Current approaches to the management of Her2-negative metastatic breast cancer

While metastatic breast cancer (MBC) remains incurable, a vast array of active therapeutic agents has provided the opportunity for long-term disease control while maintaining quality of life and physical function. Optimal management of MBC balances a multitude of factors, including a woman's performance status, social support, symptoms, disease burden, prior therapies, and surrogates for tumor biology. Choosing the most appropriate initial therapy and subsequent sequence of treatments demands flexibility as goals and patient preferences may change. Knowledge of the estrogen receptor (ER), progesterone receptor (PR), and Her2 receptor status of the metastatic tumor has become critical to determining the optimal treatment strategy in the metastatic setting as targeted therapeutic approaches are developed. Patients with ER+ or PR+ breast cancer or both have a wide array of hormonal therapy options that can forestall the use of cytotoxic therapies, although rapidly progressive phenotypes and the emergence of resistance may ultimately lead to the need for chemotherapy in this setting. So-called 'triple-negative' breast cancer - lacking ER, PR, and Her2 overexpression - remains a major challenge. These tumors have an aggressive phenotype, and clear targets for therapy have not yet been established. Chemotherapy remains the mainstay of treatment in this group, but biologically based clinical trials of new agents are critical to developing a more effective set of therapies for this patient population.


Hormone-sensitive metastatic breast cancer
Two thirds of women with diagnosed breast cancer have disease that is estrogen receptor/progesterone receptorpositive (ER/PR + ) [7]. Th ese tumors are highly responsive to anti-estrogen therapeutic strategies. However, despite widespread use of hormonal adjuvant therapy, a quarter of women with ER + disease will relapse [8]. In this situation, a determination regarding further hormonal therapy versus chemotherapy as the next step must be made. Patients whose disease is viscerally relatively 'low'volume, bone/soft tissue-predominant, and asymptomatic are reasonable candidates for upfront endocrine therapy. Figure 2 outlines the therapeutic approach to women with ER + , hormone-sensitive disease, and the evidence supporting these treatment strategies is outlined below and in Table 1. Of note, many of the earlier but pivotal studies included patients whose receptor status was unknown, thereby potentially underestimating the eff ects of endocrine blockade.

