Breast cancer is the most common female cancer in Thailand [1] and consisted of many different subtypes such as hormone receptor (HR) positive, amplified-human epidermal growth factor receptor type 2 (HER-2), or triple negative breast cancer.(2) Over two-thirds of breast cancer patients are HR positive disease [3]. Metastatic breast cancer (MBC) is so far incurable. The goal of treatment at this stage is to control tumor growth, improve quality of life and prolong survival [4]. The treatment strategies of HR positive and HER-2 non-amplified MBC included endocrine and chemotherapy [2,5]. Patient with asymptomatic, mildly symptomatic or non-visceral crisis may be treated upfront by endocrine therapy which carries less side effects and provides better quality of life compared to chemotherapy-based therapy [6-7]. Multiple classes of endocrine therapy agents are available, included selective estrogen receptor modulator (SERM) such as tamoxifen, selective estrogen receptor down regulator (SERD) such as fulvestrant, non-steroidal aromatase inhibitor (AI) (anastrozole and letrozole) and steroidal AI (exemestane) [2]. In postmenopausal women, AI are more effective than tamoxifen [8-11], while non-steroidal AI (NSAI) are equally effective to steroidal AI [12-13]. More recently, CDK4/6 inhibitors have emerged as a highly effective treatment option in combination with the aforementioned agents [14-19]. Sequential use of these agents provides meaningful disease control period before chemotherapy initiation [20-23].

Everolimus is a sirolimus derivative that inhibits mTOR through allosteric binding to mTOR complex 1 [24]. Activation of phosphatidylinositol-3-kinase (PI3K)-protein kinase B (AKT)-mammalian Target of Rapamycin (mTOR) pathways has been proposed as one mechanism of endocrine resistance [25-28], in which everolimus has been shown to reverse such occurrence. The drug has been approved for advance ER positive, HER2 negative breast cancer that has progressed on NSAI in several countries worldwide including Thailand since 2013. The approval was based on the positive results from 2 randomized control trials, a phase 2 TAMRAD study

[29] and phase 3 BOLERO-2 trial [30-33]. Both studies showed a remarkable improvement in progression free survival (PFS) with HR of 0.54 and 0.45, respectively. However, upon longer follow-up, a survival benefit could not be demonstrated so far [32]. In addition, in a more recent phase 2 trial, BOLERO-6 study [34], the effectiveness of this combination compared to capecitabine, a commonly used single agent chemotherapy in MBC remained inconclusive.

Due to CDK4/6 inhibitors is a novel and expensive drug in Thailand which only few people who can access it. And CDK4/6 inhibitor has just been launched in Thailand since middle year of 2018 while PI3K inhibitors is likely to be launched in late 2020, therefore data of CDK4/6 inhibitor including PI3K inhibitors in a real-world practice especially low to middle income regions like in Thailand is very limited. Compare to CDK4/6 inhibitors and PI3K inhibitors, everolimus is more widely accessible in Thailand.

Due to the high cost of everolimus in Thailand together with its toxicity, notwithstanding the lack of survival advantage, called for a cautious use of the agent. In spite of the fact that the population in BOLERO-2 trial were not heavily pretreated, in real life practice in Thailand, this was not a common practice pattern and many patients had received several lines of systemic therapy before being treated with everolimus-exemestane combination in later lines. There has been limited data on its efficacy and optimal timing in routine clinical practice in Thai patients. So, this study was conducted to evaluate the efficacy of combination of everolimus and exemestane in a broader population i.e. in any line of treatment compared with everolimus-free regimen using survival as a primary endpoint in HR positive, HER-2 negative MBC that had progressed on previous NSAI in a single academic center.

We described a retrospective cohort study of patients with advanced ER positive breast cancer after failure from NSAI whose subsequent therapy contained or devoided of everolimus-exemestane in a real-life practice. As of this study, CDK4 / 6 inhibitors and PI3K inhibitors were not included due to a financial incompatibility and an inaccessibility of these drugs in Thailand. Patients in both comparison groups were well-balanced in baseline characteristics including prior therapy before NSAI. Our study explored the use of EE in a much broader population than in the pivotal BOLERO-2 study, which is much more representative of the real-world situation. The result showed that the use of everolimus-exemestane combination, although exerted some therapeutic benefit, did not translate to overall survival when adjusted for an imbalance in subsequent therapy. The more important factor for survival of these patients in our study was the ability to receive as many lines of treatment as possible. This finding, in fact, is in line with the final analysis of survival in BOLERO-2.

