The efficacy and safety of docetaxel plus thalidomide vs. docetaxel alone in patients with androgen-independent prostate cancer: a systematic review.

The aim of this systematic review was taken to investigate the efficacy and safety of docetaxel plus thalidomide vs. docetaxel alone for treating androgen-independent prostate cancer (AIPC). Data were collected from different databases independently by three researchers according to the pre-defined inclusion and exclusion criteria. Total three studies were finally included, indicating that docetaxel plus thalidomide exhibited better survival prognosis and greater prostate-specific antigen (PSA) decline than docetaxel alone. There were no significant differences of hematologic toxicities in two regimens, while the frequency of non-hematologic toxicities was higher in patients with docetaxel plus thalidomide. Briefly, the available evidence indicates potential survival advantage in docetaxel plus thalidomide over docetaxel alone.

Prostate cancer is the most common malignancy in men all over the world1, and the cornerstone of therapy for metastatic prostate cancer so far is androgen deprivation23, including hormonal therapies and orchiectomy. However, androgen-independence prostate cancer (AIPC) is still in a therapeutic dilemma since extremely limited treatment options have been successful in prolongation of survival.

Chemotherapy may lead to pain control and improve quality of life, but no benefit in overall survival (OS)45. The use of docetaxel, a semisynthetic taxane, has shown notable objective responses and PSA decline678910,and the later represents the disease improvement111213. In addition, docetaxel has also shown encouraging results in combination with novel agents, such as thalidomide67. Thalidomide is a synthetic glutamic acid derivative that was used for pregnancy-associated morning sickness14, but was withdrawn from market for its teratogenic effect of causing dysmelia (stunted limb growth) in humanbeing. Nevertheless, thalidomide was recently proved to have anti-inflammatory, immunomodulatory and antiangiogenic activity15. Thalidomide is now tentatively used in some cancers, including prostate cancer6716. Dohut et al6 and Figg et al7 found that the addition of thalidomide to docetaxel contributed to a larger benefit of survival and a greater PSA decline than docetaxel-alone in AIPC patients.

To date, no systematic review has been designed to observed the efficacy and safety of docetaxel plus thalidomide vs. docetaxel alone for handling AIPC. Consequently, we performed a systematic review to gain an updated perspective on docetaxel plus thalidomide for treating AIPC.

Results

Study selection

A total of 127 articles were identified through searching databases (Figure 1).After removing 8 duplicates and 74 non-clinical trials, the remaining 45 studies underwent full-text review, then 42 single-arm studies were excluded. Finally, three projects met the pre-defined criteria were enrolled in this systematic review6717.

Figure 1

Flow chart of study selection.

Study characteristics

The characteristics of the studies included in the systematic review were summarized in Table 1 and patients' clinical data in Table 2. All three studies were randomly designed. In the study of Dohut et al6, patients received either docetaxel 30 mg/m2 intravenously every week for 3 consecutive weeks, followed by a 1-week rest period (n = 25); or docetaxel at the same dose and schedule, plus thalidomide 200 mg orally each day (n = 50). In the study of Sissung et al17, 73 men with AIPC treated with either single-agent docetaxel, administered intravenously at a dose of 30 mg/m2 (n = 23), or with docetaxel on the same schedule plus oral thalidomide at a dose of 200 mg orally each day (n = 50). In the study of Figg et al7, patients were randomized to receive either (1) docetaxel, 30 mg/m2 every week for 3 consecutive weeks, followed by a l-week rest period (ie, 4-week cycle) (n = 17); or (2) docetaxel, 30 mg/m2 every week for 3 consecutive weeks, plus thalidomide, 200 mg orally each day at bedtime (the first dose was administered for 1 week before the first docetaxel infusion), followed by a l-week rest period (ie, 4-week cycle) (n = 36).

Table 1

Characteristics of studies included in the review

Study	Study design	Patient population	Intervention	Comparison	Outcome
Sissung TM 2008	phase II trial	Androgen-independent prostate cancer	docetaxel plus thalidomide	docetaxel	1. Response to Therapy OS2. Toxicity
Dahut WL 2004	phase II trial	Androgen-independent prostate cancer	docetaxel plus thalidomide	docetaxel	1. Response to Therapy PSA decline PFS OS2. Toxicity3. Pharmacokinetics4. Changes of Circulating Angiogenic Growth Factor
Figg WD 2001	phase II trial	Androgen-independent prostate cancer	docetaxel plus thalidomide	docetaxel	1. Response to Therapy PSA decline2. Toxicity

Table 2

Summary of therapeutic efficacy for docetaxel combined thlidomide vs. docetaxel alone in AIPC

Study	Regimen	Age(years)	Median OS (months)	Median PFS (months)	≥50%PSA decline (Number)	Hematologic toxicities		Non-hematologic toxicities
Grade1–2	Grade 3–5	Grade1–2	Grade 3–5
Sissung TM 2008	docetaxel plus thalidomide	N/A	N/A	N/A	N/A	N/A	4(5%)	N/A	1(1%)
docetaxel	N/A	N/A	N/A
Dahut WL 2004	docetaxel plus thalidomide	71(52–83)	28.9	5.9	25/47	4(8%)	7(14%)	22(88%)	9(18%)
docetaxel	67(43–82)	14.7	3.7	9/24	4(16%)	7(28%)	41(84%)	2(8%)
Figg WD 2001	docetaxel plus thalidomide	69(49–80)	N/A	N/A	19/36	N/A	5(7%)	N/A	1(1%)
docetaxel	N/A	N/A	6/17

Abbreviation: OS: Overall survival; PFS: Progression-free survival; N/A: not applicable.

