Residual cancer burden after neoadjuvant chemotherapy and long-term survival outcomes in breast cancer: a multicentre pooled analysis of 5161 patients

Osdoit, Marie; Noordaa, Marieke van der; Shad, Sonal; Wei, Jane; Croze, Diane De; Hamy, Anne-Sophie; Laé, Marick; Reyal, Fabien; Sonke, Gabe S.; Steenbruggen, Tessa G; Seijen, Maartje van; Wesseling, Jelle; Martín, Miguel; Monte-Millán, Marı́a del; López-Tarruella, Sara; Goetz, Matthew P.; Hoskin, Tanya L.; Gould, Rebekah E.; Valero, Vicente; Edge, Stephen B.; Abraham, Jean; Bartlett, John M.S.; Caldas, Carlos; Dunn, Janet A.; Earl, Helena; Hayward, Larry; Hiller, Louise; Provenzano, Elena; Sammut, Stephen‐John; Thomas, Jeremy; Cameron, David; Graham, Alastair; Hall, Peter; Mackintosh, Lorna; Fan, Fang; Godwin, Andrew K.; Schwensen, Kelsey; Sharma, Priyanka; Cole, Kimberly; Kim, Miok; Veer, Laura J. van ’t; Esserman, Laura J.; Symmans, W. Fraser; Adamson, Kathi; Albain, Kathy S.; Asare, Adam; Asare, Smita; Balassanian, Ronald; Beckwith, Heather; Berry, Scott M.; Berry, Donald A.; Boughey, Judy C.; Buxton, Meredith; Chen, Yunn-Yi; Chen, Beiyun; Chien, A. Jo; Chui, Stephen Y.; Clark, Amy S.; Clennell, Julia L.; Datnow, Brian; DeMichele, Angela; Duan, Xiuzhen; Edmiston, Kirsten K.; Elias, Anthony; Ellis, Erin D.; Esserman, Laura; Euhus, David M.; Fadare, Oluwole; Feldman, Michael D.; Forero‐Torres, Andres; Haley, Barbara; Han, Hyo S.; Harada, Shuko; Haugen, Patricia; Helsten, Teresa; Hirst, Gillian; Hylton, Nola M.; Isaacs, Claudine; Kemmer, Kathleen; Khan, Qamar J.; Khazai, Laila; Klein, Molly; Krings, Gregor; Lang, Julie E.; LeBeau, Lauren; Leyland‐Jones, Brian; Liu, Minetta C.; Lo, Shelly S.; Lu, Janice; Magliocco, Anthony M.; Matthews, Jeffrey B.; Melisko, Michelle; Mhawech‐Fauceglia, Paulette; Moulder, Stacy L.; Murthy, Rashmi Krishna; Nanda, Rita; Northfelt, Donald W.; Ocal, Idris Tolgay; Olopade, Olufunmilayo I.; Pambuccian, Stefan E.; Paoloni, Melissa; Park, John W.; Parker, Barbara A.; Perlmutter, Jane; Peterson, Garry; Pusztai, Lajos; Rendi, Mara H.; Rugo, Hope S.; Sahoo, Sunati; Sams, Sharon B.; Sanil, Ashish; Sattar, Husain; Schwab, Richard B.; Singhrao, Ruby; Steeg, Katherine; Stringer-Reasor, Erica; Symmans, W. Fraser; Tawfik, Ossama; Tripathy, Debasish; Troxell, Megan L.; Veer, Laura J. van’t; Venters, Sara J.; Vinh, Tuyethoa N.; Viscusi, Rebecca K.; Wallace, Anne M.; Wei, Shi; Wilson, Amy; Yau, Christina; Yee, Douglas; Zeck, Jay

doi:10.1016/s1470-2045(21)00589-1

Cited by 218 publications

(119 citation statements)

References 32 publications

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“…At the time of surgery (approximately 6 months following core biopsy collection and after all qSMLM data were computed), clinical outcomes and residual cancer burden (RCB) indices were noted. The RCB index (RCB-0 to RCB-III) was designed to quantify residual disease in the tumor bed and lymph nodes after neoadjuvant therapy; it is a well validated prognostic indicator for breast cancer [ 112 , 113 ]. Our sample cohort comprised the following: P18 had RCB-I, P20 had RCB-II, and all other women had achieved a pathological complete response (pCR) equivalent to RCB-0.…”

Section: Resultsmentioning

confidence: 99%

Molecular Assessment of HER2 to Identify Signatures Associated with Therapy Response in HER2-Positive Breast Cancer

Maddox

Brehove

Eliato

et al. 2022

Cancers

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Trastuzumab, the prototype HER2-directed therapy, has markedly improved survival for women with HER2-positive breast cancers. However, only 40–60% of women with HER2-positive breast cancers achieve a complete pathological response to chemotherapy combined with HER2-directed therapy. The current diagnostic assays have poor positive-predictive accuracy in identifying therapy-responsive breast cancers. Here, we deployed quantitative single molecule localization microscopy to assess the molecular features of HER2 in a therapy-responsive setting. Using fluorescently labeled trastuzumab as a probe, we first compared the molecular features of HER2 in trastuzumab-sensitive (BT-474 and SK-BR-3) and trastuzumab-resistant (BT-474R and JIMT-1) cultured cell lines. Trastuzumab-sensitive cells had significantly higher detected HER2 densities and clustering. We then evaluated HER2 in pre-treatment core biopsies from women with breast cancer undergoing neoadjuvant therapy. A complete pathological response was associated with a high detected HER2 density and significant HER2 clustering. These results established the nano-organization of HER2 as a potential signature of therapy-responsive disease.