In this study, we chose overall survival as a primary endpoint as it is a more solid outcome than progression-free survival in retrospective database. To our knowledge, it is the study with the second longest follow-up time next to Italian cohort [35]. The median follow-up time was 51 months compared to 29 months in BOLERO-2 and 5 to 67 months in other phase IIIb expanded studies [32, 35-39] Hence, we are confident that the result represented a reasonably mature outcome. In addition, none of those expanded access reports and other real-world setting retrospective data have focused on overall survival; they mainly explored the response and safety aspects of EE.

Patients in our study, in some aspects, were different from BOLERO-2. They carried more visceral metastasis (79% vs 56%) and more liver metastasis (40% vs 33%). Despite high numbers of visceral metastasis, 58-67% of our patients received NSAI as their first line treatment for MBC, in accordance with the current recommendation of endocrine therapy in non-visceral crisis population. In BOLERO-2, the protocol had limited the number of prior chemotherapies in advanced disease to < 1. Therefore, in BOLERO-2, only 26% of patients had received 1 regimen of chemotherapy for metastasis, while in our EE cohort, 28% (15 patients) and 38% (20 patients) received one and > 2 lines of chemotherapy in metastatic setting before receiving EE, respectively.

The optimal timing of EE in the treatment sequence also remained inconclusive. In BOLERO-2, 74% received EE immediately after NSAI and hence the recommendation to consider treatment earlier in the course of their disease. However, in our study, only 27% received EE as an immediate subsequent therapy after NSAI and 50% of our patients received EE as their 4^th line of treatment. But even with more disease burden and late line use of EE, OS of our cohort compared well to that in BOLERO-2 (BOLERO-2: 31 months (EE) and 27 months (placebo), current study: 33 months (EE) and 25 months (NE)). When considering only 32 patients who received < 1 line of chemotherapy similar to inclusion criteria of BOLERO-2, OS was 28 months. In BOLERO-6 trial, patients who received everolimus after NSAI failure, OS was only 23 months compared to 25.6 months with capecitabine alone [34]. We found that patients who received EE in later line after NSAI refractory had longer survival (38 months) compared to earlier use although time on treatment was shorter. Because survival in this study was calculated from time of NSAI failure, it is plausible that the patients who received late-line EE were already pre-selected (able to have received several lines of systemic treatment before EE). Other large post-marketing observational studies of everolimus, most of which were also in more heavily pretreated patients similar to ours, could not confirm the adverse effect of prior chemotherapy on outcomes of patients receiving everolimus [32, 36-39]. Moreover, they also demonstrated comparable PFS to BOLERO-2. These data, including ours, thus suggested that EE could be considered at any line of treatment in ER+, HER2 – MBC, with preserved clinical activity.

As stated earlier, the initial unadjusted overall survival was in favor of EE treatment, which could be a result of differences in post-progression therapy. None of the patients in NE group received subsequent everolimus, mainly due to re-imbursement issue. On the contrary, we noted that more patients in EE group also significantly received eribulin compared to NE group. Eribulin has been shown in EMBRACE trial [40] to improve survival compared with physician’s treatment choice in patients who had been exposed to multiple systemic therapy. In addition to eribulin use, patients in EE did receive more total lines of systemic treatment than in control arm (5.2 vs 3.6 lines, p < 0.05). When these factors were included into Cox-regression multivariate analysis, numbers of line of treatment was confirmed to be a strong parameter for survival benefit whereas the effect of EE and eribulin use were no longer seen. This finding thus implied that access to multiple treatment lines in MBC is vital for good outcome and everolimus-combination was merely a surrogate marker of access to more sequential treatment, at least in our population with limited healthcare resources. Everolimus/exemestane including CDK4/6 inhibitors and PI3K inhibitors were not included in Thailand’s basic cancer protocol of universal coverage health care scheme. Therefore, this finding may have an impact on the policy change to allow access to more lines of therapy that is less costly than EE as currently only 3 lines of chemotherapy are covered for these patients.

