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Apart from tumor characteristics, host factors play a pivotal role in the treatment of cancer. Even though it has been acknowledged since long that host immunity impacts tumor development and progression, extensive research into its prognostic and predictive value in BC has only been initiated more recently. Particularly, the role of the tumor immune infiltrate in the less immunogenic, but frequently diagnosed luminal breast tumors still remains largely unknown. Luminal BC actually is the most frequently diagnosed BC subtype, especially in older patients. As of yet, the tumor immune infiltrate in BC has mainly been studied via evaluating sTILs percentages. It might be more relevant, though, to assess the full immune contexture i.e. abundance, composition, functionality, and spatial distribution of the tumor immune infiltrate. BC is an age-related disease, hence age represents another crucial host factor, which has a substantial impact on BC biology and has been associated with inflammation, deterioration of immune functions (immunosenescence) and clinical frailty. Despite this, and despite the fact that the older population is rapidly growing, older patients with cancer are still largely underrepresented in clinical trials. Although enormous advances have been made in the BC field in general, the older patient population thus remains underexplored, making elderly cancer management very challenging for oncologists. The main objective of this PhD project was to obtain insights in the tumor immune landscape in luminal B-like tumors in relation to patient age and frailty, and to improve our scientific knowledge on the interplay between aging, immunity and cancer. The framework for the project was the IMAGE study, which included patients of different ages with luminal B-like BC.
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Up to thirty percent of patients with early breast cancer (BC) will eventually develop metastases. This results in an ongoing search for treatments to improve the long-term survival of these patients. Immune checkpoint inhibitors (ICI) are one promising type of therapeutic targets and have shown good results in malignancies as melanoma and non-small cell lung cancer. In BC, and especially in triple negative BC (TNBC), a clinical benefit for the addition of ICI to standard therapy has been shown in both the metastatic and early stage of disease. However, only a small subset of patients experience durable and long-term disease control by ICI, with many tumors unlikely to respond. In addition, measurable anti-tumor activity may appear slower in immune therapies than in cytotoxic therapies and lesions may enlarge before shrinking.Therefore, we designed a window-of-opportunity trial (BioKey) to evaluate the short-term effects of the ICI pembrolizumab in patients with early BC with biomarker determination by comparing multiple markers pre-treatment and at surgery.Furthermore, a better understanding of the tumor immune microenvironment (TIME) of TNBC and the other molecular subtypes of BC tumors is paramount to identify and implement new biomarkers in ICI BC treatment. Changes related to intratumoral immunity and proliferation may provide evidence for biological activity of pembrolizumab.The vast majority of studies investigating ICI in patients with BC have focused on TNBC. In our retrospective study, we were able to show that the TIME is very similar between TNBC and HR-negative HER2-positive BC tumors by performing an in-depth characterization of the TIME. A comparative analysis of TNBC and HER2-positive BC revealed no significant differences regarding sTIL and the majority of the investigated immune cell subpopulations (CD3, CD4, CD8, CD73, PD-1, PD-L1). We nevertheless identified significantly higher levels of CD68+ and FOXP3+ cells in TNBC as compared to HER2-positive tumors. Additionally, we performed a similar comparison using publicly available transcriptomics data. Altogether, the results show a comparable TIME in both groups, with possible implications for the use of ICI in patients with HR-negative HER2-positive breast tumors.BioKey was a single center, prospective, open-label, non-randomized study in patients with a non-metastatic newly diagnosed primary invasive carcinoma of the breast. All patients were treated with one intravenous administration of 200 mg of pembrolizumab at 10 ± 4 days before surgery. The study consisted of 2 cohorts with a total of 54 patients; cohort A included 39 patients who were scheduled for upfront surgery and cohort B included 15 patients with estimated residual tumor size of at least 10 mm on imaging after neo-adjuvant chemotherapy. Patients were monitored carefully for the development of adverse events, which were actively reviewed at 10 ± 4 days and 30 ± 7 days after administration of the study medication.Single-cell transcriptome, T-cell receptor and proteome profiling was used to compare paired pre- versus on-treatment biopsies. Pre-treatment, one-third of tumors contained PD1-expressing T-cells, which clonally expanded upon anti-PD1. This expansion mainly