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Abstract P3-02-01: Initial experience of FES-dedicated breast PET imaging of early-stage ER+ invasive lobular carcinoma

Jones, Ella F ; Hathi, Deep K ; Konovalova, Natalia ; [et al.]

American Association for Cancer Research (AACR) ; 2022

In: Cancer Research Vol. 82, No. 4_Supplement ( 2022-02-15), p. P3-02-01-P3-02-01

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In: Cancer Research, American Association for Cancer Research (AACR), Vol. 82, No. 4_Supplement ( 2022-02-15), p. P3-02-01-P3-02-01

Abstract: BACKGROUND: Invasive lobular carcinoma (ILC) is the second most common histological subtype of breast cancer, representing 15% of all invasive breast cancers. Most ILC tumors are estrogen receptor-positive (ER+) and may respond to endocrine therapy. However, tumor biologic factors such as ER functionality, cell proliferation, and molecular traits may influence endocrine treatment response and long-term recurrence risk, thus necessitating a comprehensive approach to characterize the primary breast tumor. [18F]fluoroestradiol (FES) is a radiotracer developed for positron emission tomography (PET) imaging of ER status. For this work, we studied the utility of imaging FES uptake in early-stage primary ER+ ILC lesions, using high-resolution dedicated breast PET (dbPET) to assess the relationship between FES uptake and tumor characteristics. METHODS: With institutional review board approval, patients with biopsy-proven ER+/HER2- ILC were prospectively imaged using dbPET with 5 mCi of FES before treatment. FES uptake (SUVmax, SUVmean, and SUVpeak), tumor uptake volume (TUV), and background parenchymal uptake (BPU) values were calculated. Background values (SUVbkg) were obtained from the normal region of the ipsilateral breast. Lesions with background-corrected SUVmax 2 times higher than SUVbkg were considered FES-avid. Tumor grade, Ki 67 cell proliferation index, and ER expression were obtained from core biopsies before treatment. Ki67 was dichotomized to low and high using a 20% cutoff1. Tumor size (longest diameter) was measured by magnetic resonance imaging (MRI). Spearman rank correlation was used to assess the relationship between FES uptake and tumor size. Differences between FES uptake at high and low Ki67 were compared using a Wilcoxon rank-sum test. RESULTS: 13 treatment-naïve ILC patients aged 32-82 years were included in this analysis (Table 1). Despite all lesions exhibiting strongly positive ER expression & gt;90% by immunohistochemistry (IHC), we observed varying FES avidity with 9 FES avid and 4 FES non-avid ILC lesions. SUVmax, TUV, and TBR had substantial median differences between Ki67 high and low lesions (5.9, 4.3, and 9.6, respectively), but the difference did not achieve statistical significance. FES tumor uptake also correlated with tumor size, with the highest correlation observed for SUVpeak (ρ = 0.71 (95% CI: 0.22, 0.91), p=0.010) (Table 2). CONCLUSION: We found that not all highly ER expressing ILC by IHC were FES-avid. As FES-dbPET captures information from the entire tumor, it provides a more comprehensive assessment of functional ER status than IHC of a limited tumor sample. FES uptake in ILC also relates to tumor size and Ki67. This is an ongoing study; additional data may help to guide endocrine therapy decisions. Future studies with a larger cohort are planned to assess the relationship between FES uptake and tumor grade and molecular risk profiles. 1. Acs, B. et al. Ki-67 as a controversial predictive and prognostic marker in breast cancer patients treated with neoadjuvant chemotherapy. Diagn Pathol 12, 20, doi:10.1186/s13000-017-0608-5 (2017). Patient and tumor characteristicsCharacteristicsNumber of patients (Total N=13)Age (median (range))56.0 (32-80)Pre-menopausal3Post-menopausal10MRI tumor size (median (interquartile range)4.1 (2.4-6.8)Tumor grade132931Ki6712Low/High3/9FES13Avid/Non-avid9/4 Summary of FES uptake values and correlation coefficients.FES avidity (N=13)Ki67 (N=12)MRI tumor size (N=12)Avid vs Non-avidHigh vs LowSpearman rank correlationMedian Difference (95% CI)P-valueMedian Difference (95% CI)P-valueSpearman ρ (95% CI)P-valueSUVmax8.68 (2.86, 12)0.0075.9 (-19.5, 11.6)0.140.67 (0.16, 0.9)0.017SUVmean2.56 (1.43, 4.86)0.0071.34 (-4.14, 3.1)0.200.6 (0.042, 0.87)0.039SUVpeak2.86 (1.14, 4.59)0.0112.15 (-14.4, 3.72)0.190.71 (0.22, 0.91)0.01BPU-0.31 (-1.89, 1.02)0.82-0.73 (-2.34, 0.28)0.0960.01 (-0.57, 0.58)0.98TUV (cm3)5.45 (1.04, 10)0.014.3 (-185, 10)0.190.70 (0.21, 0.91)0.011TBR3.61 (2.2, 13)0.0079.57 (-19.6, 12.4)0.0640.66 (0.13, 0.89)0.02 Citation Format: Ella F Jones, Deep K Hathi, Natalia Konovalova, Julissa Molina-Vega, David C Newitt, Courtney Lawhn-Heath, Kimberly M Ray, Bonnie N Joe, Diane Heditsian, Susie Brain, I-SPY 2 TRIAL Imaging Working Group, I-SPY 2 TRIAL Consortium, A. Jo Chien, Laura J Esserman, Nola M Hylton, Rita A Mukhtar. Initial experience of FES-dedicated breast PET imaging of early-stage ER+ invasive lobular carcinoma [abstract]. In: Proceedings of the 2021 San Antonio Breast Cancer Symposium; 2021 Dec 7-10; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2022;82(4 Suppl):Abstract nr P3-02-01.

Type of Medium: Online Resource

ISSN: 0008-5472 , 1538-7445

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DOI: 10.1158/1538-7445.SABCS21-P3-02-01

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Language: English

Publisher: American Association for Cancer Research (AACR)

Publication Date: 2022

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Abstract P3-03-02: Diffusion-weighted MRI for prediction of pathologic complete response in HER2- breast cancer treated with pembrolizumab plus neoadjuvant chemotherapy

Li, Wen ; Le, Nu N ; Onishi, Natsuko ; [et al.]