Tamoxifen, fulvestrant, and ovarian suppression
Tamoxifen emerged as a non-surgical alternative for the management of ER + MBC in the late 1970s. A non-steroidal selective estrogen receptor modulator (SERM) whose primary eff ect is to competitively inhibit the binding of estradiol to ERs, tamoxifen prevents the recep tor from binding to the estrogen-response element on DNA. However, it also induces elevated estradiol levels via a partial agonist eff ect [9] that can be suppressed to normal postmenopausal levels by gonadotropin-releasing hormone (GnRH) agonists. Studies comparing tamoxifen with oopherectomy among premeno pausal women with MBC found no signifi cant diff erence in overall response rate (RR), duration of response, time to progression (TTP), or survival, nor was there a signifi cant diff erence in outcomes when GnRH agonists were compared with oopherectomy [10,11].
Complete estrogen blockade in premenopausal women can be achieved by using combination therapy and is analogous to the principle of total androgen blockade in prostate cancer. Meta-analysis has confi rmed that the combination of GnRH agonists plus tamoxifen aff ords a superior progression-free survival (PFS) and overall survival (OS) compared with luteinizing hormone release hormone agonists alone in the treat ment of premenopausal women with ER/PR + MBC [12].
Th e current practice for premenopausal women with MBC previously unexposed to hormone blockade is to be treated in the fi rst-line setting with tamoxifen as initial endocrine therapy or with aromatase inhibitor (AI) therapy in combination with ovarian suppression (via oopherectomy, radiation, or a GnRH agonist). Ovarian radiation is a less optimal mode of ablation as the success rate and time to ablation vary compared with irreversible and immediate ablation aff orded by oopherectomy. An Eastern Cooperative Oncology Group study examining adjuvant estrogen blockade in premenopausal patients randomly assigned patients to tamoxifen monotherapy versus tamoxifen plus ovarian ablation via radiotherapy, oopherectomy, or GnRH agonists [13]. Th e trial was closed early for inadequate accrual; however, 75% of those undergoing radiotherapy achieved estradiol or follicle-stimulating hormone (FSH) levels consistent with those of ovarian ablation at 6 months after completing 20 Gy in 10 fractions. Further evidence supporting the need for ovarian suppression in addition to tamoxifen is lacking; data pertaining to premenopausal women in the adjuvant setting suggest that the combi na tion of goserelin and tamoxifen is not superior to tamoxifen alone [14]. Responses to surgical castration have been observed after tamoxifen failures, and oopherectomy should be considered if a premenopausal woman relapses after adjuvant or fi rst-line tamoxifen in the metastatic setting.
Fulvestrant (Faslodex; AstraZeneca, London, UK) is a synthetic ER antagonist that down regulates and degrades ERs by competitively binding them without tamoxifen's partial agonist eff ect [9]. Intramuscular injections of fulvestrant were compared with tamoxifen in a large randomized trial to ascertain whether the absence of partial agonist properties of fulvestrant conferred better outcomes among postmenopausal women with MBC. Despite the lack of fi rst-line superiority over tamoxifen, the NCCTG (North Central Cancer Treatment Group) N0032 and CONFIRM (Comparison of Faslodex in Recurrent or Metastatic Breast Cancer) trials demonstrated that fulvestrant has effi cacy as sequential endocrine therapy in postmenopausal women in the second-and even third-line setting [15,16]. Th e latter study also established the current standard dose of fulvestrant at 500 mg monthly given the superior effi cacy compared with 250 mg monthly [15]. Subsequently, the FIRST (Fulvestrant First-line Study Comparing Endocrine Treatments) trial, a phase II study that randomly assigned women who were endocrine therapynaïve to fulvestrant (500 mg monthly) versus anastrozole (1 mg daily), showed a comparable clinical benefi t rate (CBR) and a longer TTP for fulves trant, suggesting the potential for an alternate fi rst-line endocrine agent to AIs in postmenopausal women [17].

Aromatase inhibitors: exemestane, anastrozole, and letrozole
Estrogen production in postmenopausal women is derived from the peripheral aromatization of androgens. Inhi bition of aromatase is thereby a cornerstone of hormonal blockade in the management of postmenopausal breast cancer [18]. Th ese drugs cannot be used alone safely in premenopausal women without concomitant ovarian suppression or ablation since aromatase inhibition in the setting of functional ovaries will lead to ovarian hyperstimulation [19]. AIs currently in use include anastrozole (Arimidex; AstraZeneca), letrozole (Femara; Novartis, East Hanover, NJ, USA), and exemestane (Aromasin; Pfi zer Inc, New York, NY, USA). Analysis of two large randomized trials in which postmenopausal women who were endocrine therapy-naïve in the metastatic setting showed that anastrozole was at least equivalent to tamoxifen in the fi rst-line setting; unplanned subgroup analysis restricted to patients with known positive hormone receptors demonstrated a superior TTP for anastrozole [20]. Letrozole has also been directly compared with tamoxifen in the fi rst-line setting among women with MBC and similarly increased the TTP [21]. As such, anastrozole and letrozole, non-steroidal AIs, are fi rst-line endocrine options in postmenopausal MBC. Exemestane, unlike the non-steroidals in this class, is a steroidal AI that irreversibly inhibits aromatase. In women who have progressed on tamoxifen, exemestane showed prolonged TTP and OS compared with megestrol [22,23]. In addition to having a utility in the second-line setting, exemestane showed signifi cant early improvement in TTP compared with tamoxifen in the fi rst-line setting, although after longer follow-up, the two drugs were found to have comparable effi cacy [22]. Th ere is a paucity of data comparing AIs directly to each other in the metastatic setting; however, extrapolation from a small trial showed that exemestane and anastrozole had similar RRs among postmenopausal women who had MBC and who were tamoxifen-refractory [24].

