Clinico–pathologic factors and survival of patients with breast cancer diagnosed with de novo brain metastasis: a national cancer database analysis

Purpose Patients with Breast Cancer (BC) with Brain Metastasis (BCBM) have poor survival outcomes. We aimed to explore the clinico–pathologic and therapeutic factors predicting the survival in patients with de novo BCBM using the National Cancer Database (NCDB). Patients and methods The NCDB was queried for patients with BC between 2010 and 2020. Survival analysis with Kaplan–Meier curves and log rank tests were used to find median overall survival (OS) in months (95% CI) across the different variables. A multivariate cox regression model was computed to identify significant predictors of survival. Results Out of n = 2,610,598 patients, n = 9005 (0.34%) had de novo BCBM. A trend of decreasing OS was observed with increasing age, Charlson–Deyo score (CDS), and number of extracranial metastatic sites. The highest median OS was observed in the Triple Positive and the lowest OS in the Triple Negative subgroup. Based on treatment regimen, combination of systemic therapy and local therapy achieved the highest OS. A positive trend in OS was observed in the BC subgroup analysis with targeted therapy demonstrating a survival benefit when added to systemic therapy. The multivariate cox regression model showed that age, race, ethnicity, insurance, median income, facility type, CDS, BC subtype, metastatic location sites, and treatment combinations received were significantly associated with risk of death. Receiving only local treatment for BM without systemic therapy more than doubled the risk of death compared to combining it with systemic therapy. Conclusions This analysis suggests that treatment of systemic disease is the major factor influencing survival in patients with BCBM. Moreover, targeted therapy with anti–HER2 increased survival when added to systemic therapy explaining the highest median OS noted in the Triple Positive subgroup. Supplementary Information The online version contains supplementary material available at 10.1007/s10549-024-07321-x.


Introduction
Breast Cancer (BC) ranks as the most common malignancy among females worldwide with an annual incidence of 2.3 million cases [1,2].Specifically, BC with metastasis at diagnosis (de novo metastatic BC) comprises 3-6% of all BC patients and presents a major clinical challenge as these patients have limited-life expectancy [3], with an estimated five-year survival of metastatic BC in women residing in the US limited to 30% [4].The most common sites of BC metastases include bone, liver, lung, and brain, of which the brain metastatic group has the worst survival outcomes [5].BC is the second most common source of brain metastases (BM) after lung cancer [6].The incidence of breast cancer brain metastases (BCBM) has increased steadily over the last several years owing to improved management of the primary disease [7].Many studies have explored the factors that might predict survival in patients with BCBM, with many factors identified including age, race, marital status, histology, grade, tumor size, molecular subtype, patterns of metastasis, history of chemotherapy, radiotherapy, and surgery of primary cancer [8,9].Such studies have led to the development of prognostic scores that help in clinical decision making, such as the well-studied Graded Prognostic Assessment (GPA) scoring tool, which was developed to estimate survival in different BM patients based on the tumor of origin [10].Some of the significant factors used in the score include age, Karnofsky Performance Status (KPS), extracranial metastases, and number of BM [2].According to the National Comprehensive Cancer Network (NCCN) guidelines, treatment of BM includes surgery for relief of symptoms, whole brain radiotherapy (WBRT), stereotactic radiosurgery (SRS), and palliative care if applicable [11].Additionally, BCBM require treatment based on the primary tumor characteristics including chemotherapy, hormonal, and anti-HER2 targeted therapy [12,13].There is a growing number of studies and clinical trials investigating newer targeted therapies for BCBM which span different classes such as EGFR receptor modulators, tyrosine kinase inhibitors, and CDK4/6 inhibitors to name a few [14][15][16][17][18][19][20][21][22].Despite our growing knowledge about BCBM and the many efforts to identify prognostic and therapeutic interventions, large population-based survival studies on de novo BCBM remain lacking.Therefore, we aim to retrospectively analyze the national cancer database (NCDB) to identify factors and therapeutic interventions predicting survival of patients presenting with BCBM (Figs. 1 and 2).