American Association for Cancer Research (AACR) ; 2022

In: Cancer Research Vol. 82, No. 4_Supplement ( 2022-02-15), p. P3-03-02-P3-03-02

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In: Cancer Research, American Association for Cancer Research (AACR), Vol. 82, No. 4_Supplement ( 2022-02-15), p. P3-03-02-P3-03-02

Abstract: Background: Checkpoint blockade pembrolizumab has demonstrated great potential to improve pathologic outcome for HER2- breast cancer. The apparent diffusion coefficient (ADC) is a non-contrast MRI-derived biomarker that is sensitive to changes in tumor cellularity. Clinical trial ACRIN 6698, a sub-study of I-SPY 2, demonstrated that ADC can predict pathologic complete response (pCR). This study compares the utility of ADC for early prediction of pCR in patients with HER2- breast cancer randomized to pembrolizumab versus standard neoadjuvant chemotherapy (NACT) in I-SPY 2. Methods: A retrospective analysis of imaging and clinical data was performed on a cohort of 249 women diagnosed with high-risk, stage II/III breast cancer. All patients were randomized to the standard NACT (paclitaxel) or pembrolizumab plus paclitaxel for 12 weeks, followed by doxorubicin plus cyclophosphamide. MRI exams performed at pretreatment (T0) and 3 weeks after the treatment started (T1) were analyzed. Tumor ADC was calculated within manually delineated region-of-interests on diffusion-weighted MRI. The percent change of ADC from T0 to T1 was evaluated in the prediction of pCR after NACT. Statistical analysis included Wilcoxon rank sum test and the area under the ROC curve (AUC). A p-value & lt;0.05 was considered statistically significant. Results: A subcohort of 103 patients with analyzable diffusion-weighted MRI exams and known pCR (n=30)/non-pCR (n=73) outcome were included in this analysis. Among 103 patients, 62 had HR+/HER2- and 41 had triple negative breast cancer. Twenty-eight patients (17 HR+/HER2- and 11 triple negative) were randomized to receive pembrolizumab and 75 (45 HR+/HER2- and 30 triple negative) to standard NACT. Tumor ADC increased at 3 weeks in both standard and pembrolizumab cohorts with median ADC change of 11.5% (interquartile range [IQR]: 4.6, 16.2)% and 14.4% (IQR: 0.2, 19.9)%, respectively. In the pembrolizumab cohort, the difference in ADC change between non-pCR and pCR groups was estimated as -9.7% (95% confidence interval [CI] : -22.4, -0.9), with ADC increasing more in the pCR group. The AUC of predicting pCR in the pembrolizumab cohort was estimated as 0.73 (95%CI: 0.52, 0.93), while it was estimated as 0.63 (95% CI: 0.43, 0.83) in the standard NACT cohort. In comparison, the AUCs using functional tumor volume (FTV) to predict pCR were 0.61 (95%CI: 0.39, 0.83) and 0.66 (95% CI: 0.47, 0.85) in the corresponding cohorts (Table 1). The results suggest that ADC had higher association with pCR than FTV in the pembrolizumab cohort and FTV had higher association than ADC in the standard cohort. Conclusions: Tumor ADC, measured using diffusion-weighted MRI, demonstrates potential as a biomarker for assessing early response to immunotherapy in the neoadjuvant setting for high risk HER2- breast cancer. This study is limited by sample size. Future analysis with larger cohorts is warranted. Table 1.Association between MRI variables and pCRN (pCR rate)Difference between non-pCR and pCR groups (95% CI)AUC (95% CI)pDiffusion weighted MRI (percent change of ADC)Pembrolizumab28 (54%)-9.7 (-22.4, -0.9)0.73 (0.52, 0.93)0.041Standard75 (20%)-5.6 (-13.9, 2.1)0.63 (0.43, 0.83)0.13DCE-MRI (percent change of FTV)Pembrolizumab28 (54%)10.6 (-18.3, 43.9)0.61 (0.39, 0.83)0.34Standard74 (20%)25.3 (-0.6, 49)0.66 (0.47, 0.85)0.056 Citation Format: Wen Li, Nu N Le, Natsuko Onishi, David C Newitt, Jessica E Gibbs, Lisa J Wilmes, John Kornak, Savannah C Partridge, Barbara LeStage, Elissa R Price, Bonnie N Joe, I-SPY 2 TRIAL Imaging Working Group, I-SPY 2 TRIAL Consortium, Laura J Esserman, Nola M Hylton. Diffusion-weighted MRI for prediction of pathologic complete response in HER2- breast cancer treated with pembrolizumab plus neoadjuvant chemotherapy [abstract]. In: Proceedings of the 2021 San Antonio Breast Cancer Symposium; 2021 Dec 7-10; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2022;82(4 Suppl):Abstract nr P3-03-02.

Type of Medium: Online Resource

ISSN: 0008-5472 , 1538-7445

URL: Article

DOI: 10.1158/1538-7445.SABCS21-P3-03-02

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XA 10000

Language: English

Publisher: American Association for Cancer Research (AACR)

Publication Date: 2022

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detail.hit.zdb_id: 410466-3

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Abstract P3-02-02: FES-dedicated breast PET uptake in early-stage ER+ breast cancers

Jones, Ella F. ; Hathi, Deep K. ; Molina-Vega, Julissa ; [et al.]

American Association for Cancer Research (AACR) ; 2022

In: Cancer Research Vol. 82, No. 4_Supplement ( 2022-02-15), p. P3-02-02-P3-02-02

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In: Cancer Research, American Association for Cancer Research (AACR), Vol. 82, No. 4_Supplement ( 2022-02-15), p. P3-02-02-P3-02-02