Progestins: megestrol
Progestins, such as megestrol acetate (MA), are some of the oldest compounds to be used in the treatment of MBC, indirectly reducing serum estrogen levels by reducing androgen levels [9]. While use of these agents has dropped dramatically since the introduction of AIs and GNRH agonists, there are data demonstrating the effi cacy of these agents in the MBC setting. Although randomized trials comparing MA and tamoxifen show comparable RRs and TTP, ultimately tamoxifen remains preferable to MA because of the toxicity profi le. Analyses comparing AI and MA have shown that anastrozole confers a survival advantage over MA, and letrozole shows an improved RR and time to treatment failure [18]. After failure on fi rst-and second-line therapies, data suggest that the use of MA as a second-or third-line therapy is reasonable primarily for 'durable' disease stabilization but not with the goal of response [25].

Paradoxical estrogen sensitization: estradiol
Th e development of estrogen sensitization in breast cancer cells after long-term estrogen deprivation paradoxically enables treatment with low-dose estradiol that in some cases confers re-sensitization to subsequent retreatment with an AI. Women with ER/PR + AI-resistant metastatic disease were randomly assigned to 30 mg daily of estradiol or 6 mg daily to assess CBR in the low-dose versus higher-dose group [26]. AI resistance was defi ned as relapse within 2 years after adjuvant AI or prior treatment within the metastatic setting. Study participants who had been exposed to fulvestrant within the previous 12 months were excluded because of data showing in vitro antagonism of estrogen-induced apoptosis. Th ere was no signifi cant diff erence in the CBR between the two groups, and re-treatment with the last AI used in the responders showed clinical benefi t in three of the seven patients re-treated.

Hormone receptor-positive, endocrine-refractory metastatic breast cancer: mTOR inhibition
Th e development of hormone resistance in ER + but endocrine-refractory metastatic disease is postulated to involve signal transduction pathways, including mammalian target of rapamycin (mTOR). Results from a second-line phase II study randomly assigning patients with hormone-positive MBC to tamoxifen versus tamoxifen plus an mTOR inhibitor (everolimus) showed a signifi cant improvement in the CBR, median TTP, and OS as of a September 2011 update at the European Multidisciplinary Cancer Congress [27,28]. Th e PI3K/Akt/ mTOR pathway is constitutively activated in AI-resistant breast cancer. Results of the phase III randomized controlled trial BOLERO-2 (Breast Cancer Trials of Oral Everolimus-2), updated at the San Antonio Breast Cancer Symposium in December 2011, showed that postmenopausal women refractory to letrozole or anastrozole treated with a combination of everolimus and exemestane had an improved PFS of 10.6 months compared with 4.1 months in women treated with exemestane alone [7]. Th is combination has the potential to delay initiation of cytotoxic therapy in endocrine-refractory patients.
In summary, fi rst-line endocrine therapy is preferred for women whose hormone receptor-positive MBC is limited to bone or soft tissue or both and for those whose visceral volume of disease does not appear to be fastgrowing or pose imminent threat of organ compromise. After failure of fi rst-line endocrine therapy, sequential endocrine options are preferable to cytotoxic therapy provided that metastatic sites are still hormone receptorpositive. Premenopausal women who are endocrinenaïve should receive tamoxifen and, in the second-line setting, can undergo ovarian suppression via either surgical or chemical castration and then an AI. Postmenopausal women should be off ered an AI as fi rst-line treatment of their metastatic disease. After progression on an AI, subsequent therapy could consist of sequential endocrine options, including an alternative AI (that is, steroidal if the fi rst AI was non-steroidal), tamoxifen, or fulvestrant. Megestrol should be reserved for use after failure on fi rst-and second-line therapies. Estradiol can be considered if the volume of disease permits an attempt at re-sensitization to an AI. Ultimately, postmenopausal patients who progress after a non-steroidal AI may be treated with the combination of everolimus and exemestane provided that everolimus receives US Food and Drug Administration (FDA) approval for this indication.
In the clinical scenario of hormone-sensitive disease that is rapidly progressive and threatening organ function, cytotoxic therapy can be considered with the goal of resumption of an endocrine agent if visceral crisis has abated rather than empirically persisting with a series of cytotoxic therapies.