Although we have highlighted above some of the interesting observations, this study did have limitations. As might be expected based on a retrospective nature of the non-randomized trial, selection bias was likely to exist. Patients in no-everolimus arm could have been pre-selected not to receive everolimus-exemestane if their disease were rapidly progressing and might result in poorer survival in that arm and thus over-estimated the benefit of everolimus-exemestane. To this aspect, the effect was partially adjusted by Cox-regression analysis. Secondly, our study, compared to other real-world data, was relatively small but yet, with mature data on survival. Thirdly, caution should be noted on PFS and response rate in this study as they were based on local investigator radiographic assessments, which again, could also have been biased. And lastly, our study lacked the information on side effects, dose modification of everolimus and patients’ quality of life.

With these limitations in mind, however, we felt that our data provided some valuable perspective for practicing oncologists. In summary, our study based on routine clinical practice, revealed that patients with HR +ve, HER-2 –ve advanced breast cancer that had progressed on NSAI, the sequential use of multiple treatment options for metastatic breast cancer led to increased survival. Everolimus combined with exemestane could be added into the armamentarium of such treatment with preserved clinical activity in heavily pretreated patients.

The authors would like to thank Ramathibodi Cancer Registry Unit of Ramathibodi Comprehensive Cancer Center for the support of clinical data.