Abstract: BACKGROUND: Patients with ER+ breast cancer may have a recurrence risk of aggressive disease. While clinical evidence suggests that ER+ tumors are responsive to endocrine therapy, up to one-third of patients with early-stage ER+ disease may not respond to endocrine therapy. Tumor biologic factors such as ER functionality, cell proliferation, and molecular traits may influence endocrine treatment responsiveness and long-term recurrence risk. More comprehensive tools are needed to depict the primary breast tumor. [18F]fluoroestradiol (FES) is a radiotracer developed for positron emission tomography (PET) imaging of ER status. We used FES with a high-resolution dedicated breast PET (dbPET) to quantify ER expression in primary ER+ tumors and assessed the relationship between FES uptake and tumor characteristics. METHODS: With IRB approval, patients with biopsy-proven ER+/HER2- breast cancer were imaged using dbPET with 5 mCi of FES before treatment. FES uptake (SUVmax, SUVmean, and SUVpeak), background parenchymal uptake (BPU), tumor uptake volume (TUV), and tumor to background ratio (TBR) were calculated. Background values (SUVbkg) were obtained from the normal region of the ipsilateral breast. Lesions with background-corrected SUVmax 2 times higher than SUVbkg were considered FES avid. Tumor size (longest diameter) was measured by MRI. The histologic subtype, ER expression, tumor grade, and Ki67 were obtained from core biopsies before treatment. Ki67 was dichotomized to low and high using a 20% cutoff. Spearman’s rank correlation was used to assess the correlation between FES uptake and tumor size. Differences between FES uptake, histologic subtype, and Ki67 were compared using a Wilcoxon rank-sum test. RESULTS: 19 treatment-naïve patients were included in this analysis as part of an ongoing study. Patient and tumor characteristics are listed in Table 1. While all patients had ER positivity & gt;90% by immunohistochemistry (IHC), we observed varying FES avidity in ER+ breast cancers, with 14 FES avid and 5 non-FES avid lesions. There was a statistically significant difference between FES avid vs. non-avid lesions measured by all uptake metrics except BPU. FES uptake in invasive ductal carcinoma was similar to invasive lobular carcinoma. FES uptake correlated with tumor size, with the highest correlation ρ = 0.58, 95% CI (0.17, 0.84), p=0.012, detected in TUV. FES uptake was associated with Ki67, with all uptake metrics except BPU showing a statistically significant difference between high and low Ki67 expression (Table 2). CONCLUSION: We found that not all lesions that were highly ER+ by IHC were FES avid. FES-dbPET captures information from the entire tumor, providing a more comprehensive assessment of functional ER status than IHC of a limited tumor sample. Moreover, FES uptake correlates with tumor size and cell proliferation. This is an ongoing study; additional data may help to guide endocrine therapy decisions. Future studies with a larger cohort are planned to assess the relationship between FES uptake and tumor grade and molecular risk profiles. Table 1.Patient and tumor characteristicsCharacteristicsNo. of patientsTotal N=19Age (median (IQR))56.0 (21.5)Pre-menopausal7Post-menopausal12Histologic subtypeInvasive ductal carcinoma (IDC)6Invasive lobular carcinoma (ILC)13Tumor size (N=18) (MRI LD (cm), median (IQR))3.2 (4.1)Tumor grade1421332Ki67Low12High6Unknown1FESNon-avid5Avid14 Table 2.Summary of baseline FES uptake valuesTumor Size (cm)FES AvidityHistologic SubtypeKi67Spearman CorrelationAvid vs. Non-avidILC vs. IDCHigh vs. Lowρ (95%CI)P-valueMedian Diff (95%CI)P-valueMedian Diff (95%CI)P-valueMedian Diff (95%CI)P-valueSUVmax0.51 (0.054, 0.79)0.0318.02 (3.55, 11.9)0.0010.187 (-8.04, 6.32)0.976.38 (2.36, 11.6)0.017SUVmean0.31 (-0.18, 0.68)0.2042.42 (1.47, 3.49)0.001-0.477 (-1.96, 1.37)0.571.61 (0.81, 2.77)0.028SUVpeak0.46 (-0.0053, 0.76)0.0533.16 (1.42, 5.2)0.003-0.583 (-3.76, 2.61)0.633.16 (1.32, 4.66)0.013BPU-0.09 (-0.53, 0.39)0.723-0.33 (-1.25, 0.46)0.3790.226 (-0.58, 1.19)0.40-0.49 (-1.49, 0.28)0.122TUV (cm3)0.58 (0.15, 0.82)0.0125.45 (1.09, 12.5)0.005-2.82 (-12.5, 4.06)0.405.9 (0.98, 12.66)0.021TBR0.5 (0.047, 0.79)0.0333.48 (2.2, 13.5)0.001-0.295 (-11.9, 7.42)0.9010.2 (1.47, 13.49)0.028 Citation Format: Ella F. Jones, Deep K. Hathi, Julissa Molina-Vega, David C. Newitt, Courtney Lawhn-Heath, Kimberly M. Ray, Bonnie N. Joe, Diane Heditsian, Susie Brain, Rita A. Mukhtar, A. Jo Chien, Hope S. Rugo, I-SPY 2 TRIAL Consortium, I-SPY 2 TRIAL Imaging Working Group, Laura J. Esserman, Nola M. Hylton. FES-dedicated breast PET uptake in early-stage ER+ breast cancers [abstract] . In: Proceedings of the 2021 San Antonio Breast Cancer Symposium; 2021 Dec 7-10; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2022;82(4 Suppl):Abstract nr P3-02-02.

Type of Medium: Online Resource

ISSN: 0008-5472 , 1538-7445

URL: Article

DOI: 10.1158/1538-7445.SABCS21-P3-02-02

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XA 10000

Language: English

Publisher: American Association for Cancer Research (AACR)

Publication Date: 2022

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detail.hit.zdb_id: 410466-3

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Abstract P2-07-03: Refining neoadjuvant predictors of three year distant metastasis free survival: Integrating volume change as measured by MRI with residual cancer burden

Hylton, NM ; Symmans, WF ; Yau, C ; [et al.]

American Association for Cancer Research (AACR) ; 2019

In: Cancer Research Vol. 79, No. 4_Supplement ( 2019-02-15), p. P2-07-03-P2-07-03

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In: Cancer Research, American Association for Cancer Research (AACR), Vol. 79, No. 4_Supplement ( 2019-02-15), p. P2-07-03-P2-07-03