Treatment of metastatic breast cancer that is ER + / endocrine-refractory or triple-negative or that presents with visceral threat
Admittedly, using receptor status and sensitivity to guide management of therapy in MBC oversimplifi es the discrete molecular subtypes identifi ed through advances in genomic analysis. For example, the biologic behavior and drivers of an ER + luminal breast cancer that becomes hormone-insensitive are presumably distinct from those of triple-negative basal-like subtypes, as evidenced by diff erent patterns of relapse and response to treatment [29]. However, practically speaking, molecular subtyping is not available as a routine clinical test, nor were tumors prospectively subtyped in the clinical trials that led to FDA approval for these drugs in MBC. With this limitation in mind, Figure 2 outlines the therapeutic approach to women with ER + , hormone-refractory or 'triplenegative' MBC; the evidence supporting these treatment strategies is listed in Table 2 and discussed briefl y below. A guiding principle of treatment of metastatic disease is to respect the palliative goal of this therapy given the absence of data demonstrating superior survival benefi t with combination cytotoxics rather than sequential strategies. Sequential administra tion of single agents has been considered a viable and acceptable standard of care and this is due, in part, to Intergroup trial E1193, in which, despite increased RR and time to treatment failure (primary outcomes the trial was designed to detect) with combination paclitaxel and doxorubicin in metastatic disease, sequential doxorubicin followed by paclitaxel and vice versa showed similar effi cacy and no diff erence in survival benefi t [8]. Many patients will require multiple lines of therapy for advanced disease, and, as such, use of combination chemo therapy regimens rather than sequential use of single-agent cytotoxics should be limited to specifi c circumstances in which performance status permits it and rapid response is critical, as with impending organ failure. Table 2 and the following discus sion review RRs of single-agent cytotoxics and also expected responses to combination regimens that have a particular synergy. Cytotoxics that have FDA-approved indications in MBC and that have activity as single agents include anthracyclines, taxanes, non-taxane microtubule inhibitors, and antimetabolites.
Anthracycline single-agent cytotoxic therapy: doxorubicin, epirubicin, and pegylated liposomal doxorubicin Many patients will have been exposed to anthracyclines in the adjuvant setting; however, with the advent of docetaxel/cyclophosphamide as a standard adjuvant doublet, more patients may present with recurrent disease without having been exposed to these agents. Women with metastatic disease (receptor status not reported) exposed to alkylators in the adjuvant setting or to, at most, one line of therapy in the advanced setting or to both were randomly assigned to doxorubicin 75 mg/m 2 versus docetaxel 100 mg/m 2 every 3 weeks. Although docetaxel resulted in a higher objective RR in this pretreated population with visceral disease, there was no statistically signifi cant diff erence in median TTP or OS. Neutropenic fever, infection, cardiac toxicity, nausea, and vomiting were more likely with anthracycline therapy, whereas the primary toxicities caused by docetaxel consisted of diarrhea, neuropathy, fl uid retention, and skin and nail changes [30]. In a trial designed to establish the optimal dose of fi rst-line epirubicin in MBC, women who had mostly positive/unknown hormone receptor status and whose adjuvant regimens were nonanthracycline-based were randomly assigned to four dose levels of epirubicin, including 90 mg/m 2 , which is hematologically equivalent to the maximum tolerated dose of 75 mg/m 2 of doxo rubicin. Th is dose was found to aff ord the greatest TTP at the least toxicity and is further evidence that single-agent anthracyclines have effi cacy [31]. Pegylated liposomal doxorubicin (PLD) has also been examined in the hope that preferential accumulation in tumor tissue would limit cardiotoxicity. In a noninferiority trial designed to assess effi cacy and cardiac safety, women who could have received prior adjuvant anthracycline were randomly assigned to either PLD or doxorubicin. Non-inferiority was achieved; however, not surprisingly, signifi cantly more doxorubicin-treated patients met the protocol-defi ned criteria for cardiotoxicity [32].