Division IT National Cancer Institute T HOSPITAL BASED CANCER REGISTRY 2015. Pornsup Printing Co., LTD., Bangkok, THAILAND2015. 72 p 1117 1157 Morrow M Burstein HJ Harris JR 10th ed2015 Malignant Tumors of the Breast. In: DeVita VT, Lawrence TS, Rosenberg SA, editors. Cancer Principles & Practice of Oncology 688 8 694 26 2012 Lim E Metzger-Filho O Winer EP The natural history of hormone receptor-positive breast cancer. Oncology (Williston Park) 6 12 514-520 8 2003 10.1634/theoncologist.8-6-514 Chung Cathie T. Carlson Robert W. The Oncologist Goals and Objectives in the Management of Metastatic Breast Cancer 6 11 617-632 9 2004 10.1634/theoncologist.9-6-617 Bernard‐Marty Chantal Cardoso Fatima Piccart Martine J. The Oncologist Facts and Controversies in Systemic Treatment of Metastatic Breast Cancer 01 25 09 3069-3103 34 2016 10.1200/jco.2016.67.1487 Rugo Hope S. Rumble R. Bryan Macrae Erin Barton Debra L. Connolly Hannah Klein Dickler Maura N. Fallowfield Lesley Fowble Barbara Ingle James N. Jahanzeb Mohammad Johnston Stephen R.D. Korde Larissa A. Khatcheressian James L. Mehta Rita S. Muss Hyman B. Burstein Harold J. Journal of Clinical Oncology Endocrine Therapy for Hormone Receptor–Positive Metastatic Breast Cancer: American Society of Clinical Oncology Guideline 4 144 7 2017 10.4103/ajm.ajm_20_17 Salkeni MohamadAdham Hall SamanthaJune Avicenna Journal of Medicine Metastatic breast cancer: Endocrine therapy landscape reshaped 15 22 11 3758-3767 18 2000 10.1200/jco.2000.18.22.3758 Nabholtz J.M. Buzdar A. Pollak M. Harwin W. Burton G. Mangalik A. Steinberg M. Webster A. von Euler M. Journal of Clinical Oncology Anastrozole Is Superior to Tamoxifen as First-Line Therapy for Advanced Breast Cancer in Postmenopausal Women: Results of a North American Multicenter Randomized Trial 15 22 11 3748-3757 18 2000 10.1200/jco.2000.18.22.3748 Bonneterre J. Thürlimann B. Robertson J.F. R. Krzakowski M. Mauriac L. Koralewski P. Vergote I. Webster A. Steinberg M. von Euler M. Journal of Clinical Oncology Anastrozole Versus Tamoxifen as First-Line Therapy for Advanced Breast Cancer in 668 Postmenopausal Women: Results of the Tamoxifen or Arimidex Randomized Group Efficacy and Tolerability Study 01 11 06 2101-2109 21 2003 10.1200/jco.2003.04.194 Mouridsen Henning Gershanovich Mikhail Sun Yan Pérez-Carrión Ramón Boni Corrado Monnier Alain Apffelstaedt Justus Smith Robert Sleeboom Harm P. Jaenicke Fritz Pluzanska Anna Dank Magdolna Becquart Dominique Bapsy Poonamalle P. Salminen Eeva Snyder Ray Chaudri-Ross Hilary Lang Raquel Wyld Peter Bhatnagar Ajay Journal of Clinical Oncology Phase III Study of Letrozole Versus Tamoxifen as First-Line Therapy of Advanced Breast Cancer in Postmenopausal Women: Analysis of Survival and Update of Efficacy From the International Letrozole Breast Cancer Group 20 30 10 4883-4890 26 2008 10.1200/jco.2007.14.4659 Paridaens Robert J. Dirix Luc Y. Beex Louk V. Nooij Marianne Cameron David A. Cufer Tanja Piccart Martine J. Bogaerts Jan Therasse Patrick Journal of Clinical Oncology Phase III Study Comparing Exemestane With Tamoxifen As First-Line Hormonal Treatment of Metastatic Breast Cancer in Postmenopausal Women: The European Organisation for Research and Treatment of Cancer Breast Cancer Cooperative Group 29 1 06 241-247 118 2011 10.1002/cncr.26299 Llombart-Cussac Antonio Ruiz Amparo Antón Antonio Barnadas Agustí Antolín Silvia Alés-Martínez José E. Álvarez Isabel Andrés Raquel García Saenz José A. Lao Juan Carrasco Eva Cámara Carmen Casas Isabel Martín Miguel Cancer Exemestane versus anastrozole as front-line endocrine therapy in postmenopausal patients with hormone receptor-positive, advanced breast cancer 30 2 05 441-451 139 2013 10.1007/s10549-013-2573-3 Iwata