Patient data
The NCDB was queried for patients with BC with available data on de novo BM between 2010 and 2020.A total of n = 2,610,598 records of patients with BC were identified, out of whom 9005 had de novo BM.Access to this registry was achieved based on a Participant User File award granted to the principal investigator (N.Z.).The NCDB is a clinical oncology database sourced from hospital registry data collected in more than 1500 Commission on Cancer-accredited facilities (amounting to about 70% of all cancer diagnoses in the country).These data are used to analyze and track patients with malignant neoplastic diseases, their treatments, and outcomes.Variables used from the dataset included facility and patient demographics, BC-specific variables, and treatment modalities.Several variables were computed that are relevant to prognosis in this patient population.Variables for the number and location of extracranial metastatic sites (EMS) were computed by combining five individual metastatic sites: bone, liver, lung, distant lymph nodes, and other sites.A variable on BM treatment modality was computed by combining three individual modalities: Surgery, WBRT, and SRS.A variable on BC treatment modality was computed by combing three individual modalities: chemotherapy, hormonal therapy, and immunotherapy (referring to anti-HER2 therapy and other targeted therapies).Last, a variable on treatment combination was computed by combining the treatment status for BM and BC.

Statistical analysis
Chi-square, fisher exact, independent t, and Mann Whitney U tests were performed to evaluate the association between each categorical variable and treatment combinations received.Kaplan-Meier analyses and log rank tests were performed on the whole dataset to compare median overall survival (OS) across age, facility type, Charlson-Deyo Score (CDS), BC subtype, number of EMS, location of EMS, BM treatment modality, BC treatment modality, and combination of both treatment modalities.Furthermore, the same analysis was conducted on the four BC subgroups to compare OS across the different treatment modalities.Finally Univariate and Multivariate Cox regression models were computed with backwards elimination of 0.1 for both to identify the significant predictors of survival in the patient cohort.The cutoff of statistical significance was set at p < 0.05.SAS version 9.4 and R 4.2.3 were used for data analysis.

Median OS of the Cohort across different variables
The median OS of the 9005-patient cohort was 10.9 months (95% CI, 10. 3-11.5)(10.4-13.6),which is very similar to our cohort's value of 10.9 months [23].Furthermore, the authors identified similar trends in subgroup survival, with the HR( +)/HER2( +) group having the best OS at 19.0 months (11.8-26.2) and the HR( − )/HER2( − ) having the worst OS at 7.0 months (5.4-8.6), both of which overlap with our results.Moreover, there was a similar trend in the OS of patients based on the metastatic sites with the bone only group having the longest OS (17.0 vs 16.5 months in our cohort) and all three sites (bone + liver + lung) having the lowest OS at 8.0 months (5.4-10.6)compared to Overall, Surgery + WBRT yielded the best survival benefit amongst BM treatments, and these findings were also consolidated in the BC subgroup analysis.This is in line with the findings of the GPA study by Sperduto et al. which found that Surgery + WBRT treatment achieved the highest OS amongst all other combinations in BCBM patients at 25 months [2].On the other hand, a recent systematic review on radiation therapy for BM identified five randomized trials conducted on post-surgical radiotherapy (SRS or WBRT) and found no differences in OS in the pooled results [25].A growing number of clinical trials are ongoing to explore the best treatment modality for the local treatment of BCBM patients [6].
Overall, Chemotherapy + Hormonal Therapy + Immunotherapy yielded the best survival benefit amongst all BC treatments, findings also observed in the BC subgroup analysis.Of note, immunotherapy consistently improved survival across all the BC subtypes when added to systemic therapy.For example, in the HR( +)/HER2( − ) subgroup, adding targeted therapy more than doubled survival when added to the hormonal therapy alone group (from 15.38 to 31.54 months) and to the Chemotherapy + Hormonal therapy group (from 26.91 to 55.13 months).There is a growing number of studies and clinical trials that are investigating promising targeted and biologic therapies to target BCBM and shown survival benefits [12] which could explain the improved survival outcomes in our analysis with the addition of anti-HER2 therapy and other targeted therapies.Some of the drugs being explored include the anti HER2 targeting antibodies including: Trastuzumab [26,27], Trastuzumab Emtansine [28,29], Trastuzumab Deruxtecan [30], and Pertuzumab [31]; tyrosine kinase inhibitors including: Lapatinib [32][33][34][35], Neratinib [36][37][38], Afatinib [39], Tucatinib [40], Taselisib [41], Alpelisib [42], Buparlisib [43]; and CDK 4/6 inhibitors including: Palbociclib [44], Ribociclib [45], and Abemaciclib [46]; among other classes of targeted therapies.Unfortunately, the biologic agents used in treatment of the BCBM patient cohort are not available in the NCDB, but the trend of improved survival speaks to the rapid development of new targeted therapies that are currently under study.One example is the approval of Pembrolizumab for neoadjuvant and adjuvant treatment of patients with high-risk early-stage triple-negative BC in 2021 [47].The study at hand is limited to 2020 and hence outcomes may improve even more for triple negative breast cancer in the coming years with more targeted therapies approved.
In the combined treatment analysis, receiving treatment for BM alone did not seem to prolong survival.Furthermore, treating BC alone achieved similar survival to treating both BC and BM.This suggests that the major therapeutic contributor to OS in de novo BCBM patients is the treatment of the underlying primary tumor rather than the BM itself.This finding is further supported by the findings of the multivariable cox regression model which integrates all the variables to identify and validate the individual survival benefits.In the model, treatment of BM alone increased the risk of death 2.3 folds compared to receiving dual treatment, which suggests that it is the BC treatment that confers any survival benefit.

