oligometastatic disease

De Novo Oligometastatic Breast Cancer

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Metastatic breast cancer may present clinically either as recurrence after a previous diagnosis of stage I-III disease or as de novo metastatic breast cancer that is also called stage IV disease according to the American Joint Committee on Cancer (AJCC) tumor, node, metastasis classification.1 Recurrent metastatic disease arises from clinically undetectable distant micrometastases that were already present at the time of diagnosis, were not eradicated by systemic adjuvant therapies, and grew into clinically detectable macrometastasis after a variable duration of tumor dormancy. In this conceptual framework, de novo metastatic breast cancer is a disease where micrometastases have no dormant period or the dormancy has passed before diagnosis. What determines the duration of cancer cell dormancy and how cells emerge from dormancy remain largely unknown.2 Approximately 6%-7% of newly diagnosed breast cancers present as de novo metastatic disease in the United States,3 and this proportion is larger in middle-income countries. While this fraction remained stable in the past 20 years, the absolute number of patients diagnosed with de novo metastatic breast cancer is increasing because of a growing population and more sensitive imaging technologies for staging, an estimated 18,000 patients will be diagnosed with stage IV breast cancer in 2023 in the United States.3,4 As adjuvant systemic therapies become more effective in eradicating micrometastatic disease, metastatic recurrences in stage I-III breast cancers are decreasing, and the proportion of de novo metastatic cancers is increasing. Historically, about 20% of patients with newly diagnosed metastatic breast cancers had de novo disease; in comparison, the contemporary rates are closer to 30%-40%.5,6 Clinically, a fundamental difference between recurrent and de novo metastatic disease is exposure to prior therapies. Most patients with recurrent metastatic disease have been exposed to prior systemic therapy, and their recurrent disease represents growth of partially treatment resistant cells. Despite a potentially major difference in sensitivity to systemic therapies, current treatment guidelines for metastatic breast cancer do not distinguish between recurrent and de novo metastatic cancers. A further clinical subset within de novo metastatic cancers is oligometastatic disease that could be rendered no evidence of disease (NED) with locoregional and metastases-directed therapy.

Molecular Evolution of Metastatic Breast Cancer

Phylogenetic analysis of primary tumors and metastatic lesions from the same individual revealed three distinct paths to metastatic dissemination with clinical implications.79 First, metastatic spread can occur early from a common ancestor of both the primary tumor and distant metastases, resulting in lesions evolving simultaneously. This phenomenon may explain why small primary tumors could present as micrometastatic disease. Second, metastases may arise from a small subpopulation of cells that develop within the primary tumor, which is consistent with the clinical observation that primary tumors left untreated will eventually metastasize. Finally, metastatic lesions can also give rise to new metastases, which implies that as long as any viable metastatic lesion exists, the potential to disseminate to other distant sites remains. All three types of dissemination can be observed in the same patient; the limited data that exist today suggest that the parallel evolution from a common ancestor to both the primary and the metastasis is the most common path. Another important discovery was that the molecular features of the cancer change over the course of the disease. Metastatic lesions acquire new genomic alterations spontaneously and under selective pressure from therapies.10 Comparison of primary tumors and metastatic lesions also revealed that synchronous metastases have a more similar genomic architecture to the primary tumors, presumably due to shorter divergence time and lack of therapeutic selective pressure, whereas asynchronous metastases show a larger number of genomic differences compared with the primary tumor.711 This observation raises the possibility that synchronous metastases have similar treatment sensitivities to the primary tumor. This hypothesis is supported by clinical observations including high rates of pathologic complete response (pCR) in biopsy-proven synchronous lymph node metastases in patients who achieve pCR in the breast with neoadjuvant chemotherapy12,13 and longer progression-free survival (PFS) with initial therapy in patients with de novo compared with recurrent metastatic disease.6,1416