Hiroji Masuda Norikazu Ohno Shinji Rai Yoshiaki Sato Yasuyuki Ohsumi Shozo Hashigaki Satoshi Nishizawa Yoshinori Hiraoka Masahiro Morimoto Tadaoki Sasano Hironobu Saeki Toshiaki Noguchi Shinzaburo Breast Cancer Research and Treatment A randomized, double-blind, controlled study of exemestane versus anastrozole for the first-line treatment of postmenopausal Japanese women with hormone-receptor-positive advanced breast cancer 17 20 11 1925-1936 375 2016 10.1056/nejmoa1607303 Finn Richard S. Martin Miguel Rugo Hope S. Jones Stephen Im Seock-Ah Gelmon Karen Harbeck Nadia Lipatov Oleg N. Walshe Janice M. Moulder Stacy Gauthier Eric Lu Dongrui R. Randolph Sophia Diéras Véronique Slamon Dennis J. New England Journal of Medicine Palbociclib and Letrozole in Advanced Breast Cancer 15 20 11 1926-1936 379 2018 10.1056/nejmoa1810527 Turner Nicholas C. Slamon Dennis J. Ro Jungsil Bondarenko Igor Im Seock-Ah Masuda Norikazu Colleoni Marco DeMichele Angela Loi Sherene Verma Sunil Iwata Hiroji Harbeck Nadia Loibl Sibylle André Fabrice Puyana Theall Kathy Huang Xin Giorgetti Carla Huang Bartlett Cynthia Cristofanilli Massimo New England Journal of Medicine Overall Survival with Palbociclib and Fulvestrant in Advanced Breast Cancer 03 18 11 1738-1748 375 2016 10.1056/nejmoa1609709 Hortobagyi Gabriel N. Stemmer Salomon M. Burris Howard A. Yap Yoon-Sim Sonke Gabe S. Paluch-Shimon Shani Campone Mario Blackwell Kimberly L. André Fabrice Winer Eric P. Janni Wolfgang Verma Sunil Conte Pierfranco Arteaga Carlos L. Cameron David A. Petrakova Katarina Hart Lowell L. Villanueva Cristian Chan Arlene Jakobsen Erik Nusch Arnd Burdaeva Olga Grischke Eva-Maria Alba Emilio Wist Erik Marschner Norbert Favret Anne M. Yardley Denise Bachelot Thomas Tseng Ling-Ming Blau Sibel Xuan Fengjuan Souami Farida Miller Michelle Germa Caroline Hirawat Samit O’Shaughnessy Joyce New England Journal of Medicine Ribociclib as First-Line Therapy for HR-Positive, Advanced Breast Cancer 20 24 08 2465-2472 36 2018 10.1200/jco.2018.78.9909 Slamon Dennis J. Neven Patrick Chia Stephen Fasching Peter A. De Laurentiis Michelino Im Seock-Ah Petrakova Katarina Bianchi Giulia Val Esteva Francisco J. Martín Miguel Nusch Arnd Sonke Gabe S. De la Cruz-Merino Luis Beck J. Thaddeus Pivot Xavier Vidam Gena Wang Yingbo Rodriguez Lorenc Karen Miller Michelle Taran Tetiana Jerusalem Guy Journal of Clinical Oncology Phase III Randomized Study of Ribociclib and Fulvestrant in Hormone Receptor–Positive, Human Epidermal Growth Factor Receptor 2–Negative Advanced Breast Cancer: MONALEESA-3 10 32 11 3638-3646 35 2017 10.1200/jco.2017.75.6155 Goetz Matthew P. Toi Masakazu Campone Mario Sohn Joohyuk Paluch-Shimon Shani Huober Jens Park In Hae Trédan Olivier Chen Shin-Cheh Manso Luis Freedman Orit C. Garnica Jaliffe Georgina Forrester Tammy Frenzel Martin Barriga Susana Smith Ian C. Bourayou Nawel Di Leo Angelo Journal of Clinical Oncology MONARCH 3: Abemaciclib As Initial Therapy for Advanced Breast Cancer 01 25 09 2875-2884 35 2017 10.1200/jco.2017.73.7585 Sledge George W. Toi Masakazu Neven Patrick Sohn Joohyuk Inoue Kenichi Pivot Xavier Burdaeva Olga Okera Meena Masuda Norikazu Kaufman Peter A. Koh Han Grischke Eva-Maria Frenzel Martin Lin Yong Barriga Susana Smith Ian C. Bourayou Nawel Llombart-Cussac Antonio Journal of Clinical Oncology MONARCH 2: Abemaciclib in Combination With Fulvestrant in Women With HR+/HER2− Advanced Breast Cancer Who Had Progressed While Receiving Endocrine Therapy 1142 6 1152 83 1998 Buzdar AU Jonat W Howell A Jones SE Blomqvist CP Vogel CL et al Arimidex Study Group. Cancer Anastrozole versus megestrol acetate in the treatment of postmenopausal women with advanced breast carcinoma: results of a survival update based on a combined analysis of data from two mature phase III trials 2 02 453-461 16 1998 10.1200/jco.1998.16.2.453 Dombernowsky P Smith I Falkson G Leonard R Panasci L Bellmunt J Bezwoda W Gardin G Gudgeon A Morgan M Fornasiero A Hoffmann W Michel J Hatschek T Tjabbes T Chaudri H A Hornberger U Trunet P F Journal of Clinical Oncology Letrozole, a new oral aromatase inhibitor for advanced breast cancer: double-blind randomized trial showing a dose effect and improved efficacy and tolerability compared with megestrol acetate. 