Taxane single-agent cytotoxic therapy: paclitaxel and docetaxel
Single-agent taxanes are an eff ective option in metastatic patients, particularly in those who were treated with only anthracycline-based adjuvant therapy. Taxanes induce mitotic arrest by inhibiting depolymerization of the micro tubules. Although the mechanism of paclitaxel and docetaxel of binding to tubulin and cell cycle arrest through stabilization of microtubules is similar, preclinical studies have shown that docetaxel has greater affi nity, longer retention time, and higher intracellular concentration in target cells [33]. Side eff ect profi les are also diff erent as fl uid retention and fatigue are more charac teristic of docetaxel toxicity whereas hyper sensitivity and neurotoxicity are more common with paclitaxel. Th is diff erence is thought to be related to the solvents required for stabilization of these hydrophobic compounds. Several studies have examined optimal dosing regimens of taxanes. Weekly paclitaxel appears to be as eff ective as or more eff ective than every-21-day dosing [34,35]. Docetaxel administered every 3 weeks has better effi cacy compared with either weekly or every-3-week paclitaxel but at the expense of more toxicity [33,36]. Docetaxel on a weekly schedule still results in some fatigue, fl uid retention, and excess lacrimation but less myelosuppression and neuropathy [37]. Nab-paclitaxel appears to be more eff ective and convenient than paclitaxel and docetaxel and aff ords the benefi t of taxane therapy without the steroid premedication [38,39].

Non-taxane microtubule inhibitor single-agent cytotoxic therapy: vinorelbine, ixabepilone, and eribulin
Other microtubule inhibitors effi cacious in the treatment of metastatic disease in those exposed/resistant to anthracyclines and taxanes include vinorelbine, ixabepilone, and eribulin. Nearly a quarter of patients who progressed through anthracyclines and taxanes treated with weekly vinorelbine (dose modifi ed to 25 mg/m 2 because of hematologic toxicity and neurotoxicity) had an objective response [40]. Vinorelbine binds to tubulin, inhibiting tubulin polymerization, and this may explain why sensitivity to vinorelbine is retained among patients pretreated with taxanes as excess depolymerized tubulin has been noted in vitro [9]. Ixabepilone -an epothilone B analog that increases polymerization but that, unlike the taxanes, has the capacity to bind to multiple isomers of tubulin -has been evaluated in the setting of patients pretreated with anthracyclines, taxanes, and capecitabine as well as in fi rst-line metastatic treatment of patients treated with adjuvant anthracyclines. In the fi rst-line setting, women with MBC achieved an overall RR of 41.5% and a median survival of 22 months [41,42]. Modifi cations in the administration schedule of ixabepilone in a group of women who had not had prior taxane exposure did reduce neurotoxicity while maintaining RRs comparable to those of historical controls of docetaxel or paclitaxel in the fi rst-or second-line metastatic setting [43]. Women with taxane-resistant metastatic disease or those pretreated with taxanes and capecitabine had RRs ranging from 11% to 12% and a durable response of nearly 6 months [44,45]. In this heavily pretreated population with prior exposure to taxane therapy, half experienced reversible sensory neuropathy.
Eribulin is the latest non-taxane microtubule inhibitor with a mechanism distinct from that of taxanes, epothilones, and vinca alkaloids in that it aff ects centromere dynamics and sequesters tubulin into nonfunctional aggregates and, like vinorelbine, decreases polymerization of microtubules [46]. Phase II studies have shown effi cacy in populations pretreated with anthracyclines and taxane as well as capecitabine. Despite a median of four prior regimens, women still achieved RRs ranging from 9% to 14% and a PFS of approximately 2.6 months [46,47]. A phase III trial randomly assigning heavily pretreated patients to eribulin showed an improvement in OS of 13.1 months compared with 10.6 months in women treated according to physician's choice. Neutropenia (52%), fatigue (54%), and neuropathy (35%) were common toxicities [48].

