Stroke related to androgen deprivation therapy for prostate cancer: a meta-analysis and systematic review

We systematically searched Medline, Embase and Cochrane Library databases up to September 30th 2014, with all possible combinations of the keywords as follows: prostate cancer or prostate tumor or prostate carcinoma, androgen deprivation or androgen suppression or endocrine treatment or ADT or AST; and stroke or cerebrovascular or transient ischemic attack or hemiplegia or TIA or cardiovascular (Additional file 1: Methods S1). No language, date, or other restrictions was used. Publications from potentially relevant journals were complementally searched.

Studies were included if they fulfilled the following inclusion criteria: 1) Patients diagnosed with PCa only; 2) Intervention groups must include ADT (either monotherapy or combination therapy); 3) Treatments in control groups were non-ADT (e.g. radical prostatectomy, radiotherapy, active surveillance.); 4) Studies must have the data of risk estimates with 95 % CIs; 5) Studies must report comparative data. If more than one study were identified from the same population, we extracted data from all available informations, rather than just a single publication.

Two reviewers (Meng & Zhu) independently extracted the data from eligible and potentially relevant publications, with differences resolved by the third reviewer (Niu) as necessary. General characteristics of each included publication were recorded: first author’s name, year of publication, medical center, study design, sample size, population characteristics, follow-up period, interventions, definition of stroke morbidity, HRs and corresponding 95 % CIs of estimates in each comparisons. Definition of stroke was according to what descripted in each included publication. Our meta-analysis involved different types of ADT including AA, GnRH agonists, orchiectomy, and two or more types above combined.

Study qualities of the selected trials were assessed by the Jadad score [15]. Trails were considered to be of high quality if they achieved more than 4 scores. Newcastle-Ottawa quality assessment scale (NOS) [16] was used to assess the observational studies. Studies with more than 6 scores were considered high-quality. Two authors (Zhu & Meng) respectively addressed the assessments and discussed the discrepancies until agreement reached. Level of evidence (LOE) of all eligible publications were evaluated using the classifications of Phillips et al’s, [17].

In order to minimize the influence of concomitant treatments (e.g. radiotherapy and prostatectomy), subgroup analysis of ADT monotherapy vs watchful waiting or active surveillance (WW/AS) for stroke morbidity was carried out. ADT monotherapy was defined as a single therapeutic that in addition to ADT, no other previous therapy was used in intervention group. Considering the significance of existing heterogeneity in overall-analysis, additional subgroup-analyses for various types of ADT (e.g. GnRH, AA, GnRH + AA and Orchiectomy) vs non-ADT were also performed.

Using the same methods as in our previous study [18], weighted HRs and 95 % CIs were estimate to compare all of these dichotomous variables. Different methods were employed to calculate the HRs on the basis of the data provided in the studies. When studies compared more than one types of ADT with the same control group severally (for example, GnRH vs Control, Orchiectomy vs Control), random effects meta-analyses were used to combine these results together as necessary.

Statistical heterogeneity among studies was evaluated with the Cochrane’s Q statistic [19]. In addition, inconsistency was quantified by I² statistic (100 % × [(Q-df)/Q]), different I² values (25, 50, and 75 %) denote different levels (low, medium, and high levels) of heterogeneity [20]. Using the Der-Simonian and Laird method, we chose random-effects models throughout this analysis no matter whether heterogeneity existed or not.

HRs and 95 % CIs were directly given in two publications [14, 21], and four studies [13, 14, 23, 24] respectively compared different types of ADT with control groups. All of these observational studies were of high LOE (2a). Details of the eligible studies were summarized in Table 1. According to the assessment of NOS for observational studies, all eligible studies were high-quality with scores more than seven stars (Additional file 1: Table S2).

Six studies [13, 14, 21, 23‐25] involving 160,485 participants were identified for inclusion criteria. Figure 2a showed the impact of ADT vs non-ADT on the end point of fatal or non-fatal stroke morbidity. 5578 (7.4 %) stroke events occurred among 74,538 ADT users compared with 5134 events (5.7 %) within control participants. Pooled HR showed that the incidence of stroke morbidity in ADT group was 12 % higher than non-ADT users, although statistically significant difference was not observed (HR = 1.12; 95 % CI, 0.95–1.32; P = 0.16). As to subgroup-analyses of different types of ADT, four studies [13, 23‐25] were identified: three studies [13, 23, 24] respectively compared AA alone, GnRH alone and GnRH plus AA with control groups, four studies [13, 23‐25] were available for the subgroup-analyses of orchiectomy vs non-ADT. Figure 3 showed the subgroup analyses for the effect of different types of ADT vs control on stroke events. Stroke was significantly associated with GnRH alone (HR = 1.20; 95 % CI 1.12–1.28; P < 0.001), GnRH plus AA (HR = 1.23; 95 % CI 1.13-1.34; P < 0.001), and orchiectomy (HR = 1.37; 95 % CI 1.33–1.64; P = 0.001), but not with AA alone (HR = 1.06; 95 % CI 0.71–1.57; P = 0.78). Details of meta-analyses for each type of ADT were shown in Additional file 1: Figure S1. Additionally, two studies [23, 24] with 81,402 patients were included for subgroup analysis of ADT monotherapy vs WW/AS. 6150 stroke events were recorded, containing 3317 events from ADT users (8.2 %) and 2349 from WW/AS groups (5.5 %). Pooled result revealed that ADT monotherapy could significantly increase the risk of stroke, with a higher incidence of 16 % than WW/AS (HR = 1.16, 95%CI: 1.03–1.31, P = 0.01; Fig. 2b).