20 30 10 4594-4600 28 2010 10.1200/jco.2010.28.8415 Di Leo Angelo Jerusalem Guy Petruzelka Lubos Torres Roberto Bondarenko Igor N. Khasanov Rustem Verhoeven Didier Pedrini José L. Smirnova Iya Lichinitser Mikhail R. Pendergrass Kelly Garnett Sally Lindemann Justin P.O. Sapunar Francisco Martin Miguel Journal of Clinical Oncology Results of the CONFIRM Phase III Trial Comparing Fulvestrant 250 mg With Fulvestrant 500 mg in Postmenopausal Women With Estrogen Receptor–Positive Advanced Breast Cancer 01 10 04 1664-1670 26 2008 10.1200/jco.2007.13.5822 Chia Stephen Gradishar William Mauriac Louis Bines Jose Amant Frederic Federico Miriam Fein Luis Romieu Gilles Buzdar Aman Robertson John F.R. Brufsky Adam Possinger Kurt Rennie Pamela Sapunar Francisco Lowe Elizabeth Piccart Martine Journal of Clinical Oncology Double-Blind, Randomized Placebo Controlled Trial of Fulvestrant Compared With Exemestane After Prior Nonsteroidal Aromatase Inhibitor Therapy in Postmenopausal Women With Hormone Receptor–Positive, Advanced Breast Cancer: Results From EFECT 2 04 169-176 22 2010 10.1016/j.ceb.2009.10.007 Efeyan Alejo Sabatini David M Current Opinion in Cell Biology mTOR and cancer: many loops in one pathway 01 3 02 1061s-1068s 12 2006 10.1158/1078-0432.ccr-05-2125 Johnston Stephen R.D. Clinical Cancer Research Clinical Efforts to Combine Endocrine Agents with Targeted Therapies against Epidermal Growth Factor Receptor/Human Epidermal Growth Factor Receptor 2 and Mammalian Target of Rapamycin in Breast Cancer 06 S17-S24 38 2011 10.1053/j.seminoncol.2011.04.002 Burstein Harold J. Seminars in Oncology Novel Agents and Future Directions for Refractory Breast Cancer 23 7418 09 61-70 490 2012 10.1038/nature11412 Nature Comprehensive molecular portraits of human breast tumours 7403 06 353-360 486 2012 10.1038/nature11143 Ellis Matthew J. Ding Li Shen Dong Luo Jingqin Suman Vera J. Wallis John W. et al Nature Whole-genome analysis informs breast cancer response to aromatase inhibition 01 22 08 2718-2724 30 2012 10.1200/jco.2011.39.0708 Bachelot Thomas Bourgier Céline Cropet Claire Ray-Coquard Isabelle Ferrero Jean-Marc Freyer Gilles Abadie-Lacourtoisie Sophie Eymard Jean-Christophe Debled Marc Spaëth Dominique Legouffe Eric Allouache Djelila El Kouri Claude Pujade-Lauraine Eric Journal of Clinical Oncology Randomized Phase II Trial of Everolimus in Combination With Tamoxifen in Patients With Hormone Receptor–Positive, Human Epidermal Growth Factor Receptor 2–Negative Metastatic Breast Cancer With Prior Exposure to Aromatase Inhibitors: A GINECO Study 09 6 02 520-529 366 2012 10.1056/nejmoa1109653 Baselga José Campone Mario Piccart Martine Burris Howard A. Rugo Hope S. Sahmoud Tarek Noguchi Shinzaburo Gnant Michael Pritchard Kathleen I. Lebrun Fabienne Beck J. Thaddeus Ito Yoshinori Yardley Denise Deleu Ines Perez Alejandra Bachelot Thomas Vittori Luc Xu Zhiying Mukhopadhyay Pabak Lebwohl David Hortobagyi Gabriel N. New England Journal of Medicine Everolimus in Postmenopausal Hormone-Receptor–Positive Advanced Breast Cancer 10 10 870-884 30 2013 10.1007/s12325-013-0060-1 Yardley Denise A. Noguchi Shinzaburo Pritchard Kathleen I. Burris Howard A. Baselga José Gnant Michael Hortobagyi Gabriel