Antimetabolite single-agent cytotoxic therapy: capecitabine and gemcitabine
Antimetabolite therapy should be considered in women with prior exposure to anthracycline and taxane therapy. Capecitabine is an orally administered precursor of 5-deoxy-5-fl uorouridine monotherapy that is prefer entially converted in tumor tissue through exploitation of high intratumoral concentrations of thymidine phosphorylase to 5-fl uorouracil [9]. A group of women who had received over three prior cytotoxic regimens, including prior anthracycline and taxane therapy, achieved an objective RR of 26% and a median survival of 12.2 months with capecitabine monotherapy, even though nearly half required dose reduction. Retrospective analysis suggested that dose reduction for palmar-plantar erythrodysesthesia, diarrhea, and nausea did not aff ect effi cacy [49]. Capecitabine monotherapy was also tested in the fi rstline setting against cyclophosphamide/methotrexate/fl uorouracil with comparable RRs, although palmar-plantar erythrodysesthesia induced by capecitabine required treatment interruptions and dose reductions in a third of patients [50]. Capecitabine at a lower dose of 1,000 mg/ m 2 daily for 14 days out of a 21-day cycle was compared with previously tested regimens of 1,250 mg/m 2 to assess safety in women at least 65 years old, half of whom had received prior systemic treatments. Th e lower dose aff orded similar rates of tumor response with better tolerability in the lower-dose group [51]. Gemcitabine has also been evaluated as single-agent therapy in multiple trials in both the fi rst-line and refractory/resistant setting in doses ranging from 800 to 1,200 mg/m 2 weekly for 3 weeks on a 28-day cycle with RRs as varied as 14.5% to 37% and OS of 21 months in the fi rst-line setting to RRs of 20% to 37.1% and OS of 11 months in a pretreated setting [52,53].

Combination cytotoxic therapy
Combination therapies generally increase RR and TTP but with a concomitant increase in toxicity. Moreover, a critical shortcoming of studies in this area is the use of study designs in which the combination is compared with one or the other of the agents alone. Th e lack of comparison between sequential use of both agents and the combination biases these studies in favor of the combination. Many cytotoxic combinations have been assessed in the metastatic setting; however, only a few have shown synergy in phase III studies to prolong OS over single-agent cytotoxics with manageable toxicities, and these regimens will be reviewed here.
Th e low myelotoxicity associated with capecitabine made it an attractive agent to consider in combination with other cytotoxics, and preclinical work showing tumor overexpression of thymidine phosphorylase by taxanes suggested that this was an opportunity for synergy. Patients pretreated with anthracycline (prior paclitaxel was permitted) were randomly assigned to capecitabine/docetaxel or docetaxel monotherapy, and the combination resulted in an increased RR, TTP, and OS, but the improvement in effi cacy was at the cost of more grade 3 adverse events (71% versus 49%) in the combination arm. Th e 1,250 mg/m 2 twice daily dose of capecitabine may have been too high to use in combination with docetaxel given evidence that 1,000 mg/m 2 twice daily of capecitabine monotherapy was equivalent to higher doses in women at least 65 years old. Treatment interruption was required in 34% of capecitabine cycles and 27% of docetaxel cycles compared with 20% in the single-agent arm [50]. Th is trial did not answer the question of whether sequential administration would have had equivalent benefi t with less toxicity.
Another study compared the combination of gemcitabine plus paclitaxel to gemcitabine alone in the fi rst-line treatment of metastatic disease. Median survival was 18.6 versus 15.8 months (P = 0.0489) with a longer TTP (6.14 versus 3.98 months; P = 0.0002) and a higher RR (41.4% versus 26.2%; P = 0.0002). However, the 22% improvement in OS and 43% improvement in TTP were at the expense of more neutropenia, fatigue, and neuropathy. Again, the trial did not answer the question of whether sequential single-agent therapy would have yielded equivalent results [54]. Th e study design also precluded comparison with a weekly paclitaxel schedule which appears preferential to a three-weekly schedule in the advanced setting [34,54,55].
A third combination regimen that has shown synergy is ixabepilone plus capecitabine in women previously treated with, but not necessarily resistant to, anthracycline and taxane therapy [56]. Although the combination arm had better PFS, there was no signifi cant diff erence in OS between the two arms. Notably, there was an imbalance between the two groups in performance status. After adjustment for performance status, OS was also improved in the combination arm. Nearly a quarter of those in the ixabepilone plus capecitabine arm experienced reversible grade 3 or 4 neuropathy.
Given the proposed defi ciency of DNA repair mechanisms in triple-negative and basal-like tumors, platinumbased chemotherapy combinations have been presented as a strategy to treat these subtypes of MBC. Although phase II studies of carboplatin-or cisplatin-based combination regimens have demon strated overall RRs ranging from 29% to 41% in triple-negative MBC, these responses are often at the expense of signifi cant hematologic and non-hematologic side eff ects, including peripheral neuropathy, nephrotoxicity, and nausea [57][58][59]. In light of the high rates of grade 3/4 toxicities for a palliative regimen and absence of pros pective phase III data showing improvement in PFS and OS, use of combination platinum-based therapy in triple-negative MBC warrants further study [60].
In summary, women whose MBC requires cytotoxic therapy have multiple alternatives. Monotherapy is prefer able to minimize side eff ects given the paucity of data comparing combination regimens to sequential use of single agents. Presuming adequate performance status, women with prior exposure to anthracyclines only should receive paclitaxel, albumin-bound paclitaxel, or docetaxel as fi rst-line treatment for their triple-negative or endocrine-refractory metastatic disease. Women who have progressed through taxane therapy can be treated with alternative microtubule inhibitors such as vinorelbine or eribulin if they do not have prohibitive residual neuropathy. A reasonable alternative is to treat these women with either capecitabine or gemcitabine. Combina tion cytotoxic regimens should be reserved for women who have good performance status and whose organ function is threatened by rapidly progressive disease.