Abstract: Background: Patients achieving a pathologic complete response (pCR) following neoadjuvant therapy have significantly improved event-free survival relative to those who do not; and pCR is an FDA-accepted endpoint to support accelerated approval of novel agents/combinations in the neoadjuvant treatment of high risk early stage breast cancer. Previous studies have shown that recurrence risk increased with increasing burden of residual disease (as assessed by the RCB index). As well, these studies suggest that patients with minimum residual disease (RCB-I class) also have favorable outcomes (comparable to those achieving a pCR) within high risk tumor subtypes. In this study, we assess whether integrating RCB with MRI functional tumor volume (FTV), which in itself is prognostic, can improve prediction of distant recurrence free survival (DRFS); and identify a subset of patients with minimal residual disease with comparable DRFS as those who achieved a pCR. Imaging tools can then be used to identify the subset that will do well early and guide the timing of surgical therapy. Method: We performed a pooled analysis of 596 patients from the I-SPY2 TRIAL with RCB, pre-surgical MRI FTV data and known follow-up (median 2.5 years). We first assessed whether FTV predicts residual disease (pCR or pCR/RCB-I) using ROC analysis. We applied a power transformation to normalize the pre-surgical FTV distribution; and assessed its association with DRFS using a bi-variate Cox proportional hazard model adjusting for HR/HER2 subtype. We also fitted a bivariate Cox model of RCB index adjusting for subtype; and assessed whether adding pre-surgical FTV to this model further improves association with DRFS using a likelihood ratio (LR) test. For the Cox modeling, penalized splines approximation of the transformed FTV and RCB index with 2 degrees of freedom was used to allow for non-linear effects of FTV and RCB on DRFS. Result: Pre-surgical MRI FTV is significantly associated with DRFS (Wald p & lt;0.00001), and more effective at predicting pCR/RCB-I than predicting pCR alone (AUC: 0.72 vs. 0.65). Larger pre-surgical FTV remains associated with worse DRFS adjusting for subtype (Wald p & lt;0.00001). The RCB index is also significantly associated with DRFS adjusting for subtype (Wald p & lt;0.00001). Adding FTV to a model containing RCB and subtype further improves association with DRFS (LR p=0.0007). RCB-I patients have excellent DRFS (94% at 3 years compared to 95% in the pCR group). Efforts are underway to identify an optimal threshold for dichotomizing pre-surgical FTV and FTV change measures for use in combination with pCR/RCB-I class to generate integrated RCB (iRCB) groups as a composite predictor of DRFS. Conclusion: Pre-surgical MRI FTV is effective at predicting minimal residual disease (RCB0/I) in the I-SPY 2 TRIAL. Despite the association between FTV and RCB, FTV appears to provide independent added prognostic value (to RCB and subtype), suggesting that integrating MRI volume measures and RCB into a composite predictor may improve DRFS prediction. Citation Format: Hylton NM, Symmans WF, Yau C, Li W, Hatzis C, Isaacs C, Albain KS, Chen Y-Y, Krings G, Wei S, Harada S, Datnow B, Fadare O, Klein M, Pambuccian S, Chen B, Adamson K, Sams S, Mhawech-Fauceglia P, Magliocco A, Feldman M, Rendi M, Sattar H, Zeck J, Ocal I, Tawfik O, Grasso LeBeau L, Sahoo S, Vinh T, Yang S, Adams A, Chien AJ, Ferero-Torres A, Stringer-Reasor E, Wallace A, Boughey JC, Ellis ED, Elias AD, Lang JE, Lu J, Han HS, Clark AS, Korde L, Nanda R, Northfelt DW, Khan QJ, Viscusi RK, Euhus DM, Edmiston KK, Chui SY, Kemmer K, Wood WC, Park JW, Liu MC, Olopade O, Tripathy D, Moulder SL, Rugo HS, Schwab R, Lo S, Helsten T, Beckwith H, Haugen PK, van't Veer LJ, Perlmutter J, Melisko ME, Wilson A, Peterson G, Asare AL, Buxton MB, Paoloni M, Clennell JL, Hirst GL, Singhrao R, Steeg K, Matthews JB, Sanil A, Berry SM, Abe H, Wolverton D, Crane EP, Ward KA, Nelson M, Niell BL, Oh K, Brandt KR, Bang DH, Ojeda-Fournier H, Eghtedari M, Sheth PA, Bernreuter WK, Umphrey H, Rosen MA, Dogan B, Yang W, Joe B, I-SPY 2 TRIAL Consortium, Yee D, Pusztai L, DeMichele A, Asare SM, Berry DA, Esserman LJ. Refining neoadjuvant predictors of three year distant metastasis free survival: Integrating volume change as measured by MRI with residual cancer burden [abstract]. In: Proceedings of the 2018 San Antonio Breast Cancer Symposium; 2018 Dec 4-8; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2019;79(4 Suppl):Abstract nr P2-07-03.

Type of Medium: Online Resource

ISSN: 0008-5472 , 1538-7445

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DOI: 10.1158/1538-7445.SABCS18-P2-07-03

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Language: English

Publisher: American Association for Cancer Research (AACR)

Publication Date: 2019

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Abstract PS4-09: Pathologic features of the inter-regimen biopsy predict response to neoadjuvant therapy in the I-SPY 2 TRIAL

Carter, Jodi M ; Klein, Molly E ; Venters, Sara J ; [et al.]

American Association for Cancer Research (AACR) ; 2021

In: Cancer Research Vol. 81, No. 4_Supplement ( 2021-02-15), p. PS4-09-PS4-09

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In: Cancer Research, American Association for Cancer Research (AACR), Vol. 81, No. 4_Supplement ( 2021-02-15), p. PS4-09-PS4-09

Abstract: Background: I-SPY 2 is a neoadjuvant platform trial open to patients with locally advanced, molecular high-risk breast cancer. In a concerted pursuit of mid-therapy response biomarkers, we evaluated inter-regimen biopsies, to identify patients who may be candidates for treatment de-escalation. In a pilot study, we observed that absence of carcinoma in an inter-regimen biopsy may predict pathologic complete response (pCR). In this expanded study of 100 participants, we sought to confirm that finding and assess pathologic features of the inter-regimen biopsy as predictors of tumor response to neoadjuvant therapy. Methods: Digital H & E images of 100 inter-regimen (12 week) image-guided breast biopsies +/- ancillary immunohistochemistry (p63 and/or cytokeratin) were reviewed by 9 I-SPY affiliated pathologists to record 1) tumor bed and 2) presence/absence of residual invasive carcinoma (IC) (with tumor cellularity scored as 0-100%). The data set included 393 cores (mean 3.9 (2-4) cores/biopsy). Fisher’s exact t-test was used for association of presence/absence of IC with pCR, and tumoral hormone receptor (HR) and HER2 status. Association between biopsy tumor cellularity and residual cancer burden (RCB) indices used Pearson’s correlation. Results: In the biopsy set, 84 (84%) had ≥80% inter-observer diagnostic agreement on both 1) presence of tumor bed and 2) presence/absence of IC (53 IC+ /31 IC-). IC+/IC- biopsies had equal numbers of evaluable tissue cores. The primary tumors were 63% HR+/37% HR-. The presence of IC in the biopsy correlated with tumoral HR/HER2 status (p=0.0014: 74%: HR+HER2-; 62%: TN; 60%: HR+HER2+; 10%: HR-HER2+). Of 31 patients with IC- biopsies, 25 (80%) went on to pCR, whereas only 7/53 (13%) of patients with IC+ biopsies had pCR, conferring an odds ratio for pCR of 26, Fisher p=7.5E-10. Overall, IC- biopsies had a positive predictive value (PPV) for pCR of 81%, with a PPV for HR- tumors of 94% vs. 67% for HR+ tumors (Table 1). In the 6 IC- biopsies from patients with non-pCR (“false-negatives”), most were HR+ (5/6, Table 1), and tumor bed size in the resection specimen was smaller than for IC+ biopsies with non-pCR: 276 mm2 (0.4-1000 mm2) vs. 1166 mm2 (1-11960 mm2). In contrast, the 46/53 IC+ biopsies in patients with non-pCR had a PPV for predicting non-pCR of 86%, (PPV for HR+ tumors: 94% vs. PPV for HR- tumors: 66%. Tumor cellularity in the biopsy (mean 37%, [2.5-93%]) did not correlate with RCB index (p=0.57) or RCB breast-only index (p = 0.17) at resection. Conclusion: In this 100 biopsy set from the I-SPY2 trial, the absence of residual carcinoma in inter-regimen biopsies was highly predictive of pCR, particularly for HR- tumors. The “false-negative” biopsies (IC-/non-pCR) were predominantly HR+ tumors with small residual tumor beds at resection. Conversely, the presence of carcinoma in inter-regimen biopsies was highly predictive of non-pCR, particularly for HR+ tumors. These data demonstrate the utility, and the limitations, of the inter-regimen biopsy as one tool to identify patients who may benefit from therapeutic de-escalation. Table 1: PPV for pCR/non-PCR by Inter-regimen Biopsy StatusInter-regimen biopsy with or without Invasive carcinoma (IC+/-)pCRnon-pCRPPV (Sensitivity) for pCR(IC- Biopsies)PPV (Sensitivity) for non-pCR(IC+ biopsies)IC- biopsiesAll25681% (78%)-HR+10567% (83%)-HR-15194% (75%)-IC+ biopsiesAll746-86% (88%)HR+236-94% (88%)HR-510-66% (91%) Citation Format: Jodi M Carter, Molly E Klein, Sara J Venters, Kimmie Rabe, I Tolgay Ocal, Kamaljeet Singh, Denise M Wolf, Sunati Sahoo, Shuko Harada, Laila Khazai, Malini Harigopal, Alexander D Borowsky, Gregor Krings, Ronald Balassanian, Yunn-Yi Chen, Kimberley Cole, Sonal Shad, Amy Delson, Lamorna Brown-Swigart, I-SPY 2 TRIAL Consortium, Laura Esserman, Laura van ‘t Veer, W Fraser Symmans. Pathologic features of the inter-regimen biopsy predict response to neoadjuvant therapy in the I-SPY 2 TRIAL [abstract] . In: Proceedings of the 2020 San Antonio Breast Cancer Virtual Symposium; 2020 Dec 8-11; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2021;81(4 Suppl):Abstract nr PS4-09.