Limitations
The study at hand has several limitations by virtue of it being conducted on a retrospective database which impedes control of certain variables.Furthermore, the NCDB does not provide information about relevant prognostic indicators identified in many studies such as number and size of BM, KPS, and the type of chemotherapy and targeted therapy received.Additionally, it was not possible to delineate the extent of BM surgery, and the radiation dose and number of treatment fractions to the BM in the analysis.Last, the NCDB provides information only about de novo BM and not recurrent BM.Recurrent BM constitutes a bigger percentage of BM and remains an important factor to consider when predicting prognosis.Despite these limitations, this remains, to the best of our knowledge, the biggest cohort of de novo BCBM patients to date and provides valuable information for clinical practice.

Conclusion
We retrospectively analyzed the biggest cohort of de novo BCBM patients exploring clinical and therapeutic factors associated with survival.Our results maintain the short survival of BCBM patients while also providing subgroup specific values that can guide clinical decision making.The BM-specific treatment that yielded the best survival outcomes was surgery combined with WBRT, and targeted therapy improved survival when added to systemic therapy across all subgroups.Further analysis showed that treating BM alone may decrease survival compared to receiving treatment for both BM and BC indicating that the primary disease is the main predictor of survival, and the BM management may serve a palliative role.Prospective studies are needed to consolidate these findings and to further highlight the role of targeted personalized therapy in improving survival of patients with BCBM.

Fig. 1
Fig. 1 Kaplan-Meier plots of overall survival for breast cancer patients with brain metastases stratified by a age, b facility type, c Charlson-Deyo score, d breast cancer subtype, e number of extracranial metastatic sites, and f location of extracranial metastatic sites

Fig. 2
Fig. 2 Kaplan-Meier plots of overall survival for breast cancer patients with brain metastases stratified by a brain metastases treatment modality, b breast cancer treatment modality, and c combination of both breast cancer and brain metastases treatments

Table 4
Univariate and multivariate cox regression models for variables predicting risk of death in the patient cohort

Table 4 (
[24]inued) Similar trends were also observed in another study conducted on 248 patients with de novo BCBM between 2010 and 2018 from the SEER database[24].In our analysis, OS decreased with increasing age, number of comorbidities, and number of EMS, which is in line with previously noted studies.