Bevacizumab
Th e addition of bevacizumab to cytotoxic therapy for the fi rst-line treatment of Her2-negative MBC has recently undergone considerable scrutiny. In 2008, the FDA granted accelerated approval for its use in combination with chemotherapy based on a 5.5-month increase in PFS achieved in E2100, which compared paclitaxel plus bevacizu mab with paclitaxel alone [61]. Subsequent trials, including AVADO (Avastin and Docetaxel ), RIBBON (Regimens in Bevacizumab for Breast Oncology ), and TRIO-10 (Translational Research In Oncology), which evaluated the addition of bevacizumab to taxanes, anthracyclines, and capecitabine, showed notably smaller, albeit statistically signifi cant, improvements in PFS [62][63][64][65]. As with E2100, these trials showed no improvement in OS, and, in some instances, OS appeared to favor the chemotherapy-alone arms. Although some women appear to benefi t from bevacizumab, there remains no clear marker to predict activity and bevacizumabcontaining arms did have more adverse events that were serious. As a result of these analyses, the National Institute for Health and Clinical Excellence in the UK concluded in February 2011 that the addition of bevacizu mab was not a cost-eff ective use of resources and the FDA decided in June 2011 to revoke the indication for the use of bevacizumab in MBC [66,67]. To date, compendium guidelines put forth by the National Comprehensive Cancer Network still support consideration of weekly paclitaxel and bevacizumab, and the European Medicines Agency endorses the addition of bevacizumab to paclitaxel or capecitabine as a viable option in MBC.

