Antiangiogenic therapy in breast cancer

Summary Based on a strong rationale for anti-VEGF (vascular endothelial growth factor) treatment in breast cancer and promising preclinical data, great hopes have been placed on the anti-VEGF antibody bevacizumab. Clinical trials, however, reported conflicting results. In metastatic human epidermal growth factor receptor 2(HER2)-negative breast cancer, the addition of bevacizumab to standard chemotherapy improved consistently progression-free survival (PFS), however, without effect on overall survival (OS). In early breast cancer bevacizumab increased the pathologic complete response rate (pCR) after neoadjuvant therapy, but adjuvant trials did not demonstrate an effect on long-term survival. Unfortunately, despite extensive research, there is still no biomarker for bevacizumab efficacy available, making patient selection difficult. This review summarizes all phase III trials investigating efficacy and toxicity of bevacizumab in early, locally advanced and metastatic breast cancer. It recapitulates the main toxicities, gives an overview on biomarker studies and discusses the role and future aspects of antiangiogenic therapy in breast cancer.


Introduction
There is a strong rationale for the usage of antiangiogenic therapies in early, locally advanced and metastatic breast cancer. The concentration of hypoxia-inducible factor(HIF-1)alpha, a key player in angiogenesis regulation, is higher in breast tumors than in normal breast tissue and is even higher in poorly differentiated lesions than in the corresponding type of well-differentiated lesions [1]. Furthermore, increased angiogenesis, measured by vascular endothelial growth factor (VEGF) expression or microvessel density, is an independent negative prognostic factor in early breast cancer [2][3][4].
The addition of the anti-VEGF antibody bevacizumab to standard therapy improved both progression-free (PFS) and overall survival (OS) in several advanced cancers (colorectal cancer, non-small cell lung cancer, ovarian cancer, cervical cancer). In metastatic breast cancer (MBC), however, bevacizumab did not show an OS benefit and increased the grade 3/4 toxicity rate. This led to a discussion about the clinical utility of this drug in this indication. In the neoadjuvant setting, several trials showed an improved pathologic complete response rate (pCR); however, adjuvant trials did not show any effect on disease-free (DFS) or OS. Other antiangiogenic drugs like sunitinib and sorafenib were investigated in advanced breast cancer as well, with consistently negative trial results [5,6]. Therefore, this review focuses on bevacizumab and summarizes the available clinical data in 194 Antiangiogenic therapy in breast cancer K review early, locally advanced and metastatic breast cancer, respectively.

First-line trials
Four prospective phase III trials investigated the efficacy and tolerability of bevacizumab in combination with chemotherapy as first-line therapy in human epidermal growth factor receptor 2(HER2)-negative metastatic breast cancer ( Table 1). The approval for this indication was based on the results of the E2100 trial, where the combination of bevacizumab 10 mg/kg on days 1 and 15 and paclitaxel 90 mg/m 2 on days 1, 8 and 15 every 4 weeks showed a significant and clinically meaningful improvement in progression-free survival (PFS) compared to paclitaxel alone (11.8 months vs. 5.9 months; hazard ratio [HR] 0.60; P < 0.001) [7]. The subsequent phase III trials (AVADO and RIBBON-1), however, found a much less pronounced effect on PFS with other chemotherapybackbones like docetaxel, capecitabine or anthracyclines [8,9]. In AVADO the PFS difference was 1.9 months between docetaxel plus bevacizumab and docetaxel plus placebo [8]. In RIBBON-1 a PFS-difference of 2.9 months in the capecitabine cohort and of 1.2 months in the anthracycline/taxane cohort were reported ( [9]; Table 1). The recently published MERiD-iAN trial, using the same combination as in E2100, showed a similar median PFS of 11.0 months in the bevacizumab/paclitaxel arm compared to the E2100 trial. The control arm, however, performed much better with a median PFS of 8.8 months (5.6 months in E2100) resulting in a lower HR of 0.68 (P < 0.001; Table 1). None of these trials, nor a subsumption in a meta-analysis, showed a benefit in OS by the addition of the anti-VEGF antibody and the rate of grade 3/4 toxicity was increased [10,11]. In HER2-positive disease bevacizumab did not even show a significant improvement in PFS when added to docetaxel and trastuzumab (AVEREL trial, Table 1; [12]).
These results led in November 2011 to the decision of the Food and Drug Administration (FDA) to withdraw the accelerated approval for bevacizumab for the indication breast cancer. In contrast, based on the consistently improved PFS and overall response rate (ORR), bevacizumab is still approved in Europe by the EMA as first-line therapy in HER2-negative metastatic breast cancer when combined with paclitaxel or capecitabine. However, also in European countries like Austria, a significant decline in bevacizumab prescriptions for MBC became evident after the FDA decision [13].
The two approved chemotherapy backbones, each in combination with bevacizumab, were compared within the TURANDOT trial [14]. The primary objective of this study was to show non-inferiority of capecitabine/bevacizumab when compared to pa-clitaxel/bevacizumab in terms of OS. The primary endpoint, in fact, was met (median OS 30.2 months vs. 26.1 months; stratified HR 1.02; P = 0.007 indicating non-inferiority); however, this was not supported by the unstratified analysis. In addition, the median PFS was significantly longer in the paclitaxel arm (10.9 months vs. 8.1 months 95% CI 10.8-12.9; stratified HR 1.32, 95%; P = 0.007) and the objective response was also significantly superior with paclitaxel compared to capecitabine (44% vs 27%; P < 0.001; [14]). In the ATHENA registry, including 2251 patients with HER2-negative breast cancer, the superiority of paclitaxel over capecitabine to improve time-to-progression (TTP: 9.8 months vs. 7.0 months) and response rate (49% vs. 36%) was confirmed (not statistically tested) [15].
Two phase III trials investigated the efficacy and tolerability of bevacizumab in combination with endocrine therapy for locally advanced or metastatic breast cancer. Both trials showed conflicting results: while the CALGB 40503 trial reported a statistically significant improvement in PFS by the addition of bevacizumab to letrozole (20.2 months vs. 15.6 months; HR 0.75; P = 0.016) [16], the LEA trial failed to show superiority (median PFS 19.3 months vs. 14.4 months; HR 0.83, P = 0.126) [17]. In both trials, similar benefits were observed with respect to ORR and clinical benefit rate (CBR), but again neither study showed a difference in OS.