Oligometastatic Disease

The extent of metastatic disease at the time of diagnosis varies from a single or few metastatic lesions to extensive disease with many lesions in multiple organs. Oligometastatic disease is defined by the European Society for Medical Oncology and by the European Society for Radiotherapy and Oncology and American Society for Radiation Oncology as a disease with up to five lesions each amenable to local therapy aimed at achieving a NED status.17,18 Approximately 40% of newly diagnosed metastatic breast cancers, including de novo disease, are oligometastatic.19,20 Multiple studies showed longer overall survival (OS) for oligometastatic de novo metastatic breast cancers, which may be due to (1) slower growth rate and more limited metastatic ability of these cancers, (2) lead time bias (ie, being diagnosed at an earlier time point during the course of the disease), or (3) more aggressive treatment approaches including local ablative therapy in addition to systemic therapy.21,22 The individual contributions of these potential causes are difficult to distinguish on the basis of current data. In breast cancer, several retrospective studies documented 20-year disease-free survival in a quarter of patients who were rendered NED with multimodality local and systemic therapies.2230 Analysis of the National Cancer Database (NCDB) including 12,838 patients with de novo metastatic breast cancer also showed improved survival among patients who received trimodality therapy (ie, surgery, radiation, and systemic therapy) compared with patients who had systemic therapy only.29 These studies indicate that long-term disease control is possible in select patients with oligometastatic cancers; however, these retrospective studies are all subjects to selection bias since patients treated with multimodality therapy were likely younger with fewer comorbidities and better overall prognosis. Two small phase II randomized trials, including mostly recurrent oligometastatic cancers, showed no benefit from stereotactic ablative body radiotherapy (SABR) in breast cancer. The SABR-COMET phase II randomized trial enrolled 99 patients with a variety of cancers and ≤5 metastatic sites; the 5-year OS was improved in the SABR arm, but there was no difference in outcomes in the very small breast cancer subset (n = 18).31 The randomized NRG-BR002, that accrued patients with oligometastatic breast cancer (N = 125), that had not progressed on initial systemic therapy within 12 months also found no statistically significant improvement in progression-free survival (PFS), OS, or new metastases rate.32 These results indicate that SABR to stable oligometastatic lesions of recurrent estrogen receptor–positive (ER+) metastatic cancers have very limited (hazard ratio for PFS: 0.92), or no, effect on survival end points. Because 71% of patients in BR002 had recurrent metastatic disease and 80% had ER-positive breast cancer, it is uncertain to what extent these results may be extrapolated to patients with oligometastatic stage IV disease. Among the 25 patients with de novo metastatic cancer, the 24-month PFS rates were 70% and 65% in the SABR plus systemic therapy and systemic therapy alone arms, respectively. These differences were not statistically significant. Several randomized trials continue to examine the value of SABR in oligometastatic breast cancers (Table 1).

Table 1. Ongoing Clinical Trials for Patients With Oligometastatic Breast Cancer

Impact of Management of the Primary Tumor in De Novo Metastatic Breast Cancer

Four randomized trials addressed whether surgical removal of the primary tumor is beneficial in de novo metastatic breast cancer. The Tata Memorial trial showed no survival benefit from locoregional therapy,33 and the ABSCG-28-Posytive trial was terminated early because of low accrual but suggested no benefit.34 By contrast, the MF07-01 trial showed a 34% improvement in OS in the locoregional therapy arm.35 The most recent trial, EA2108, randomly assigned patients who responded or had stable disease after 4-8 months of initial systemic therapy to surgery and radiation to the primary tumor site versus continuing systemic therapy. The trial showed that locoregional progression was less frequent in the locoregional therapy arm (3-year rate: 16.3% v 39.8%; P < .001), but there was no improvement in OS.36 Each of these trials included both oligometastatic and nonoligometastatic cancers; in EA2108, very few participants received ablative therapy to metastatic sites, and systemic therapies were standard-of-care metastatic treatments. Collectively, these studies established that selectively removing some of the cancer (ie, the primary tumor) without ablating all lesions is not beneficial in de novo metastatic breast cancer. Unfortunately, these trials cannot answer whether removing the primary tumor and ablating all detectable distant metastatic lesions, coupled with molecular subtype-specific multidrug systemic therapy, could improve survival of oligometastatic de novo metastatic disease.

The National Comprehensive Cancer Network guidelines do not include distinct treatment recommendations specifically for patients with oligometastatic de novo metastatic breast cancer.37 By contrast, the European Society for Medical Oncology guidelines acknowledge that patients with oligometastatic de novo disease may achieve complete remission after systemic therapy and have a potential for longer survival and hence a multimodal approach including locoregional therapy with curative intent should be considered for selected patients.38 Routine practice in the United States reflects a highly variable approach to the management of patients with de novo oligometastatic breast cancer. Analysis of the NCDB data showed that approximately 52% of patients were treated with systemic therapy only, 22% received systemic therapy plus radiation treatment, 13% had systemic therapy and surgery for the primary tumor, and 12% received multimodality therapy between 2010 and 2015.29