Type of Medium: Online Resource

ISSN: 0008-5472 , 1538-7445

URL: Article

DOI: 10.1158/1538-7445.SABCS20-PS4-09

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Language: English

Publisher: American Association for Cancer Research (AACR)

Publication Date: 2021

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Abstract P5-01-04: Personalized monitoring of circulating tumor DNA during neoadjuvant therapy in high-risk early stage breast cancer reflects response and risk of metastatic recurrence

Magbanua, Mark Jesus M ; Brown-Swigart, Lamorna ; Hirst, Gillian ; [et al.]

American Association for Cancer Research (AACR) ; 2020

In: Cancer Research Vol. 80, No. 4_Supplement ( 2020-02-15), p. P5-01-04-P5-01-04

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In: Cancer Research, American Association for Cancer Research (AACR), Vol. 80, No. 4_Supplement ( 2020-02-15), p. P5-01-04-P5-01-04

Abstract: Background: The detection of circulating tumor DNA (ctDNA) during neoadjuvant therapy (NAT) may serve as an early indicator of emerging resistance and disease progression. In this study, we analyzed ctDNA from high-risk early breast cancer patients who received NAT and definitive surgery in the I-SPY 2 TRIAL (NCT01042379). We hypothesized that ctDNA can serve as a biomarker of response and survival in this setting. Methods: ctDNA analysis was performed on 291 plasma samples from 84 high-risk stage II and III breast cancer patients randomized either to an investigational agent MK-2206, an AKT inhibitor, in combination with paclitaxel followed by doxorubicin and cyclophosphamide (AC) (n=52)—or standard-of-care (paclitaxel followed by AC) (n=32). HER2+ patients also received trastuzumab. Serial plasma was collected at pretreatment (T0), at 3 weeks after initiation of paclitaxel treatment (T1), between paclitaxel and AC regimens (T2), and after NAT prior to surgery (T3). A personalized ctDNA test was designed to detect a set of 16 patient-specific somatic variants, initially identified from whole exome sequencing of pretreatment tumor, then tested in plasma samples. Regions containing the somatic variants were amplified from cell-free DNA using specific polymerase chain reaction primers. Amplified products were subjected to ultra-deep sequencing (mean: 94,000x) to detect somatic variants. Association between ctDNA and clinicopathologic variables was assessed using Fisher’s exact test. Association of ctDNA with response and survival was analyzed using logistic and Cox regressions, respectively. The survival endpoint of the study was distant disease-free survival. The median follow-up was 4.8 years. Results: At pretreatment (T0), 61 of the 84 (73%) patients had detectable ctDNA. Pretreatment (T0) ctDNA positivity and levels (mean mutant molecules per mL of plasma) were significantly associated with increased tumor burden (clinical T stage T3/T4), more aggressive tumor biology (higher Mammaprint scores) and subtype (HER2+ and Triple negative). CtDNA detection during NAT decreased over time (T0- 73%; T1- 35%; T2- 14%; T3- 9%). Of the 84 patients, 23 (27%) achieved pCR and all were ctDNA-negative after NAT (T3), while all 6 patients who had detectable ctDNA at T3 did not achieve pCR. Patients who cleared ctDNA early at T1 (n=27, 48% pCR rate) had significantly increased probability of achieving a pathologic complete response (pCR) compared to those who remained ctDNA-positive (n=29, 17% pCR rate; Odds ratio=4.33, Likelihood ratio p=0.012). Patients who were ctDNA-positive at T3 (n=6) had significantly increased risk of metastatic recurrence (HR 14.7; 95% CI 1.6-131.5) compared to those who achieved pCR and were ctDNA-negative (n=17). The risk of metastatic recurrence in patients who cleared ctDNA during NAT was not significantly different from those who were negative at T0 and remained negative by T3 (hazard ratio, HR: 2.1, 95% CI: 0.22-20.2). Interestingly, patients who were ctDNA-negative (n=37) but failed to achieve pCR had similar risk of metastatic recurrence with those who achieved pCR (HR 1.4; 95% CI 0.15-13.5). Conclusions: Early clearance of ctDNA during NAT was significantly associated with increased likelihood of achieving pCR. Residual ctDNA after NAT was a significant predictor of metastatic recurrence, while clearance of ctDNA at any point during NAT was associated with improved outcomes. Taken together, personalized monitoring of ctDNA during NAT may aid in real-time assessment of treatment response and help fine-tune pCR as a surrogate endpoint of survival. Validation studies in a larger cohort are warranted. Citation Format: Mark Jesus M Magbanua, Lamorna Brown-Swigart, Gillian Hirst, Christina Yau, Denise Wolf, Hsin-Ta Wu, Antony Tin, Svetlana Shchegrova, Himanshu Sethi, Raheleh Salari, Alexey Aleshin, Maggie Louie, Bernhard Zimmermann, Angela DeMichele, Minetta Liu, Amy Delson, Amy Jo Chien, Smita Asare, Laura Esserman, I-SPY 2 TRIAL Consortium, Laura van't Veer. Personalized monitoring of circulating tumor DNA during neoadjuvant therapy in high-risk early stage breast cancer reflects response and risk of metastatic recurrence [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr P5-01-04.

Type of Medium: Online Resource

ISSN: 0008-5472 , 1538-7445

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DOI: 10.1158/1538-7445.SABCS19-P5-01-04

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Language: English

Publisher: American Association for Cancer Research (AACR)

Publication Date: 2020

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Abstract PD14-02: Biomarkers predicting response to durvalumab combined with olaparib in the neoadjuvant I-SPY 2 TRIAL for high-risk breast cancer

Wolf, Denise M ; Yau, Christina ; Brown-Swigart, Lamorna ; [et al.]

