediction rule for residual mass histology of nonseminomatous testicular cancer in 105 recently treated patients with good prognosis disease. However, the clinical relevance of the rule was disappointing for these patients.
The prevalence of benign masses was low, that is, 26% in contrast to 45% in the development population. This may seem surprising, since we only considered patients with good prognosis disease. However, the studied patients were a selection of all good prognosis patients. Predominantly, patients with residual masses larger than 10 mm were candidates for resection and included in the validation population (92% vs 70% of the development population). It is well-known that small masses are more often benign. If more good prognosis patients with very small masses had undergone resection, the proportion of benign residual masses would have been higher.
In total, 30% of all patients (32 out of 105) had larger masses after chemotherapy than before, compared with 8% of the patients in the development population. Ignoring the 13 masses that were enlarged by less than 25% (which may simply reflect measurement error) reduces the proportion of enlarged masses to 18% (19 out of 105).
Low predicted probabilities showed disagreement with the observed frequencies, while higher predicted probabilities were well calibrated (Figure 2). Since a physician will choose surveillance over resection only if the predicted probability for benign histology is relatively high, the rule can still be valuable in that decision-making process. A larger sample size would, however, be required to provide solid evidence of adequate calibration.
Discriminative ability depends, apart from the studied model, also on the patients to whom the model is applied. If the predictor values of the patients show little variability (homogeneous population), it is difficult to distinguish between patients with different outcomes. Therefore, an ROC area of 0.76 is considered reasonable for our more homogeneous validation population containing only patients with good prognosis disease. A model with the same six predictor variables developed with the validation data resulted in a slightly larger ROC area (0.78). This confirms the finding that the original model was statistically valid for the good prognosis patients, even though the small sample size and the large confidence interval of the ROC area leave some room for doubt.
If a threshold value of 70% was used for the present patients, only four patients (4%) would be classified as benign. Thus, surveillance would be chosen over resection for 4% of the resected patients. Therefore, application of the model would have little clinical relevance for the present candidates of resection.
We also studied the clinical relevance of simpler models. If all patients with masses ⩽10 mm were to be offered surveillance, eight patients would have been denied resection of whom five had tumour. Considering mass size (⩽10 mm) together with the primary tumour histology (mature teratoma elements absent) would have resulted in only two patients being offered surveillance of whom one still had tumour. This suggests that simpler models are not to constitute good alternatives in good prognosis patients. Better discriminating selection models are required, to reduce the morbidity of treatment in these patients.
One-third of the patients who did not undergo resection because of small residual masses had predicted probabilities of benign histology under 70%, which indicates a substantial risk for residual tumour. A number of these patients should have been candidates for resection, particularly since the risks of short-term morbidities associated with resection are probably low given the size of the residual masses (Gels et al, 1997). The patients mainly had mature teratoma-positive primaries, elevated prechemotherapy levels of AFP or HCG or a low LDH level. Thus, the prediction rule could be particularly relevant in identifying small masses containing tumour. Future studies are required among patients currently offered surveillance to evaluate the role of the prediction rule.
To classify masses as benign or tumour using the prediction rule, we applied a threshold value of 70%. The assessment of a sensible threshold value is often difficult. We previously found that the policy to resect all masses larger than 10 mm had an implicit threshold value of 62% (Steyerberg et al, 1999b). A more stringent policy such as resection in all patients, except in those with masses smaller or equal to 20 mm, having a teratoma-negative primary tumour, and normal prechemotherapy levels of AFP and HCG (Fosså et al, 1992) implied a threshold value of 85%. A threshold value of 70 or 80% therefore seems reasonable.
Like any scientific hypothesis, the transportability of a prediction rule is established by being tested and being found valid across increasingly diverse settings (Justice et al, 1999). The more numerous and diverse the settings in which the rule is tested and found valid, the more likely it is that it will be transportable to an untested setting. Previously, we demonstrated the statistical performance of the prediction rule in a population of the late 1980s (Table 2), which was rather similar to the development population (Steyerberg et al, 1998). The rule systematically predicted too high probabilities, for patients treated between 1985 and 1999 at Indiana University Medical Center (Vergouwe et al, 2001). For these patients, a simple adjustment of the prediction rule would result in better calibrated probabilities.
The rule was mainly clinically relevant for the patients from the development and first validation populations. Around 30% of the masses in these patients might have been considered benign and consequently would have been treated by surveillance. The clinical relevance was poor for the good prognosis patients from the present study (4% would have been treated by surveillance).
In conclusion, the prediction rule for residual mass histology is statistically valid in diverse settings. Given the small number of patients in the current study, the validity in good prognosis patients is still not fully certain. Although the clinical relevance was low for the resected patients, the rule may be valuable to identify candidates for resection among these with masses smaller than 10 mm containing tumour.