Unanswered Questions and Future Directions

The current therapeutic approach in patients with early-stage disease is based on four decades of clinical trials that have established the critical importance of multimodality therapy in improving survival. Patients at high risk for recurrence are treated with surgical resection of all detectable disease in the breast, resection or radiation of ipsilateral axillary lymph nodes, locoregional radiation therapy to eradicate microscopic residual disease in the ipsilateral breast, and adjuvant, molecular subtype-specific, multidrug systemic therapy that has become increasingly effective in eliminating distant microscopic disease. No prospective randomized trial has tested whether the same multimodality treatment strategy that we apply to stage III breast cancers might also improve survival in de novo oligometastatic breast cancer. The hypothesis that some of these patients may achieve long-term survival with multimodality therapy is supported by several retrospective case series.39,40 However, the promise of benefit from multimodality therapy have not yet been demonstrated by clinical trials, and enthusiasm must be tempered by the significant short- and long-term morbidity from aggressive local therapies. Surgical removal of the primary tumor is associated with all the risks and costs of a surgical intervention. Although modern SABR techniques are generally safe, a meta-analysis of 21 clinical trials including 948 patients treated with SABR for oligometastatic disease showed that up to 10% of patients may experience acute or late grade 3 or greater toxicity.21,41 Multidrug regimens that combine the most effective agents into an adjuvant-like treatment administered to patients with de novo oligometastatic disease may also deprive patients from using the same agents sequentially during progression and could limit future treatment options. It is, therefore, crucial to investigate in prospective randomized trials the potential benefits and toxicities of multimodality therapy for oligometastatic de novo metastatic breast cancer. A prospective online registry study (CHLOE) is currently open for patients with stage IV oligometastatic human epidermal growth factor receptor 2-positive breast cancer to collect outcomes with multimodality therapy in the real-world setting.42

In summary, accumulating clinical and molecular data suggests that de novo metastatic breast cancers represent a distinct subset of metastatic disease where distant metastases often share molecular similarities with the primary tumor, and these cancers are all treatment naïve. Among these patients, those with oligometastatic disease represent a unique subset that could be rendered NED, through a combination of surgery and SABR. This clinical setting resembles patients with stage IIIC disease after surgical resection and radiation therapy; in both settings, macroscopic disease was eliminated, but the presence of micrometastasis is very likely, or certain. In stage III disease, adjuvant/neoadjuvant systemic therapies improved survival and reduced distant recurrence rates dramatically in the past 30 years. It is time to test if the same multimodality strategy might also improve survival in oligometastatic de novo breast cancer. Until 2002, supraclavicular lymph node involvement at presentation was considered M1 (stage IV) metastatic disease, and these patients were considered incurable and often received systemic therapies only with palliative intent. However, clinical data indicated that this group of patients when treated with combined modality therapy had long-term survival similar to stage III breast cancers,43 eventually leading to reclassification to N3c (stage IIIC) disease (AJCC edition 7), and today they all receive multimodality therapy with curative intent. Might in one day we consider oligometastatic stage IV breast cancer as stage IIID disease?

Is it time for redefining oligometastatic disease? Analysis of lung metastases CT in ten tumor types

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Abstract

Background

Oligometastatic disease (OD) is usually defined arbitrarily as a condition in which there are ≤ 5 metastases. Given limited disease, it is expected that patients with OD should have better prognosis compared to other metastatic patients and that they can potentially benefit from metastasis-directed therapy (MDT). In this study, we attempted to redefine OD based upon objective evidence that fulfill these assumptions.

Discussion

The concept of OD envisioned by Samuel Hellman in 1995 has attracted much attention in recent years [1,2,3,4,5, 8, 11, 12]. It hypothesizes an interim condition in which a tumor has spread to only a few sites and cure by MDT may be possible. Unfortunately, there is no reliable biomarker for OD and no universally accepted definition [10]. In most studies, OD was arbitrarily defined as a condition in which there are five metastases or less in imaging studies that are technically treatable with MDT [7]. In this study, we suggest adding metastases clonal origin to the definition of OD to identify those patients with greatest chance for cure by MDT.

Tracking a given metastasis’ clonal origin is not an easy task. It requires retrieval of tumorous tissue and complex genetic and epigenetic studies [13,14,15]. However, in a previous study it was showed that the relatively straightforward analysis of metastases number and diameter may provide readily available information regarding clonal origin by differentiating between linear and parallel patterns of appearance [9]. In brief, the linear model asserts that when a malignant clone gains the capabilities needed to become a metastasis (invasion, angiogenesis etc.); a cluster of metastases disperses from this clone. Since all these metastases have the same clonal origin and commission time, a similar growth rate is expected at any landing site. Thus, all metastases originating in that clone have a similar diameter in any specific organ at any time point. Additional clones may reach this maturity and spread as clusters of metastases but for each cluster, a distinct diameter of all its metastases is expected. By contrast, the parallel model suggests early spread of disseminated tumor cells (DTCs). These cells mature to metastases independently in the target organs and are therefore expected to be at varying diameters. LPR quantitatively displays how much of the tumorous spread was linear and how much parallel. LPR =  + 1 means unmixed linear spread and LPR = − 1 unmixed parallel.