American Association for Cancer Research (AACR) ; 2021

In: Cancer Research Vol. 81, No. 4_Supplement ( 2021-02-15), p. PD14-02-PD14-02

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In: Cancer Research, American Association for Cancer Research (AACR), Vol. 81, No. 4_Supplement ( 2021-02-15), p. PD14-02-PD14-02

Abstract: Background: Preclinical studies suggest synergy between PARP inhibitors and immune checkpoint inhibitors. In the I-SPY 2 TRIAL, the anti-PDL1 therapeutic antibody durvalumab combined with the PARP inhibitor olaparib showed increased efficacy relative to control in both the HR+/HER2- and TN subtypes. Pre-specified biomarker analysis was performed to test 7 immune genes/signatures previously associated with response to pembrolizumab [Pembro] and/or durvalumab and a DNA Repair Deficiency (DRD) signature previously associated with response to veliparib/carboplatin, as specific predictors of response to durvalumab/olaparib [Durva] . We also assessed MammaPrint (MP) High1/(ultra)High2 risk class (MP1/2), a prognostic signature used in the trial’s adaptive randomization engine, and performed exploratory analysis on additional signatures. Methods: 105 patients (Durva: 71, controls: 34) had Agilent 44K gene expression from FFPE pre-treatment biopsies and pCR data; and 370 (Durva: 71, controls: 299) had MP1/2 and pCR data. We evaluated 13 genes/signatures (10 immune, 1 DRD, 1 ER, 1 proliferation) and MP1/2 as biomarkers of Durva response, using logistic modeling to assess performance. A biomarker is considered a specific predictor of Durva response if it associates with response in the Durva arm, and if the biomarker x treatment interaction is significant (likelihood ratio test, p & lt;0.05). pCR rates within MP1/2 classes are estimated using Bayesian logistic modeling. Analysis is also performed adjusting for HR status as a covariate, and numbers permitting, within receptor subsets. Our statistics are descriptive rather than inferential and do not adjust for multiplicities. Results: 8/10 immune biomarkers, including the genes PD1 and PDL1, and B-cell, dendritic cell and mast cell (but not T-cell or CD68) signatures associate with response to Durva in the population as a whole and in a model adjusting for HR status. As seen in previous immunotherapy trials, higher levels generally associate with pCR, with the exception of the mast cell signature, where high levels associate with non-response as was also shown for Pembro (I-SPY 2). In addition, high levels of the DRD (PARPi7) and proliferation signatures associate with response, as do low levels of ER signaling (ESR1/PGR average). Many of these biomarkers also associate with response in the control arm, and for no immune biomarker is the treatment interaction significant, suggesting a lack of predictive specificity. In subset analysis, 13/14 biomarkers (all but CD68) predict Durva response in the HR+/HER2- subset, with the strongest association to pCR being a low level of ESR1/PGR (p=2E-08). In our Bayesian analysis, the difference in estimated pCR rates between arms are primarily observed in the MP2 subtype, particularly in the HR+/HER2- MP2 patients (estimated pCR rate of 64% in Durv vs 22% in Ctr). In the TN subset, only 3/14 biomarkers associate with response: the STAT1 and TAM/TcCassII-ratio signatures that also associate with durvalumab response in a prior study (NCT02489448) and, interestingly, the proliferation signature. Notably, the dendritic, T-cell and tumor inflammatory signatures (TIS) predicting TN response to Pembro (I-SPY2, GeparSixto) do not associate with Durva response in TNBC, suggesting differences in the biology underlying response to PD1 and PDL1 inhibitors. Conclusion: Multiple immune, DRD, proliferation, and ER signatures associate with response to durvalumab/olaparib therapy, but many lack predictive specificity. MP2 class and/or low ESR1/PGR are the strongest predictors of pCR in the HR+/HER2- subset; whereas for TNs, cytokine- and monocyte-dominated immune signatures like STAT1 [PMID: 19272155] and TAM/TcClassII ratio [PMID: 24205370] are most predictive of response. These results require validation. Citation Format: Denise M Wolf, Christina Yau, Lamorna Brown-Swigart, Nick O'Grady, Gillian Hirst, Laura Sit, I-SPY 2 TRIAL Consortium, Smita Asare, Don Berry, Laura Esserman, Hyo Han, Lajos Pusztai, Laura van 't Veer. Biomarkers predicting response to durvalumab combined with olaparib in the neoadjuvant I-SPY 2 TRIAL for high-risk breast cancer [abstract]. In: Proceedings of the 2020 San Antonio Breast Cancer Virtual Symposium; 2020 Dec 8-11; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2021;81(4 Suppl):Abstract nr PD14-02.

Type of Medium: Online Resource

ISSN: 0008-5472 , 1538-7445

URL: Article

DOI: 10.1158/1538-7445.SABCS20-PD14-02

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Language: English

Publisher: American Association for Cancer Research (AACR)

Publication Date: 2021

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Abstract P3-10-14: LIV-1 expression in primary breast cancers in the I-SPY 2 TRIAL

Yau, C ; Brown-Swigart, L ; Asare, S ; [et al.]

American Association for Cancer Research (AACR) ; 2019

In: Cancer Research Vol. 79, No. 4_Supplement ( 2019-02-15), p. P3-10-14-P3-10-14

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In: Cancer Research, American Association for Cancer Research (AACR), Vol. 79, No. 4_Supplement ( 2019-02-15), p. P3-10-14-P3-10-14