Future directions: molecular subtypes and targeted therapy
While ER, PR, and Her2 status primarily inform the selection of therapy for MBC, recent advances in genomic analysis have provided insight into metastatic behavior of breast cancers within specifi c biologic subtypes. In addition to the conventional prognostic factors of size and lymph node involvement, analysis of archival specimens in women by breast cancer subtypessuch as luminal A, luminal B, luminal/Her2-enriched, non-luminal/Her2-enriched, basal-like, and triplenegative tumors -appears to show diff erent patterns of relapse and response to treatment [29]. ER − tumors (characteristic of non-luminal/Her2-enriched, basal-like, or triple-negative subtypes) are associated with early relapse and a higher proportion of metastatic disease involving the central nervous system, whereas ER + tumors (characteristic of luminal A, luminal B, or luminal/Her2-enriched subtypes) carry a risk of late relapse with a predilection for bone. Her2-enriched tumors (characteristic of luminal/Her2 or non-luminal/ Her2-enriched subtypes) demonstrate a high relapse rate in the brain, liver, and lung. Triple-negative basal-like tumors demonstrate a high and early relapse rate, with a greater incidence of brain, lung, and nodal metastases; triple-negative non-basal like subtypes also demonstrate a higher rate of visceral involvement that includes a greater proportion of liver metastases [29]. Although molecular subtype analysis is not yet a standard component of pathologic evaluation, knowledge of these subtypes in the future may add to the evaluation of women with MBC, aff ording both prognostic and predictive tools.
Molecular profi ling will ideally enable analysis within and across subtypes to isolate therapeutic targets as diff erent tumor subtypes appear to share some mutational hotspots. New agents targeting critical pathways in metastatic disease are currently in late-stage development (Table 3), and combinations of these agents and existing therapies will undoubtedly be necessary to better control systemic disease.
Th e development of endocrine-refractory, ER + metastatic disease appears to involve cell signaling pathways, including insulin-like growth factor receptor-I (IGFR-I) and mTOR. Although early results from IGFR-I inhibitors in overcoming resistance to AIs have been disappointing, the results from BOLERO-2 demonstrating the potential for use of mTOR inhibition to overcome AI resistance appear to be a promising alternative to cytotoxic therapy in these patients.
Proteins involved in DNA repair, such as poly (ADPribose) polymerase (PARP), are a therapeutic target in both BRCA mutation carriers and non-BRCA mutant triple-negative tumors. In basal-like subtype and sporadic triple-negative patients, intrinsic hypermethylation of the BRCA gene in combination with PARP inhibition may aff ord the synthetic lethality necessary to make these tumors more susceptible to cell death from chemotherapy [53]. Phase II data initially demonstrated that patients with triple-negative MBC had an improvement in CBR and OS when treated with PARP inhibitor iniparib when combined with carboplatin and gemcitabine; however, results of the phase III trial presented at the 2011 ASCO meeting did not result in a signifi cant increase in OS and PFS [68,69]. Although phase I and II studies testing olaparib showed response in BRCA1/2 mutation carriers with MBC, current trials have shifted the clinical focus of this drug toward ovarian carcinoma [70]. Velaparib, for which phase II results of a combination regimen with temozolomide were presented at the 2010 ASCO meeting, also showed lower-than-expected RRs [71]. Unfortunately, the initial promise of PARP inhibitors in triple-negative patients with MBC has yet to be realized.
Other potential targets that appear specifi c to basallike and triple-negative tumors include hedgehog ligands and tyrosine phosphatases. Overexpression of hedgehog ligands, thought to mediate tumor-stromal interactions, in basal-like tumors is associated with poor prognosis, and blockade of this ligand may aff ord another therapeutic target. Tyrosine phosphatases, such as PTPN12 (tyrosine-protein phosphatase non-receptor type 12), normally inhibit tyrosine kinases such as epidermal growth factor receptor (EGFR) and Her2 and may act as tumor suppressors. Th eir expression is frequently lost or inactivated in triple-negative tumors, and, as such, these subtypes may be more sensitive to inhibitors of tyrosine kinase inhibitors. However, as yet, phase III trials adding agents like sunitinib to standard cytotoxics like docetaxel have not demonstrated improved outcomes compared with cytotoxic monotherapy [72].
Preclinical work examining the role of proto-oncogene c-Met, also known as hepatocyte growth factor receptor, in the pathogenesis of basaloid tumors and trastuzumabresistant, Her2-positive tumors points to another potential opportunity for targeted therapy [9,19,73]. Oral small-molecule inhibitors of c-Met are currently in phase I trials both as monotherapy and in combination with gemcitabine and sorafenib [74][75][76].

Conclusions
Despite the development of numerous new agents over the past two decades and the rare durable remission, MBC remains an incurable disease. While the treatment of women with MBC will become even more complex as novel therapies emerge alongside of clinical decisionmaking tools that allow personalization of therapies according to molecular and genomic subtype, one basic principle ultimately will remain unchanged: do no harm. Th e current goal of care in metastatic disease is to palliate. Any therapeutic approach that seeks to harness the potential of a given drug to improve upon existing RRs and survival must be balanced against toxicities. Everolimus (Novartis, East Hanover, NJ, USA) Binds to FKBP-12 to generate complex that inhibits activation of mammalian target of rapamycin (mTOR), a regulatory kinase, resulting in inhibition of T lymphocyte activation and proliferation associated with antigen and cytokine stimulation and inhibition of antibody production. Inhibiting the mTOR pathway could overcome endocrine resistance mediated by ligandindependent receptor activation Phase III Approved for renal transplant immunosuppressive therapy; application for breast cancer indication yet to be submitted.