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Section: Resultsmentioning

confidence: 99%

Molecular Assessment of HER2 to Identify Signatures Associated with Therapy Response in HER2-Positive Breast Cancer

Maddox

Brehove

Eliato

et al. 2022

Cancers

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“…It has recently been recognized that the binary approach of pCR and non-pCR does not stratify the risk groups optimally. Yau et al introduced a categorization according to the residual disease burden, which categorizes the tumor into three grades, according to the size of the residual tumor [ 32 ]. The authors recently found that with an increase in the residual cancer burden, the outcome worsened.…”

Section: Future Approachesmentioning

confidence: 99%

Post-Neoadjuvant Treatment Strategies in Breast Cancer

Matuschek

Jazmati

Bölke

et al. 2022

Cancers

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Neoadjuvant chemotherapy enables close monitoring of tumor response in patients with breast cancer. Being able to assess tumor response during treatment provides an opportunity to evaluate new therapeutic strategies. Thus, for triple-negative breast tumors, it was demonstrated that additional immunotherapy could improve prognosis compared with chemotherapy alone. Furthermore, adjuvant therapy can be escalated or de-escalated correspondingly. The CREATE-X trial randomly assigned HER2-negative patients with residual tumor after neoadjuvant therapy to either observation or capecitabine. In HER2-negative patients with positive BRCA testing, the OlympiA study randomly assigned patients to either observation or olaparib. HER2-positive patients without pathologic remission were randomly assigned to trastuzumab or trastuzumab–emtansine within the KATHERINE study. These studies were all able to show an improvement in oncologic outcome associated with the escalation of therapy in patients presenting with residual tumor after neoadjuvant treatment. On the other hand, this individualization of therapy may also offer the possibility to de-escalate treatment, and thereby reduce morbidity. Among WSG-ADAPT HER2+/HR-, HER2-positive patients achieved comparable results without chemotherapy after complete remission following neoadjuvant treatment. In summary, the concept of post-neoadjuvant therapy constitutes a great opportunity for individualized cancer treatment, potentially improving outcome. In this review, the most important trials of post-neoadjuvant therapy are compiled and discussed.

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“…Neoadjuvant chemotherapy (NAC), is currently used for the treatment of aggressive breast carcinomas that are nonetheless operable [ 6 ], to increase conservative breast surgery rates [ 7 ]. Neoadjuvant chemotherapy has many advantages such as a less extensive breast and axillary surgery and a monitoring of the treatment response [ 8 , 9 ]. Pathological complete response (pCR) has been reported to occur in about 20–60% of patients on NAC, and is associated with better survival outcomes [ 10 – 13 ].…”

Section: Introductionmentioning

confidence: 99%

Digital phenotyping in young breast cancer patients treated with neoadjuvant chemotherapy (the NeoFit Trial): protocol for a national, multicenter single-arm trial

et al. 2022

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Background Breast cancer (BC) has particular characteristics in young women, with diagnosis at more advanced stages, a poorer prognosis and highly aggressive tumors. In NeoFit, we will use an activity tracker to identify and describe various digital profiles (heart rate, physical activity, and sleep patterns) in women below the age of 45 years on neoadjuvant chemotherapy for BC. Methods NeoFit is a prospective, national, multicenter, single-arm open-label study. It will include 300 women below the age of 45 years treated with neoadjuvant chemotherapy for BC. Participants will be asked to wear a Withing Steel HR activity tracker round the clock for 12 months. The principal assessments will be performed at baseline, at the end of neoadjuvant chemotherapy and at 12 months. We will evaluate clinical parameters, such as toxicity and the efficacy of chemotherapy, together with quality of life, fatigue, and parameters relating to lifestyle and physical activity. The women will complete REDCap form questionnaires via a secure internet link. Discussion In this study, the use of an activity tracker will enable us to visualize changes in the lifestyle of young women on neoadjuvant chemotherapy for BC, over the course of a one-year period. This exploratory study will provide crucial insight into the digital phenotypes of young BC patients on neoadjuvant chemotherapy and the relationship between these phenotypes and the toxicity and efficacy of treatment. This trial will pave the way for interventional studies involving sleep and physical activity interventions. Trial registration Clinicaltrials.gov identifier: NCT05011721. Registration date: 18/08/2021.

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Residual cancer burden after neoadjuvant chemotherapy and long-term survival outcomes in breast cancer: a multicentre pooled analysis of 5161 patients

Cited by 218 publications

References 32 publications

Molecular Assessment of HER2 to Identify Signatures Associated with Therapy Response in HER2-Positive Breast Cancer

Molecular Assessment of HER2 to Identify Signatures Associated with Therapy Response in HER2-Positive Breast Cancer

Post-Neoadjuvant Treatment Strategies in Breast Cancer

Digital phenotyping in young breast cancer patients treated with neoadjuvant chemotherapy (the NeoFit Trial): protocol for a national, multicenter single-arm trial

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