Abstract: Background: LIV-1 is an estrogen-inducible gene that has been implicated in epidermal-to-mesenchymal transition (EMT) in preclinical models of progression and metastasis. Its expression is associated with node-positivity in breast cancer; and has been detected in a variety of cancer types, including estrogen receptor positive breast cancers. SGN-LIV1A is a novel antibody drug conjugate targeting LIV-1 that is currently being evaluated in the I-SPY 2 TRIAL. In this pilot study, we evaluated LIV-1 levels by IHC within HR/HER2/MammaPrint (MP) defined subtypes among patients screening for the I-SPY 2 TRIAL and its correlation to microarray assessed LIV-1 expression levels. Method: In a pilot study, LIV-1 IHC staining was performed by Quest Diagnostics on the pre-treatment samples of 38 patients screening for the I-SPY 2 TRIAL. Pre-treatment expression data generated on a custom Agilent 44K platform was also available. We summarized the LIV-1 H-Scores and percent (%)-positivity across the population and within HR/HER2/MP subtypes; and we assessed the Pearson correlation between LIV-1 H-Score and LIV-1 gene expression levels. In addition, we compared the pre-treatment LIV-1 expression levels within HR/HER2/MP subtypes across I-SPY 2 TRIAL patients from completed arms and their relevant controls (n=989) using ANOVA and post-hoc Tukey tests. Our statistics are descriptive rather than inferential; and does not take into account multiplicities of other biomarkers outside of this study. Results: Of the 38 patients evaluated, 37 have LIV-1 %-positivity & gt; 0; and 18 (47%) have 100% LIV1 positivity. The median LIV-1 H-Score is 200; and 89% of patients (34/38) have moderate/high LIV-1 staining (with H-Score≥100). Of the 34 patients who proceeded onto the trial (and have known HR/HER2/MP status), 9 are triple negative, 19 are HR+HER2-, and 6 are HER2+. Due to our small sample size, we did not further subset the triple negative and HER2+ cases; but within the HR+HER2- patients, 10 are MP1 compared to 9 who are MP2 class. LIV1 H-Score appears highest within the HR+HER2-MP1 cases (median: 290), followed by the HER2+ (median: 216), then the HR+HER2-/MP2 (median: 155), and the TN (median: 120) subtype. LIV1 H-score is significantly correlated with LIV-1 mRNA expression levels (Rp=0.79, p & lt;0.0001). Consistent with these observations, LIV-1 pre-treatment expression levels are significantly higher in the HR+HER2-MP1 group relative to all other HR/HER2/MP defined subtypes (Tukey HSD p & lt; 0.0001) across the I-SPY 2 TRIAL population. The HR+HER2+MP1 group also have high LIV-1 expression levels. Conclusion: Our result suggest that although LIV-1 expression differs by subtype, it is expressed at a moderate/high level in the majority of patients. The good correlation between IHC and array-based LIV-1 expression levels enables us to leverage the entire existing I-SPY 2 dataset and confirm the high rates of LIV-1 expression across the I-SPY 2 population. Further studies to evaluate LIV-1 expression as a biomarker of response to LIV-1 targeting therapies for the neoadjuvant treatment of breast cancer are warranted and ongoing in I-SPY 2. Citation Format: Yau C, Brown-Swigart L, Asare S, I-SPY 2 TRIAL Consortium, Esserman L, van' t Veer L, Beckwith H, Forero A, Rugo H. LIV-1 expression in primary breast cancers in the I-SPY 2 TRIAL [abstract]. In: Proceedings of the 2018 San Antonio Breast Cancer Symposium; 2018 Dec 4-8; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2019;79(4 Suppl):Abstract nr P3-10-14.

Type of Medium: Online Resource

ISSN: 0008-5472 , 1538-7445

URL: Article

DOI: 10.1158/1538-7445.SABCS18-P3-10-14

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Language: English

Publisher: American Association for Cancer Research (AACR)

Publication Date: 2019

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Abstract GS5-01: Residual cancer burden after neoadjuvant therapy and long-term survival outcomes in breast cancer: A multi-center pooled analysis

Yau, Christina ; van der Noordaa, Marieke ; Wei, Jane ; [et al.]

American Association for Cancer Research (AACR) ; 2020

In: Cancer Research Vol. 80, No. 4_Supplement ( 2020-02-15), p. GS5-01-GS5-01

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In: Cancer Research, American Association for Cancer Research (AACR), Vol. 80, No. 4_Supplement ( 2020-02-15), p. GS5-01-GS5-01

Abstract: Background: Recent studies have demonstrated independent validation of the prognostic relevance of residual cancer burden (RCB) after neoadjuvant chemotherapy. However, a pooled subject-level analysis of multiple cohorts is needed to determine estimates of long-term prognosis for each class of RCB in each phenotypic subtype of breast cancer (BC) to better inform on patient outcomes. Also, a pooled subject-level analysis allows more detailed analyses of generalizability of the prognostic meaning of RCB assessments in a broader experience of practice settings. Method: Subject-level RCB results, with relevant clinical and pathologic stage, tumor subtype and grade, demographic, treatment and follow-up data from 11 institutes/trials are being collected for combined analysis. The association between the continuous RCB index and event-free survival (EFS), and distant recurrence free survival (DRFS) were assessed using mixed effect Cox models with the incorporation of random RCB coefficients to account for between-study heterogeneity. We will also allow for differences in baseline hazard across biological BC subtypes and, if needed, across studies as well. In addition to this stratified mixed effect model, a multivariate analysis adjusting for age, T-category, nodal status and grade was performed within each subtype. In addition, mixed effect Cox models will be employed to evaluate association between RCB index with EFS and DRFS within each HR/HER2 subtype. Kaplan Meier estimates of EFS and DRFS at 5 and 10 years were computed for each RCB class within subtype. Results: We analyzed subject-level data from 9 institutes/trials representing 4077 patients currently available from an anticipated final total of 4,800 patients (to be presented at the meeting). There were 950 EFS and 876 DRFS events during follow up (median 65 months, IQR: 70 months). RCB index (continuous) was independently prognostic within each subtype: HR+/HER2- (EFS HR (per unit increase in RCB index) =1.64, 95%CI 1.48-1.82; DRFS HR=1.68, 1.51-1.87), HR+/HER2+ (EFS HR=1.80, 1.57-2.05; DRFS HR=1.93, 1.67-2.24), HR-/HER2+ (EFS HR=2.15, 1.76-2.62; DRFS HR=2.10, 1.77-2.50), and HR-/HER2- (EFS HR=2.05, 1.89-2.22; DRFS HR=2.16, 1.90-2.46); and remained prognostic in multivariate models adjusting for age, grade, and clinical T and N stage at diagnosis. Table 1 contains the response rate and estimated EFS at 5 years and 10 years for each RCB class within each HR/HER2 phenotype (DRFS results were similar). Conclusions: Long-term prognosis after pCR was similarly excellent in all phenotypic subtypes. RCB index and classification was independently and strongly prognostic in all subtypes, and generalizable to multiple practice settings. Prognostic differences by RCB class occurred within 5 years in HR- BC, but extended to 10 years in HR+ BC. RCB-I had slightly worse EFS than pCR in HR- BC and HR+/HER2+ BC (after 5 years), but the same EFS as pCR in HR+/HER2- BC. Complete analysis of all subjects, including neoadjuvant treatments, will be presented at the meeting. PhenotypeOutcomepCRRCB-IRCB-IIRCB-IIIHR+/HER2-Frequency (%)11%10%52%27%(N=1467)5 yr EFS (95% CI)91% (86-96)93% (89-98)82% (79-85)70% (65-75)10 yr EFS (95% CI)84% (75-93)88% (82-95)71% (67-75)52% (46-58)HR+/HER2+Frequency (%)38%18%35%9%(N=762)5 yr EFS (95% CI)94% (91-97)93% (88-98)78% (73-84)49% (37-65)10 yr EFS (95% CI)91% (86-96)79% (70-90)65% (59-73)42% (29-60)HR-/HER2+Frequency (%)66%11%18%5%(N=550)5 yr EFS (95% CI)93% (90-96)88% (79-97)60% (50-71)45% (30-69)10 yr EFS (95% CI)90% (86-94)84% (74-95)56% (46-68)45% (30-69)HR-/HER2-Frequency (%)41%13%33%13%(N=1293)5 yr EFS (95% CI)92% (90-94)85% (79-91)68% (63-72)28% (21-36)10 yr EFS (95% CI)87% (82-91)80% (72-88)63% (58-68)24% (18-33) Citation Format: Christina Yau, Marieke van der Noordaa, Jane Wei, Marie Osdoit, Fabien Reyal, Anne-Sophie Hamy, Marick Lae, Miguel Martin, Maria del Monte, I-SPY 2 TRIAL Consortium, Judy C Boughey, Rebekah Gould, Jelle Wesseling, Tessa Steenbruggen, Maartje van Seijen, Gabe Sonke, Stephen Edge, Stephen-John Sammut, Elena Provenzano, Jean Abraham, Peter Hall, Ashley Graham, Lorna Mackintosh, David Cameron, Alice Wang, Priyanka Sharma, Kimberly Cole, Lajos Pusztai, Mi-Ok Kim, Laura van ‘t Veer, Laura Esserman, W. Fraser Symmans. Residual cancer burden after neoadjuvant therapy and long-term survival outcomes in breast cancer: A multi-center pooled analysis [abstract]. In: Proceedings of the 2019 San Antonio Breast Cancer Symposium; 2019 Dec 10-14; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2020;80(4 Suppl):Abstract nr GS5-01.