Second-line trials
Two phase III trials investigated bevacizumab after one prior chemotherapy-line for metastatic disease (RIBBON-2 and TANIA). Both trials showed an improvement in PFS by the addition of bevacizumab to different chemotherapy backbones (ΔPFS 2.1 months in both trials; [18,19]). Noteworthy, all patients included in the TANIA trial, where already pretreated with bevacizumab in the first-line setting and received bevacizumab for two additional therapy lines. Thus, the study investigated the principle of treatment-beyond-progression, as it is established in HER2-positive disease with trastuzumab. The primary endpoint, second-line PFS, was significantly longer when bevacizumab was continued (6.3 months vs. 4.2 months, HR 0.75; P = 0.007; [19]). The secondary endpoints, third-line PFS, second-plus third-line PFS and OS, however, where not improved ( [20]; Table 1). The only chemotherapy-based phase III trial in HER2-negative MBC which did not show a significant improvement in PFS was the AVG2119g trial. In this pioneer trial, published already in 2005, patients pretreated with one or two chemotherapy lines for metastatic disease where randomized between bevacizumab plus capecitabine or capecitabine alone. Both the TANIA and the AVG2119g trial indicate that an early application of the anti-VEGF antibody is essential to gain the review

Maintenance therapy
One prospective trial addressed the question of maintenance therapy with bevacizumab after an induction phase with chemotherapy plus bevacizumab. Patients included in the IMELDA trial were treated with six cycles of docetaxel plus bevacizumab and were then randomized to maintenance therapy with bevacizumab alone or in combination with capecitabine. The combination therapy showed significantly improvement in PFS (median 11.9 months vs. 4.3 months; stratified HR 0.38; 95%CI 0.27-0.55; P < 0.0001; [21]) indicating that maintenance bevacizumab alone is not an effective treatment option. Furthermore, the median duration of docetaxel induction was short (3.5 months) which may have contributed to the positive effect of early second-line chemotherapy with capecitabine. Several retrospective case series investigated the question of maintenance therapy as well. A multicenter retrospective observational study, including 314 patients with HER2-negative disease, reported a significantly longer median PFS (18 months vs. 13 months; P < 0.001) and OS (55 months vs. 38 months; P < 0.001) in patients where maintenance therapy was prescribed [22]. These results, however, must be interpreted with caution because such retrospective non-randomized trials harbor the risk of multiple biases.

Neoadjuvant trials
Based on the clear effect on response rate in the palliative setting, three phase III neoadjuvant trials with bevacizumab were started. All three trials showed a significantly higher rate of pathologic complete response (pCR) when bevacizumab was added to neoadjuvant chemotherapy (Table 2; [23][24][25][26][27][28]). The effect on pCR, however, was modest at best (ΔpCR 5-11%) and no significant differences in DFS where reported. In the ARTEMIS trial, patients achieving a pCR in the bevacizumab group showed no longer DFS suggesting a lack of activity against micrometastases. Interestingly, the NSABP B-40 study, which additionally used bevacizumab postoperatively, showed a statistically significant difference in OS in favor of bevacizumab (HR 0.65; 95%CI 0.49-0.88; P = 0.004) [25]. In the context of the other neoadjuvant and adjuvant trials showing no effect on long-term survival; this observation should not be over-interpreted.
A special situation for neoadjuvant treatment is inflammatory breast cancer. Since this subtype is highly angiogenic showing high microvessel density and VEGF expression, an especially strong effect of bevacizumab was expected. A recent single arm phase II trial investigated FEC followed by docetaxel both in combination with bevacizumab every 3 weeks. Postoperatively, all patients received adjuvant bevacizumab (plus endocrine therapy in case of hormonereceptor positivity). The trial did not meet the prespecified criteria for efficacy with a pCR rate of 19% and a 3-year DFS of 57% (95%CI 47-66%) and a median DFS of 53 months (95%CI 31-not estimable); however, longer follow-up is needed for definitive conclusions [29].

