The mode of progressive disease affects the prognosis of patients with metastatic breast cancer

Patients with metastatic breast cancer (MBC) are treated with drug therapies, such as hormone therapy and chemotherapy. Although MBC is still an incurable disease [1], the survival of such patients has been improved by new therapeutic agents [2, 3]. The efficacy of drug therapies is evaluated by imaging modalities, such as computed tomography (CT), bone scintigraphy, and positron emission tomography (PET), and the therapy is continued as long as it seems to be effective [4]. The efficacy of drug therapies is evaluated based on Response Evaluation Criteria in Solid Tumors (RECIST) especially in clinical trials [5] as well as in daily practice.

Under the RECIST criteria, the efficacy is divided into four categories: complete response (CR), partial response (PR), stable disease (SD), and progressive disease (PD). Usually, the therapy is changed when the efficacy is evaluated as PD. According to the RECIST criteria, PD is diagnosed under two conditions: an increase in the size of pre-existing lesions and the appearance of new lesions [5]. These situations should be interpreted as indicative of the progress of metastatic disease. However, the precise meanings of these situations seem to differ, as the size of pre-existing lesions may be decreased again by subsequent therapy, while new lesions rarely disappear, regardless of therapy. Thus, the European Medicines Agency (EMA) has recently recommended that the mode of progressive disease (an increase in the size of pre-existing lesions or the appearance of new lesions) should be taken into account when progression-free survival (PFS) is used as the endpoint of a clinical trial [6].

Given the above, we suspected that the prognosis of patients with new metastatic lesions might differ from that of patients whose pre-existing metastatic lesions have only increased in size. Therefore, we retrospectively investigated the prognosis of these patients after PD and the relationship between the mode of PD and drugs.

The records of breast cancer patients who received drug therapy for locally advanced or metastatic breast cancer at Gifu University Hospital between 2004 and 2015 were reviewed. The therapy in each case was investigated, and the efficacy of drug therapy was evaluated from the viewpoint of the objective response, which was categorized as mentioned above: CR, PR, SD, and PD. This categorization was determined based on the RECIST criteria.

In the present study, PD was further divided into the appearance of new lesions (NL) and an increase in the size of existing lesions (IS). NL indicates that the patient developed new metastatic lesions that had never been detected before, regardless of the size of pre-existing lesions. IS indicates that the target lesions had increased in size, and no new lesions had developed. When judging the mode of PD, the most recent therapies the patients had received were excluded, as the efficacies of these therapies were deemed poor and had not been evaluated sufficiently in most cases. We then compared the survival after PD between the patients with NL and IS using the Kaplan–Meier curves with a log-rank test and calculated the frequency of NL to determine which drugs was most strongly associated with NL. We also analyzed the impact of these factors on the patients’ survival using a Cox proportional hazard model. All statistical analyses were carried out using the software EZR software program (version 3.4.1 with R commander 2.4–0).

This study was approved by the ethics committee of Gifu University, Graduate School of Medicine.

We analyzed the relationship between the mode of PD and the prognosis and found that the survival time in patients who developed NL at second-line chemotherapy was statistically worse than that in patients with IS.

Some reports have described the relationship between the mode of PD and the prognosis. In the RECORD-1 study investigating the benefit of everolimus over placebo for metastatic renal cell carcinoma, a multivariate Cox proportional hazard model revealed that the growth of non-target lesions and appearance of new lesions were predictive factors for the overall survival [7]. In the Nordic VI trial comparing FLIRI therapy and Lv5FU2-IR therapy for metastatic colorectal cancer, patients with new lesions or unequivocal progression of non-measurable lesions had a worse prognosis than those with an increase in the size of pre-existing lesions, and a ≥ 10% decrease in the size of pre-existing lesions was a positive prognostic factor [8]. Another report has also described the influence of the mode of PD on the overall survival in MBC. Twelves et al. reported that, in study 301 and study 305, which investigated the efficacy of eribulin for MBC, patients who developed new metastases had a worse prognosis than did those with PD due to the growth of pre-existing lesions [9]. Kotake et al. also reported similar findings based on the data from Japanese patients receiving eribulin [10]. The results of these studies have consistently suggested that new lesions are associated with a worse prognosis than IS after PD, which agrees with the findings of the present study. These present and previous findings suggest that simply observing MBC patients whose lesions have slightly increased in size without changing the therapy may be feasible, as long as new lesions do not appear.

Litiere et al. also reported that an increase in the size of target lesions had a low explanatory value, and the appearance of new lesions and the progression of non-target lesions resulted in a worse overall survival, according to the results of a meta-analysis investigating the explanatory values of the mode of PD based on the RECIST criteria in breast, lung, and colorectal cancer. Therefore, those authors suggested that this information be included in the updated version of RECIST [11]. According to the current consensus, the drug therapy in MBC patients must be changed when PD develops [1]. However, we have limited effective drugs. Therefore, if we were to distinguish the treatment protocol after PD between patients with NL and those with IS, we could continue otherwise effective drug therapies for longer.

Another important finding of our study is that NL at second-line chemotherapy itself was not an independent factor for the total survival. NL at second-line chemotherapy is related to a poor prognosis after PD, and patients receiving maintenance therapy frequently develop NL. However, this does not necessarily mean that the total survival time is shortened. The mode of PD was a factor for predicting not the total survival time but only the survival time after PD.

Despite the small population and retrospective nature of the present study, we believe that our results provide some important evidence to support our hypothesis and that these findings may help prolong the survival of patients using limited drugs for metastatic breast cancer. A larger prospective study investigating the prognoses of patients with NL and IS will be required in the future.

We found that patients with NL had a worse survival after PD than did those with IS. When patients develop NL, their therapy must be changed. However, patients with only IS might be able to be observed without changing their therapy, allowing them to continue otherwise effective drug therapies for longer.