involved CD8+ T-cells with increased expression of cytotoxic-activity, immune-cell homing and exhaustion markers, as well as CD4+ T-cells with improved T-helper-1 and follicular-helper activity. We designated these as patients with clonotype expansion or 'expanders' (E), whereas patients lacking clonotype expansion were considered 'non-expanders' (NE). Pre-treatment, immunoregulatory dendritic cells and several macrophage phenotypes expressing PD-L1, and cancer cells exhibiting MHC class I/II expression correlated positively with T-cell expansion. We depicted an immune landscape consisting of various immunophenotypes and associated gene sets being either positively or negatively correlated with T-cell expansion following anti-PD1. Our data suggest novel biomarkers or potential immunotherapeutic modalities to improve clinical benefit from immune checkpoint blockade.Finally, we investigated the TIME of the expander phenotype with central pathology. We observed that i) higher levels of sTIL, PD-1+ sTIL, PD-L1+ and FOXP3+ cells in the pre-treatment biopsies, ii) higher levels of sTIL, PD-1+ sTIL, PD-L1+, CD3+, CD4+, CD8+, CD68+, FOXP3+ cells and Ki67 in the post-treatment surgical specimen, as well as, iii) higher delta values (surgical specimen - biopsy) of sTIL, CD3+, CD4+, CD8+, CD68+ and Ki67 are associated with the expander phenotype. We were able to detect associations between various cell populations of the tumor immune microenvironment evaluated before and after a single dose of pembrolizumab and the T-cell expansion phenotype previously defined at the single-cell level.In a chapter we discuss the immune related adverse events (irAEs) after a single dose of pembrolizumab. Twenty-two patients (41%) experienced at least one adverse event in the follow-up period. In general, the irAEs were mild (grade I or II), and in most cases, no intervention was needed. The observed AEs were common AEs in the context of ICI and were mainly related to gastrointestinal disorders, skin and subcutaneous disorders and hyperthyroidism.Two patients developed late irAEs, which they reported 115 and 101 days after administration of the study medication. The first patient was diagnosed with sarcoidosis and uveitis and the second patient with severe hepatitis. Both patients initially developed hyperthyroidism which later evolved into hypothyroidism. Our observations reinforce the importance of clinical vigilance for late irAEs after ICI discontinuation and imply that merely a single dose of ICI can have a long-lasting immunomodulating effect.In conclusion, we observed that one in three patients demonstrated pronounced clonotype expansion of PD-1-expressing proliferative T-cells along CD8+ or CD4+ trajectories in the post-treatment samples after one dose of pembrolizumab. We hypothesize that this T cell clonotype expansion is a mechanism of response to pembrolizumab. This pronounced clonotype expansion was not limited to patients with TNBC, but was also observed in patients with HR-positive HER2 positive and HR positive BC.Clonotype expansion is clearly measurable via single-cell profiling. The immunohistochemistry data showed associations between the clonotype expansion status, predefined based on single cell profiling, and levels of sTIL and expression of various other immune markers. Nonetheless, we were not able to predict the clonotype expansion status of patients by immunohistochemistry alone. A new neo-adjuvant clinical trial has been designed and will start soon to allow the validation of our findings and to evaluate if T-cIell clonotype expansion is indeed associated with clinical benefit to ICI.
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Non-primary breast tumors are a very rare phenomenon. It occurs most often in patients with a history of malignancies. The symptoms similar to primary breast carcinoma. To conduct this study we first got Ethical approval by The Research Ethics Committee UZ/KU Leuven. Next, we searched the pathology database. We further gathered the used immunohistocytochemistry (IHC) markers, age at diagnosis of metastasis, survival, follow-up and type of therapy. We further examined the literature for single center retrospective reviews and included 7 studies. Our dataset, consisting of 118 patients, was the largest among these studies. In our center, the average age at diagnosis of metastasis was 61 years. The most frequently observed tumor was Diffuse Large B-cell Lymphoma (DLBCL), which occurred in 24 different patients, accounting for 20% of cases. Second most frequent was malignant melanoma with 16 different patients (14%). This was followed by ovarian carcinoma, which occurred in 9 cases (8%). The other studies showed some differences in tumor types, such as more frequent lung adenocarcinomas than ovarian carcinoma, which might have been due to referral bias in our center. Histological diagnosis can be tricky and this highlights the importance of sufficient clinical history and IHC. Survival is overall poor and therapeutic options are mostly systemic, reflecting late stage metastatic disease. Both are however very heterogenous in different tumor types.