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ISSN: 0008-5472 , 1538-7445

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DOI: 10.1158/1538-7445.SABCS19-GS5-01

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Language: English

Publisher: American Association for Cancer Research (AACR)

Publication Date: 2020

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Abstract PS6-05: Impact of body mass index on pathological complete response after neoadjuvant chemotherapy: Results from the I-SPY 2 trial

Wang, Haiyun ; Yee, Douglas ; Potter, David ; [et al.]

American Association for Cancer Research (AACR) ; 2021

In: Cancer Research Vol. 81, No. 4_Supplement ( 2021-02-15), p. PS6-05-PS6-05

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In: Cancer Research, American Association for Cancer Research (AACR), Vol. 81, No. 4_Supplement ( 2021-02-15), p. PS6-05-PS6-05

Abstract: Purpose: Increased body mass index (BMI) is a risk factor for breast cancer and has been associated with poor outcomes in both premenopausal and postmenopausal breast cancer patients. Several retrospective studies have demonstrated higher BMI to be associated with inferior pathological complete response (pCR) to neoadjuvant chemotherapy, yet it remains unclear if this difference is related to chemotherapy underdosing among obese breast cancer patients. We evaluated the association between BMI and response to neoadjuvant chemotherapy (defined by pCR) in the I-SPY 2 trial, an adaptive clinical trial platform enrolling biologically high-risk breast cancer patients (triple negative, human epidermal growth factor receptor 2 (HER2) positive and MammaPrint high-risk) that utilizes standard neoadjuvant therapy regimens with treatment based on actual body weight. Patients and Methods: From 3/2010 to 11/2016, 989 patients were enrolled in the I-SPY 2 trial, 978 had a recorded baseline BMI prior to treatment and were included in the analysis. Tumor subtypes were defined by hormone receptor and HER2 status. Pretreatment BMI was categorized as obese (BMI & gt;=30 kg/m2), overweight (25= & lt;BMI & lt;30 kg/m2), and normal or underweight ( & lt;25 kg/m2) based on World Health Organization criteria. pCR was defined as elimination of detectable invasive cancer in the breast and lymph nodes (ypT0/Tis and ypN0) at the time of surgery. Logistic regression analysis was used to determine associations between BMI and pCR, and we reported odds ratios (OR) and 95% confidence intervals (CI). Event-free survival (EFS) and overall survival (OS) between different BMI categories were examined using Cox proportional hazards regression. Results: The median age in our study population was 49 years. 35% of patients were normal/underweight, 32% overweight, and 33% obese. Black patients were more likely to be obese (P & lt;0.0001). pCR rates differed significantly by tumor subtype (P & lt;=0.0001) and tumor stage (P=0.0009). pCR rates were 32.8% in normal/underweight, 31.4% in overweight, and 32.5% in obese patients. In univariable analysis, there was no significant difference in pCR with BMI. In multivariate analysis adjusted for race/ethnicity, age, menopausal status, breast cancer subtype, and clinical stage, there was no significant difference in pCR to neoadjuvant chemotherapy for obese compared with normal/underweight patients (OR=1.1, 95%CI: 0.68-1.63, p=0.83), and for overweight compared with normal/underweight (OR=1, 95%CI: 0.64-1.47, p=0.88). We tested for potential interaction between BMI and breast cancer subtype, however, the interaction was not significant in the multivariate model (P=0.09) (Table 1). Multivariate Cox regression showed there was no difference in EFS (p=0.81) or OS (p=0.52) between obese, overweight and normal/underweight breast cancer patients with a median follow-up time of 4.0 years. Conclusions: There was no difference in pCR rates by BMI with actual body weight based neoadjuvant chemotherapy in this biologically high-risk breast cancer population. In contrast, breast cancer subtype and stage showed predictive value for pCR in this high-risk operable breast cancer population receiving neoadjuvant chemotherapy in the I-SPY 2 clinical trial. Table 1: pCR rate of different BMI categories by breast cancer subtypes.Breast Cancer SubtypepCRNormal/underweight Frequency (%)OverweightFrequency (%)ObeseFrequency (%)P-valueHR+/HER2+No39 (61.9)27 (61.4)32 (66.7)0.83Yes24 (38.1)17 (38.6)16 (33.3)HR+/HER2-No105 (80.8)116 (89.2)93 (78.8)0.06Yes25 (19.2)14 (10.8)25 (21.2)HR-/HER2+No7 (25.0)11 (35.5)15 (51.7)0.11Yes21 (75.0)20 (64.5)14 (48.3)HR-/HER2-No83 (65.4)58 (55.8)76 (60.8)0.33Yes44 (34.7)46 (44.2)49 (39.2)(HR: hormone receptor, HER2: human epidermal growth factor receptor 2) Citation Format: Haiyun Wang, Douglas Yee, David Potter, Patricia Jewett, Christina Yau, Heather Beckwith, Allison Watson, Nicholas G O'Grady, Amy Wilson, Susie Brain, I-SPY 2 TRIAL Consortium, Anne Blaes. Impact of body mass index on pathological complete response after neoadjuvant chemotherapy: Results from the I-SPY 2 trial [abstract]. In: Proceedings of the 2020 San Antonio Breast Cancer Virtual Symposium; 2020 Dec 8-11; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2021;81(4 Suppl):Abstract nr PS6-05.

Type of Medium: Online Resource

ISSN: 0008-5472 , 1538-7445

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DOI: 10.1158/1538-7445.SABCS20-PS6-05

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Language: English

Publisher: American Association for Cancer Research (AACR)

Publication Date: 2021

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