The MEDLINE, EMBASE and Cochrane Library databases were systematically searched until December 2011. Comparative studies were identified using any of the following keywords: cisplatin, platinum, carboplatin, paraplatin, oxalipatin, lobaplatin, breast cancer and breast carcinoma. The search was not limited to controlled or randomized trials to minimize the chance of missing a study. A manual search of the relevant references was performed to identify further relevant trials. There were no date or language restrictions. Studies involving neo-adjuvant therapy for advanced/metastatic cancers were excluded. The studies identified through the search were independently screened by two authors (M.L. and Q-G.M.) for inclusion. Any disagreements were arbitrated by a third author (CY.W.).

The primary outcomes evaluated in the present review were the complete response (CR), PR, pCR, clinical benefit, DFS, progression-free survival (PFS) and overall survival (OS) rates. The secondary outcome was the adverse effects of treatment/toxicity (including withdrawals and discontinuations).

The present systematic review was conducted in accordance with the Quality of Reporting of Meta-analyses (QUOROM) statement (8). Two authors independently evaluated all included trials based on randomized sequence generation, allocation concealment, blinding of outcome assessors and reporting of an intention-to-treat analysis. Trials were considered to be of low quality if they reported none of the items, medium quality if they reported on <3 and of high quality if they reported on 3 or 4.

Two authors independently extracted the data concerning the author details, year, methodological quality, number of patients, patient characteristics, interventions (i.e., drugs, schedule and number of therapeutic sessions) and outcomes using a data extraction form. Discrepancies were resolved by consensus. When multiple publications of the same trial were identified, data were extracted and reported as a single trial.

The Cochrane Collaboration Review Manager 4.2.2 statistical software was used for for meta-analysis. To test for heterogeneity in the included studies and analyze the statistical heterogeneity using the χ² test, the significance level was set at P≤0.10. When heterogeneity existed between the results, I² heterogeneity quantitative analysis was used and the significance level set at 50%, so I²>50% indicated heterogeneity in the results. If the test results indicated that the heterogeneity between the groups was not signficant, then a fixed-effects model was used for meta-analysis. On the contrary, if I²> 50%, then there was heterogeneity. After been processed the heterogeneity still can not be eliminated, and is intended merger analysis using a random-effects model. A random-effects model was used for pooled analysis if there was clinical heterogeneity in a subgroup analysis and treatment heterogeneity was not eliminated. The standardized mean difference (SMD) or weighted standard deviation (MD) were the effect indicators of the present study and the 95% CI was used for the efficacy analysis statistics.

A total of 103 references were identified and 42 studies were excluded by reading the titles and abstracts to identify the repeated studies, animal experiments and synthesis. The studies were read further to identify case reports, clinical observations without contrast and studies where the molecular typing was unclear, to exculde a total of 54 studies. Ultimately, seven studies were selected with a total of 717 patients. The reference flow is shown in Fig. 1.

The seven studies were retrospective cohorts, including 108 patients (9–14). The basic characteristics are shown in Table I.

The only platinum drugs used in the studies were cisplatin and carboplatin. The study by Sirohi et al(9) analyzed neo-adjuvant chemotherapy in 94 and 155 cases of advanced/metastatic breast cancer, so the study was divided into Sirohi 1 et al and Sirohi 2 et al, neo-adjuvant and advanced/metastatic cases, respectively, to analyze the outcome, as shown in Tables II, III and IV. Two studies (10,11) were neo-adjuvant chemotherapy studies and the remaning four (12–15) were of advanced/metastatic breast cancer. Of the seven studies of TNBC, five (9–12,14) had a clear description of ER and PR detection using an immunohistochemical method, where ER and PR were defined as negative in TNBC. HER2 testing was performed differently and the negative standard was different. One study (9) described an immunohistochemical assay for HER2. HER2 immunohistochemistry or FISH gene amplification were used to define negative HER2 expression. The neo-adjuvant chemotherapy, intervention and outcome measures used in the studies are shown in Table II and another study of a platinum single-agent neo-adjuvant chemotherapy used in an observational study of clinical efficacy was added as a comparison (6). The studies were divided into groups of three; except the Sirohi 1 study (9) which used doxorubicin, the other 2 studies (10,11) used a drug combination of carboplatin and paclitaxel. The Sirohi 1 (9) study reports only the cCR as certain cases did not receive surgical treatment; the other 2 studies both have pCR data. Sirohi 1 (9) reported that in certain cases the cisplatin was replaced with carboplatin (AUC=5), due to adverse reactions causing renal toxicity, neutropenia and anemia.

Two studies (9,10) reported the cCR rate for 167 patients and the test for heterogeneity was statistically significant (P=0.05, I²=73.8%), indicating the presence of a large statistical heterogeneity, so a random-effects model was used for the pooled analyses. The meta-analysis results showed that the difference in the cCR rate was statistically significant (OR, 2.68; 95% CI, 1.69–6.57; P= 0.03; Fig. 2) between the the TNBC group and non-TNBC group with regard to neo-adjuvant therapy. The cCR rate of the TNBC group was 2.68-fold higher than that of the non-TNBC group.

Two studies (10,11) reported the pCR for 168 patients and the test for heterogeneity was not statistically significant (P=0.41, I²=0%), so the fixed-effects model was used. The meta-analysis results (Fig. 3) showed that the difference in pCR rates was statistically significant (OR, 2.89; 95% CI, 1.28–6.53; P=0.01) between the TNBC and non-TNBC groups, with regard to carboplatin-paclitaxel chemotherapy. The effect of the neo-adjuvant therapy on the TNBC group was superior to that of the non-TNBC group.

Only one study (9) reported the OS and DFS rates for neo-adjuvant platinum-based chemotherapy which included 94 cases with descriptive analysis. The 5-year OS rates in the TNBC and the non-TNBC groups were 0.65 and 0.8, respectively, while the 10-year OS rates in the TNBC and the non-TNBC groups were 0.53 and 0.65 respectively. The median DFS times were 68 and 90 months, respectively, with no significant difference observed between the two groups (P= 0.6), while the median OS times were 125 and 169 months, respectively. The distant recurrence and survival of the patients treated using neo-adjuvant chemotherapy with epirubicin, cisplatin and 5-Fu was not significantly different between the TNBC and the non-TNBC groups.

Four studies (9,13–15) reported PR in 406 patients, and three studies (9,14,15) reported cCR in 365 patients. There was no statistical heterogeneity within each sub-group, so a fixed-effects model was used to analyze the combinations. The results show that the PR and cCR of the TNBC group were 1.26- and 1.81-fold that of the non-TNBC group, respectively, but no significant differences were observed (P=0.33, P=0.53; Figs. 4 and 5). The clinical benefit rate (cCR + PR + stable disease) of the TNBC group was 1.18-fold higher than that of the non-TNBC group, but no significant differences were observed (P=0.48; Fig. 6).

Three studies (9,12,15) reported 6-month and 1-year PFS rates for a total of 234 patients, while two studies reported 2-year OS rates for 298 patients. There was no statistical heterogeneity within the subgroups, so a fixed-effects model was used to analyze the combinations (Fig. 7). The 6-month PFS rate of the TNBC group was higher compared with the non-TNBC group (OR, 1.81; 95% CI, 1.11–2.96; P=0.02; Fig. 8). The 1-year PFS rate was not significantly different between the two groups (OR, 1.42, 95% CI, 0.69–2.92; P=0.35; Fig. 9).