Survival

The prognosis is summarized in Table 2. Generally speaking, prognosis was more favorable in patients treated with docetaxel plus thalidomide than those treated with docetaxel alone.

Dahut et al6 and Figg et al7 reported response to therapy based on PSA, an over 50% decline in PSA occurred more frequently in the patients treated with docetaxel plus thalidomide than those treated with docetaxel alone. Dahut et al6 reported progression-free survival (PFS) and 18 month-OS rate, the results showed the median PFS in the combined group (5.7 months) was higher than that in docetaxel alone group (3.7 months, P = 0.32), and 18-month survival was 68.2% in the combined group, higher than that in docetaxel alone group (42.9%, P = 0.11).

Side-effects

All patients in three studies6717 were evaluated for toxic effects. Dahut et al6 compared the frequency of the hematologic toxicities and non-hematologic toxicities in patients receiving different regimens, and the results showed that the hematologic toxicities were mild in both groups. As for the non-hematologic toxicitie, the incidence of depression, peripheral neuropathy and cardiac arrhythmia were slightly higher in the combined group than the docetaxel alone group. Sissung et al17 and Figg et al7 evaluated the toxic effects of all patients as a group, the results showed that they were more likely to experience hematologic toxicities and peripheral neuropathy than toxicities of other systems.

Discussion

In this systematic review, we analyzed the efficacy and safety of docetaxel plus thalidomide vs. docetaxel alone for handling AIPC. A total of three randomized studies, involving 201 patients, were included in the review. In general, the findings from these studies demonstrated superior survival in patients treated with docetaxel plus thalidomide, and all patients were more likely to experience hematologic toxicities and peripheral neuropathy than toxicities of other systems.

In the study of Dohut et al6, docetaxel plus thalidomide resulted in greater PSA decline, longer median PFS, and higher 18-month survival rate than docetaxel alone. Figg et al7 confirmed the better efficacy treated with docetaxel plus thalidomide in PSA decline than docetaxel alone. That might be due to the antiangiogenetic effect of thalidomide. Prostate tumors require angiogenic phenotype for progression to aggressive form1516. Thalidomide inhibits angiogenesis, induces apoptosis in culture systems, and reduces higher levels of angiogenesis factors, such as VEGF and bFGF, that are present in patients with prostate cancer17. Thus, the antiangiogenetic effect of thalidomide combined regimen could possibly open up a promising new avenue for treating AIPC.

In terms of the toxicities of both regimens, the hematologic toxicities were mild while the non-hematologic toxicities, such as the incidence of depression, peripheral neuropathy and cardiac arrhythmia were slightly higher in the combined arm than the docetaxel alone arm. The results showed the combined regimen was well tolerated in the vast majority of patients. The addition of thalidomide might cause slightly higher non-hematologic toxicities, especially neuropathies, but the mechanism is still unknown.

We conducted a systematic review of the current literature to compare the efficacy and safety of docetaxel plus thalidomide vs. docetaxel alone for handling AIPC. Noticeably, the available evidence indicates potential survival advantage in docetaxel plus thalidomide over docetaxel alone. Futher well-designed and prospective studies are advisable.

Methods

Search strategy

PubMed, Biomedical Central, Google Scholar and Cochrane databases were searched using combinations of the following terms: prostate cancer/prostate carcinoma, docetaxel/taxotere, thalidomide. PubMed - prostate cancer AND docetaxel AND thalidomide (limits English), prostate carcinoma AND docetaxel AND thalidomide (limits English), prostate cancer AND taxotere AND thalidomide (limits English); Biomedical Central -prostate cancer AND docetaxel AND thalidomide; Google Scholar -prostate cancer AND docetaxel AND thalidomide; Cochrane -prostate cancer AND docetaxel AND thalidomide. The search was performed in Feb 10, 2014. Reference lists of retrieved studies were hand searched where appropriate to identify other potentially relevant studies.

Selection

Studies were included in the systemic review meeting the following inclusion criteria: they were randomized clinical trials and involved patients with AIPC. Studies were excluded for case reports, focusing on other type of prostate cancer, or lack of efficacies and toxities analyzing.

Data extraction

Data were extracted from eligible studies by two independent reviewers (L.C. and X.X.Q.). Any disagreement was resolved through consultation with the third reviewer (R.X.W.). The following data were extracted from studies that met the eligibility criteria: author details, year of publication, study design, therapeutic regimens, number of patients, age of patients, median survival, survival rate, median PFS, PFS rate, and PSA decline, and toxicity response.

Outcome measurement

The primary outcome was median survival in months. Secondary prognosis included survival rate, median PFS, PFS rate and PSA decline. Toxicity data are also summarized.