Clearly, the ideal patient to be defined as possessing OD will have a pure a linear (LPR =  + 1), monoclonal, single cluster of metastases, preferably with only a few tumors technically permitting MDT. Patients with a linear multi-clonal or parallel metastatic spread have a more genetically diverse disease and are expected to respond less well to MDT. It is therefore anticipated that a patient with “true” OD will demonstrate a better prognosis compared to patients with non-OD.

In this study using chest CTs of patients with lung metastases originating in ten different malignancies, we showed that patients with a single metastasis or a single cluster of metastases demonstrating diameter variations of 1 mm or less can be classified together into a group possessing significantly better prognosis compared to other patients with metastatic disease (Table 1 and Figs. 1a and 2a). We also showed that if metastases diameter is ignored, the prognosis of patients with 2–5 metastases is similar to that of patients with 6–10 metastases; supporting the concept the five metastases upper limit requirement of OD is probably not biologically true. (Fig. 1b).

Not all tumor types showed the same prognostic dependence on the number of metastases and metastatic clusters. Metastases number had no significant prognostic impact in cancers of the breast, prostate, thyroid, pancreas, and stomach. This is probably due to the small number of patients with a single metastasis in these tumors (only 2, 1, 0, 7, and 3 patients with these tumor types respectively). Metastatic cluster number had no significant impact on the prognosis of patients with tumors of the bladder, breast, melanoma, prostate, and stomach. This could also stem from a small number of patients with a single metastases cluster (only 3, 6, 4, 10, and 8 patients with these tumor types respectively).

Variability of metastases number between clusters and LPR also showed a highly significant impact on OS (p < 0.0001). Both parameters are related to genetic diversity of the metastases. This observation is important scientifically and supports the previous conclusion. However, since these parameters are less intuitive and require computerized calculation, it is suggested not to include them in the definition of the OD. As stated earlier, a single cluster means LPR =  + 1. In search of confounders to this model, the features of patients with single and multiple clusters of metastases were compared (supplementary material S5). Tumor’s origin and patients’ age were similar but there were significantly more men than women in the single cluster group (66.4% Vs. 52.9%, p = 0.06). Gender itself had no significant effect on OS (supplementary material S6) so the significance of this finding is not clear and merits further studies.

The model presented here, with the suggestion of qualifying only patients with a single metastatic cluster (representing a single clone) in the definition of OD, is obviously oversimplified. Yet it could be useful for planning clinical research in OD and may potentially provide better results compared to the poor results obtained with the standard definition of five metastases or less [3,4,5, 8].

We acknowledge that this study has several notable limitations:

  1. 1. Although patients with a single cluster of metastases showed significantly better prognosis, this may not automatically translate into better response to MDT.
  2. 2. Metastases growth rate may be influenced by proximity to anatomical structures; thus, metastases originating in a single clone may grow at different rates and mimic several clones.
  3. 3. Similarly, an earlier slow growing clone can reach the same diameter as a later but faster growing clone. In this way, several clones may mimic a single clone. Given the improved survival of patients with a single cluster noted according to the proposed model, this condition is unlikely.
  4. 4. This study was performed on lung metastases only. Measurement of metastases diameter in other organs is less straightforward and may show different results. Thus, further assessment of these alternative tumor microenvironments will be necessary.
  5. 5. Primary tumor control and metastases outside the lungs were not considered in the analysis. As shown by Niibe et al. patients with 1–5 metastases after control of the primary tumor (oligo-recurrent disease) have good prognosis with three-year OS of 64% after SABR [12].
  6. 6. Only metastases largest diameter was considered here, due to the simplicity of its measurement. Future studies assessing the potential role of lesion volume and perhaps using deep learning techniques are encouraged.

In summary, this study addresses OD from a biologic/pathophysiologic rather than surgical/anatomic point of view. We demonstrate that patients with a single cluster of metastases, potentially originating from a single clone, even with more than five lesions, have significantly better prognosis compared to patients with polyclonal disease. Accordingly, we propose including monoclonality in the definition of OD. The upper limit of metastases number should not be set arbitrarily and should be determined by the technical capabilities of the MDT. These criteria can potentially improve patient selection for MDT and provide a higher percentage of curative procedures for patients with metastatic disease.

Fig. 3

Representative scans of patients diagnosed with a few metastases with similar diameters representing a single (presumably monoclonal spread) cluster. a-liposarcoma, b-pancreas, c-stomach. These patients are suitable for inclusion in an oligometastasis trial. Patients were diagnosed with few metastases but with different diameters (presumably representing multiclonal spread) d-colorectum, e-melanoma, f-osteosarcoma. Despite having only a few metastases, these patients may not be suitable for inclusion in an oligometastasis trial,

Source: springer.com