N. Campone Mario Pistilli Barbara Piccart Martine Melichar Bohuslav Petrakova Katarina Arena Francis P. Erdkamp Frans Harb Wael A. Feng Wentao Cahana Ayelet Taran Tetiana Lebwohl David Rugo Hope S. Advances in Therapy Everolimus Plus Exemestane in Postmenopausal Patients with HR+ Breast Cancer: BOLERO-2 Final Progression-Free Survival Analysis 12 12 2357-2362 25 2014 10.1093/annonc/mdu456 Piccart M. Hortobagyi G.N. Campone M. Pritchard K.I. Lebrun F. Ito Y. et al Annals of Oncology Everolimus plus exemestane for hormone-receptor-positive, human epidermal growth factor receptor-2-negative advanced breast cancer: overall survival results from BOLERO-2 13 6 02 703-714 21 2013 10.1007/s12282-013-0444-8 Noguchi Shinzaburo Masuda Norikazu Iwata Hiroji Mukai Hirofumi Horiguchi Jun Puttawibul Puttisak Srimuninnimit Vichien Tokuda Yutaka Kuroi Katsumasa Iwase Hirotaka Inaji Hideo Ohsumi Shozo Noh Woo-Chul Nakayama Takahiro Ohno Shinji Rai Yoshiaki Park Byeong-Woo Panneerselvam Ashok El-Hashimy Mona Taran Tetiana Sahmoud Tarek Ito Yoshinori Breast Cancer Efficacy of everolimus with exemestane versus exemestane alone in Asian patients with HER2-negative, hormone-receptor-positive breast cancer in BOLERO-2 01 10 10 1367 4 2018 10.1001/jamaoncol.2018.2262 Jerusalem Guy de Boer Richard H. Hurvitz Sara Yardley Denise A. Kovalenko Elena Ejlertsen Bent et al JAMA Oncology Everolimus Plus Exemestane vs Everolimus or Capecitabine Monotherapy for Estrogen Receptor–Positive, HER2-Negative Advanced Breast Cancer 16 07 2018 10.3892/mco.2018.1672 Riccardi Ferdinando Colantuoni Giuseppe Diana Anna Mocerino Carmela Carten� Giacomo Lauria Rossella Febbraro Antonio Nuzzo Francesco Addeo Raffaele Marano Ombretta Incoronato Pasquale De Placido Sabino Ciardiello Fortunato Orditura Michele Molecular and Clinical Oncology Exemestane and Everolimus combination treatment of hormone receptor positive, HER2 negative metastatic breast cancer: A retrospective study of 9 cancer centers in the Campania Region (Southern Italy) focused on activity, efficacy and safety 07 6 11 753-760 20 2017 10.1007/s12094-017-1784-1 Ciruelos E. Vidal M. Martínez de Dueñas E. Martínez-Jáñez N. Fernández Y. García-Sáenz J. A. Murillo L. Carabantes F. Beliera A. Fonseca R. Gavilá J. Clinical and Translational Oncology Safety of everolimus plus exemestane in patients with hormone-receptor-positive, HER2-negative locally advanced or metastatic breast cancer: results of phase IIIb BALLET trial in Spain 30 4 10 877-885 144 2018 10.1002/ijc.31738 Tesch Hans Stoetzer Oliver Decker Thomas Kurbacher Christian M. Marmé Frederik Schneeweiss Andreas et al International Journal of Cancer Efficacy and safety of everolimus plus exemestane in postmenopausal women with hormone receptor-positive, human epidermal growth factor receptor 2-negative locally advanced or metastatic breast cancer: Results of the single-arm, phase IIIB 4EVER trial 01 BCBCR.S12443 10 2016 10.4137/bcbcr.s12443 Lousberg Laurence Jerusalem Guy Breast Cancer: Basic and Clinical Research Safety, Efficacy, and Patient Acceptability of Everolimus in the Treatment of Breast Cancer 10 96-101 29 2016 10.1016/j.breast.2016.07.005 Moscetti L. Vici P. Gamucci T. Natoli C. Cortesi E. Marchetti P. et al The Breast Safety analysis, association with response and previous treatments of everolimus and exemestane in 181 metastatic breast cancer patients: A multicenter Italian experience 9769 03 914-923 377 2011 10.1016/s0140-6736(11)60070-6 Cortes Javier O'Shaughnessy Joyce Loesch David Blum Joanne L Vahdat Linda T Petrakova Katarina et al The Lancet Eribulin monotherapy versus treatment of physician's choice in patients with metastatic breast cancer (EMBRACE): a phase 3 open-label randomised study