Adjuvant trials
In the adjuvant setting three phase III trials were published until now ( Table 3). The BEATRICE trial included patients with triple-negative disease [30,31], the E5103 patients with HER2-negative [32] and the NSABP B44 patients with HER2-positive breast cancer [33]. The Kaplan-Meier curves for disease-free survival (DFS) and OS in all three were completely overlapping. This treatment failure can be explained by the fact that anti-angiogenic drugs can only work at a time point where neoangiogenesis is actually running, which is not the case in the adjuvant setting. Since senescent disease cannot be affected by antiangiogenic treatment and since no clinicopathological characteristics or biomarkers have been identified to indicate bevacizumab efficacy, anti-VEGF therapy has no application in the adjuvant setting.

Biomarker research
The trials results, both in advanced and in early breast cancer, call for biomarkers allowing identification of patients with or without a relevant chance of clinical benefit from this drug. Unfortunately, clinicopathologic parameters like triple-negativity or highrisk features (visceral disease, ≥3 metastatic sites, prior [neo]adjuvant chemotherapy) do not help to identify patients with special benefit from the addition of bevacizumab [10]. In a meta-analysis of the three firstline trials in metastatic breast cancer (E2100, AVADO, RIBBON-1), the hazard ratio (HR) for PFS in these subgroups was similar to the HR in the overall population ranging from 0.60 to 0.64 [10]. Several promising biomarkers like plasma levels of VEGF-A or VEGFR-2 [31,35,36], tissue markers like the VEGFR co-receptor neuropilin-1 (NRP-1) [37][38][39], single nucleotide polymorphisms (SNPs) in VEGF-A [40] or clinical markers like treatment-induced hypertension [40][41][42] showed convincing results in their early development as treatment predictors. However, all these markers either lack validating studies or failed to demonstrate clinical utility or reproducibility. The best example is plasma vascular endothelial growth factor-A (pVEGF-A), which showed a clear predictive value in the exploratory biomarker program of AVADO [36]. Therefore, the double-blind placebo-controlled randomized biomarker phase III trial MERiDiAN used the short isoforms of pVEGF-A as stratification factor [35]. Both co-primary endpoints of the trial were met: in the intent-to-treat (ITT) population, the stratified PFS HR was 0.68 (99%CI 0.51-0.91; P < 0.001) and in the VEGF-Ahigh subgroup, the stratified PFS HR was 0.64 (96%CI 0.47-0.88; P = 0.004). The PFS benefit, however, was similar in the pVEGF-Alow subgroup (HR 0.73; 95%CI 0.52-1.03). The VEGF-A-by-treatment interaction test (P = 0.462) for PFS in the ITT population did not support a predictive effect of pVEGF-A [35].

Future aspects
Despite extensive research, an applicable biomarker for bevacizumab efficacy is still lacking. Further research is ongoing; however, the patent expiry of Avastin ® (Roche, Basel, Switzerland) in 2018 will probably hinder further development. For the same reason, no new phase III trials in breast cancer investigating solely the addition of bevacizumab to standard therapy are expected. However, besides its antiangiogenic activity, bevacizumab has a substantial immunomodulatory capacity. VEGF-A has been shown to suppress dendritic-cell maturation, to inhibit proliferation of regulatory T cells and to attract myeloid-derived suppressor cells [43][44][45]. These immunosuppressive effects are counteracted by bevacizumab. It has been shown that the tumor infiltration by CD4+ and CD8+ T cells and dendritic cells was increased after bevacizumab treatment and that the antigen-presenting capacity of dendritic cells was augmented [46][47][48]. These effects increase the immunogenicity of tumors and could therefore increase the number of patients benefiting from immunotherapy. Because of this potential synergistic effect, several combination studies with checkpoint inhibitors and bevacizumab are ongoing in different cancer types (colorectal cancer-NCT02982694, renal cell carcinoma-NCT02724878 and NCT01984242, melanoma-NCT03175432, cervical cancer-NCT029 21269, and non-small cell lung cancer-NCT02366143). In case of positivity, the immunological effect of antiangiogenic therapeutics, which has been ignored for a long time, could lead to new treatment indications and new therapeutic goals, probably also in breast cancer.
Take home message Bevacizumab consistently prolonged progression-free survival and increased response rate in metastatic HER2-negative breast cancer in first-and second-line. An effect on overall survival, however, was not observed stirring up a debate about the value of bevacizumab in this indication. In the neoadjuvant setting the pathologic complete response rate (pCR) was increased, however in adjuvant trials no effect on disease-free survival was reported. Therefore, antiangiogenic treatment is not standard in early and locally advanced breast cancer at least until a biomarker for patient selection is available.