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Introduction Phyllodes tumors (PT) of the breast are a rare type of breast tumors. They are classified into three categories: benign, borderline and malignant. The differential diagnosis on core needle biopsy can be challenging because of tumor heterogeneity and overlapping histological features. There is a need for new diagnostic markers that aid in the differential diagnosis between the different subcategories of PT and between PT and fibroadenomas (FA). In this study we evaluate immunohistochemical staining trimethyl lysine 27 of Histone 3 (H3K27me3) as a diagnostic and prognostic marker. Methods We conducted a retrospective study cohort of all cases of primary PT, surgically removed at the UH Leuven since 1990. Control cases of fibroadenomas (FA) were selected. We created tissue micro-arrays (TMAs) on which we performed H3K27me3 immunohistochemistry. We evaluated stromal expression pattern with open source software for digital pathology QuPath. Differences in stromal expression, quantified by semi-quantitative H-score and in the ratio of stromal expression versus epithelial expression (S/E) were compared between the different subgroups of PT and between FA and PT. Statistical analyses was performed using SAS software. Results We included 81 patients with PT and 44 patients with FA. We observed gradually less stromal expression from FA to malignant PT, with an outlier of higher stromal expression in borderline PT. We found statistically significant differences in H-score between FA and all PT (P < 0.001) and between benign PT and malignant/borderline PT combined (P = 0.038). There is no evidence that expression of H3K27me3 is predictive for DFS (HR = 1.031), OS (HR = 0.985 ) or DSS (HR = 1.115). Conclusion A statistically significant difference in expression of H3K27me3 was observed between FA and PT (P = < 0.001). This marker can potentially be used as an additional tool in challenging diagnosis of phyllodes tumors on core needle biopsy. There is no evidence that expression of H3K27me3 expression is predictive for DFS, OS or DSS.
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Background: High levels of stromal tumor infiltrating lymphocytes (TILs) in breast cancer (BC) patients treated with neoadjuvant therapy is predictive of higher levels of pathological complete response (pCR). In this study we evaluated whether the predictive value of TILs is influenced by body mass index (BMI) in HER2+ BC patients treated with neoadjuvant chemotherapy (NACT). Methods: TILs scoring at baseline and post NACT were done on a retrospective series of nonunderweight HER2+ BC patients from 2007-2015 (N = 120). Relevant clinic-pathological information was retrieved from the MBC database of UZL, missing data were collected from medical files of the patients. All patients received anti-HER2 therapy. All variables were considered as categorical (BMI: lean vs overweight vs obese, different predefined cut offs were used for TILs). Descriptive statistical analyzes were performed using the Fisher exact test. Associations between clinicopathological variables and pCR were assessed using Firth logistic regression models. Results: 52 (43%) patients were lean, 44 (37%) overweight and 24 (20%) obese. Overall, pCR was achieved in 53 (44%) of the patients. Median TILs at baseline and post NACT was 8.16 and 2.68, respectively. High TILs were associated with pCR in all BMI categories and regardless of ER status. A decline of mean TILs after neoadjuvant treatment was greater in tumors achieving pCR (16.93% to 2.05%) as compared to tumors with residual disease. The highest rate of pCR was established in overweight patients with ER- BC (20 of 29, 69%). In obese patients a much lower rate of pCR (6 of 24, 25%) was seen compared to lean (21 of 52, 40%) and overweight (26 of 44, 59%) patients. However, no interactions were observed after multivariate analyses using categorical values. Conclusion: High level of TILs are a strong predictor of pCR in HER2+ BC regardless of ER status. The interaction between TILs and BMI deserve further study in HER2+ BC treated with neoadjuvant chemotherapy.
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Worldwide, breast cancer represents about 25% of all cancers in women. There is extensive research effort into this highly complex and heterogeneous disease comprising many different histological and molecular subtypes with luminal, oestrogen receptor (ER)-positive human epidermal growth factor receptor 2 (HER2)-negative tumours being the most frequent subtype. Even within this subtype, there is a lot of heterogeneity, which complicates accurate patient selection for therapeutic decision-making. Patients with luminal early-stage breast cancer receive endocrine treatment for at least 5 years after surgery as standard of care. Some patients also benefit from the addition of adjuvant chemotherapy (aCT). As chemotherapy has many side effects on the short- and long-term, we need to correctly identify the patients who would really benefit from aCT. Multiple demographic and clinical-pathological features are taken into account for aCT recommendation. In addition to these markers, the molecular biology of the tumour is gaining importance in the decision-making through the development of multigene signatures (MGS) tests. These MGS, such as MammaPrint® (MP) and Oncotype DX® (ODX), estimate the risk of recurrence based on the expression of genes in the tumour, and have already proven their clinical utility. However, several factors impede the broad use of these MGS, such as its high cost, the lack of consensus on preselection of a defined target population and the lack of local, decentralised tests that can be integrated in existing workflows in molecular diagnostic laboratories.In this thesis, our general aim was to improve the selection of systemic treatment in patients with ER-positive HER2-negative breast cancer by using prognostic algorithms