A combined index to classify prognostic comorbidity in candidates for radical prostatectomy

The study sample consisted of all 2205 patients who underwent radical prostatectomy between December 1st, 1992 and December 31st, 2005 at our institution (a university hospital). Approval by the institutional review board of the University Hospital Dresden was obtained (approval reference: EK 268092009). Seventy-four patients with missing data on Gleason score, local tumor stage or lymph node status were excluded thus leaving 2131 patients for analysis. Further demographic data is given in Tables 1 and 2.

Prostate-specific antigen (PSA), Gleason score, tumor stage, Charlson score [6], American Society of Anesthesiologists (ASA) physical status class [8], New York Heart Association (NYHA) class of cardiac insufficiency [9], Canadian Cardiovascular Society (CCS) class of angina pectoris [10], number of concomitant diseases (disease count), diabetes mellitus, and body mass index were investigated as categorical variables. Age was treated as a continuous variable. Patients with neoadjuvant treatment and, therefore, uncertain preoperative PSA values were included in the highest PSA risk groups.

Data was obtained from the patient records. The specimens of patients who underwent surgery prior to 1999 were reclassified in order to ascertain data uniformity. Perioperative cardiopulmonary risk assessment (ASA, NYHA, CCS) classifications were derived from the anesthesiology premedication records. In cases with obviously incorrect classifications these were corrected under the surveillance of a senior anesthesiologist before being entered into a database.

The Charlson score was assigned based on the comorbidity data available in the database supplemented by information derived from the discharge letters largely following the original description of this comorbidity index [6]. The presence of diabetes mellitus with or without end organ damage was recorded separately as another comorbidity classification. Codes for each condition contributing to the Charlson score [6] were included in the database. A disease count was calculated by adding one point for any concomitant disease recorded in our database (angina pectoris, hypertension, history of thrombembolism, body mass index 30 kg/m² or higher, history of myocardial infarction, cardiac insufficiency, peripheral vascular disease, cerebrovascular disease, lung disease, ulcer disease, mild liver disease, diabetes mellitus, connective tissue disease, hemiplegia, moderate or severe renal disease, solid tumors, leukemia, lymphoma, moderate or severe liver disease, dementia, metastatic solid tumors). This was done regardless of the severity of each condition analogous to an approach described by Houterman and co-workers [11]. Follow-up data were collected from urologists and/or general practitioners, the patients, relatives, health insurance companies, local authorities or the local tumor register, whichever was necessary. Thereby, only one patient was lost to follow-up. Causes of death were assigned to the relevant categories by a senior urologist (MF). Prostate cancer was considered the cause of death in cases with uncontrolled disease progression. Second cancers were considered the cause of death when an uncontrolled second malignancy was present at the time of death. Deaths in the absence of uncontrolled prostate or second cancer were considered from deaths from non-cancer competing (“comorbid”) causes. Deaths from accidents or suicide were considered a separate category. The cause of death was identified reliably in all deceased patients.

Comorbidity variables were included into the analysis when they were available in our database and allowed for a stratification by the degree of severity into 3 categories (none, mild or severe). Two- and three-sided stratifications were investigated for each variable. The stratifications used are shown in Tables 1 and 2. Commonly used stratifications promising a maximal contrast for each parameter were chosen in order not to miss potentially relevant prognostic information.

Overall mortality was the primary study endpoint. Kaplan-Meier curves and Mantel-Haenszel hazard ratios were calculated. Univariate comparisons were made with the log rank test. Only parameters significantly associated with mortality in univariate analysis were used for multivariate analysis. Cox proportional hazard models were calculated to analyze combined effects of variables. Only parameters that remained significantly associated with mortality upon multivariable analysis were retained in the final models. After stratification by body mass index (<30 kg/m² versus higher), the contribution of different causes of death (prostate cancer: uncontrolled recurrent disease, competing causes: all causes of death other than uncontrolled recurrent prostate cancer, non-cancer competing causes: all non-cancer causes other than accidents or suicide, second cancers: all cancer deaths other than from uncontrolled recurrent prostate cancer) was determined by competing risk analysis [12]. The statistical analyses were performed with the Statistical Analysis Systems (SAS Institute, Cary, NC) statistical package.