Change history
16 November 2011
This paper was modified 12 months after initial publication to switch to Creative Commons licence terms, as noted at publication
References
de Wit R, Roberts JT, Wilkinson P, de Mulder PHM, Mead GM, Fosså SD, Cook P, de Prijck L, Stenning S, Collette L (2001) Final analysis demonstrating the equivalence of 3 BEP vs. 4 cycles and the 5 day schedule vs. 3 days per cycle in good prognosis germ cell cancer. An EORTC/MRC phase III study. J Clin Oncol 19: 1629–1640
Donohue JP, Rowland RG, Kopecky K, Steidle CP, Geier G, Ney KG, Einhorn L, Williams S, Loehrer P (1987) Correlation of computerized tomographic changes and histological findings in 80 patients having radical retroperitoneal lymph node dissection after chemotherapy for testis cancer. J Urol 137: 1176–1179
Fosså SD, Qvist H, Stenwig AE, Lien HH, Ous S, Giercksky KE (1992) Is postchemotherapy retroperitoneal surgery necessary in patients with nonseminomatous testicular cancer and minimal residual tumor masses?. J Clin Oncol 10: 569–573
Gelderman WA, Koops HS, Sleijfer DT, Oosterhuis JW, Oldhoff J (1986) Treatment of retroperitoneal residual tumor after PVB chemotherapy of nonseminomatous testicular tumors. Cancer 58: 1418–1421
Gels ME, Nijboer AP, Hoekstra HJ, Sleijfer DT, Molenaar WM, Plukker JT, Droste JH, Schraffordt Koops H (1997) Complications of the post-chemotherapy resection of retroperitoneal residual tumour mass in patients with non-seminomatous testicular germ cell tumours. Br J Urol 79: 263–268
Harrell Jr FE (1997) Design: S-plus functions for biostatistical/epidemiological modelling, testing, estimation, validation, graphics, prediction, and typesetting by storing enhanced model design attributes in the fit. Programs available at internet; http://lib.stat.cmu.edu/DOS/S/Harrell/
Harrell Jr FE, Califf RM, Pryor DB, Lee KL, Rosati RA (1982) Evaluating the yield of medical tests. JAMA 247: 2543–2546
He X, Shen L (1997) Linear regression after spline transformation. Biometrika 84: 474–481
Hosmer DW, Lemeshow S (1989) Applied Logistic Regression. New York: John Wiley & Sons, Inc.
IGCCG (1997) International germ cell consensus classification: a prognostic factor-based staging system for metastatic germ cell cancers. J Clin Oncol 15: 594–603
Jansen RL, Sylvester R, Sleyfer DT, ten Bokkel Huinink WW, Kaye SB, Jones WG, Keizer HJ, van Oosterom AT, Meyer S, Vendrik CP (1991) Long-term follow-up of non-seminomatous testicular cancer patients with mature teratoma or carcinoma at postchemotherapy surgery. EORTC Genitourinary tract Cancer Cooperative Group (EORTC GU Group). Eur J Cancer 27: 695–698
Justice AC, Covinsky KE, Berlin JA (1999) Assessing the generalizability of prognostic information. Ann Intern Med 130: 515–524
Mead GM, Stenning SP, Parkinson MC, Horwich A, Fosså SD, Wilkinson PM, Kaye SB, Newlands ES, Cook PA (1992) The second medical research council study of prognostic factors in nonseminomatous germ cell tumors. J Clin Oncol 10: 85–94
Peckham M (1988) Testicular cancer. Rev Oncol 1: 439–453
Steyerberg EW, Gerl A, Fosså SD, Sleijfer DT, de Wit R, Kirkels WJ, Schmeller N, Clemm C, Habbema JDF, Keizer HJ (1998) Validity of predictions of residual retroperitoneal mass histology in nonseminomatous testicular cancer. J Clin Oncol 16: 269–274
Steyerberg EW, Keizer HJ, Fosså SD, Sleijfer DT, Toner GC, Schraffordt Koops H, Mulders PFA, Messemer JE, Ney K, Donohue JP, Bajorin DF, Stoter G, Bosl GJ, Habbema JDF (1995) Prediction of residual retroperitoneal mass histology following chemotherapy for metastatic nonseminomatous germ cell tumor: multivariate analysis of individual patient data from six study groups. J Clin Oncol 13: 1177–1187
Steyerberg EW, Marshall PB, Keizer JH, Habbema JDF (1999a) Resection of small, residual retroperitoneal masses after chemotherapy for nonseminomatous testicular cancer: a decision analysis. Cancer 85: 1331–1341
Steyerberg EW, Keizer HJ, Habbema JDF (1999b) Prediction models for the histology of residual masses after chemotherapy for metastatic testicular cancer. Int J Cancer 83: 856–859
Vergouwe Y, Steyerberg EW, Foster RS, Habbema JDF, Donohue JP (2001) Validation of a prediction model and its predictors for the histology of residual masses in nonseminomatous testicular cancer. J Urol 165: 84–88
Acknowledgements
Yvonne Vergouwe was supported by the Netherlands Organisation for Scientific Research. Ewout W Steyerberg was supported by a fellowship from the Royal Netherlands Academy of Arts and Sciences.
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For the European Organisation for Research and Treatment of Cancer Genito-Urinary Group and the Medical Research Council Testicular Tumour Working Party
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Vergouwe, Y., Steyerberg, E., de Wit, R. et al. External validity of a prediction rule for residual mass histology in testicular cancer: an evaluation for good prognosis patients. Br J Cancer 88, 843–847 (2003). https://doi.org/10.1038/sj.bjc.6600759
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DOI: https://doi.org/10.1038/sj.bjc.6600759
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