and specific biomarkers in early and metastatic setting. In the early setting, we retrospectively investigated the administration of aCT in Belgium, we evaluated the impact of MGS in the recommendation of aCT during the multidisciplinary meeting (MDM), and we benchmarked several statistical models that are predictive for MGS outcome to assist clinicians during the MDM discussions whether to perform an MGS.First, we studied the difference in aCT administration in clinical low- and clinical high-risk ER-positive HER2-negative early-stage Belgian breast cancer patients, diagnosed in 2008 versus 2014. In addition, we studied the difference in aCT administration across the Belgian regions (Flemish, Brussels-Capital and Walloon region). We observed a significant reduction in aCT administration for both risk groups when comparing the two periods and were able to confirm this observation for the clinical high-risk patients diagnosed in 2013-2015 versus 2007-2009 at University Hospitals Leuven (UHL). The reduction did not change the 5-year survival in any of the patient groups. Additionally, we observed regional differences in aCT administration in the clinical low-risk group in 2014, with more aCT administration in the Brussels-Capital and Walloon regions versus the Flemish region.The differences in aCT administration observed across Belgian regions illustrates the need for standardised criteria allowing accurate patient selection for aCT and potentially MGS testing. To this end, we evaluated the impact of different MGS tests in assisting decision-making during the MDM for aCT administration in luminal early-stage breast cancer patients with uncertain risk of recurrence based on demographic and clinical-pathological parameters. The integration of MGS results into the MDM recommendations resulted in a decisional switch in 47% of cases and a 9% absolute reduction in aCT administration. However, when we considered each MGS separately, we observed the reduction in the administration of aCT with MP and ODX but not with Prosigna®.Unfortunately, not every country has access to MGS tests as these are quite expensive. Moreover, the analysis in a centralised test laboratory located abroad can prevent MGS use because of privacy regulations. We therefore aimed at increasing patient accessibility to MGS by prospectively validating a targeted RNA-based next-generation sequencing (NGS) kit, MP/BluePrint® (BP), in a decentralised setting. We compared raw data generated by MP/BP NGS at UHL and Curie Institute Paris, with those obtained centrally at Agendia by NGS and by the gold standard microarray technique. We also compared breast cancer subtypes by molecular MP and BP targeted RNA sequencing with immunohistochemistry (IHC). We showed high concordance between risk results obtained at two independent laboratories and the central laboratory at Agendia. We also observed a high concordance between NGS and microarray molecular subtyping, indicating a successful translation of the MP and BP microarray test to the MP and BP NGS test, in a decentralised setting.However, it currently remains unclear which patients benefit most from MGS due to the lack of consensus on preselection of a defined target population. In order to assist the recommendation for MGS testing of the clinicians during the MDM, we aimed to analyse the possibility of preselecting patients for MGS testing. We determined the concordance between the outcomes of existing inexpensive statistical models, developed for predicting the outcome of MGS, and MGS risk outcomes. All cases predicted as being high risk by either the Magee average equation or the breast cancer recurrence score estimator, had a high risk outcome with the MGS. This could result in a 5% reduction in MGS testing. We further investigated the possibility of developing our own predictive model for risk assessment by the MP/BP MGS using machine learning. As the MP/BP MGS is the most widely used in Belgium, preselection of patients through such a model could further assist the selection of patients during the MDM who could benefit from MGS testing. We considered including the risk outcome of existing predictive statistical models based on multiple clinical-pathological features, mainly developed for ODX, into our own predictive model. We also considered using the clinical-pathological features themselves, and the combination of the existing models with the clinical-pathological features into a single model. These three feature sets were tested as input for a new model based on machine learning. Support vector machine (SVM), random forest (RF), linear discriminant analysis (LDA) and decision tree (DT) machine learning models were tested. The best performance was obtained through DT, resulting in accuracies up to 77.8% with a sensitivity of 83.3% (15/18 true high risk) and a specificity of 72.2% (13/18 true low risk). Our model still needs some fine-tuning before it can be validated in a larger cohort. In addition, these results should be tested further to prove its clinical applicability.In the metastatic setting, chemotherapy is not the treatment of choice for patients with luminal breast cancer and is typically only used as a last resort when there are no other options. Cyclin-dependent kinases 4 and 6 (CDK4/6) inhibitors, in combination with endocrine therapy in first or second line of treatment, are currently standard of care in this setting. With the approval by the United States food and drug administration (FDA) and the European medicines agency (EMA) of alpelisib, an α-specific phosphatidylinositol 3-kinase (PI3K) inhibitor which showed benefit in patients with a PIK3CA mutation, testing for these mutations has gained importance. However, in the metastatic setting, a tissue biopsy is not always feasible or available. Therefore, we implemented a highly sensitive droplet digital PCR assay (ddPCR) for the detection of PIK3CA hotspot mutations in circulating cell-free DNA (cfDNA) from plasma. We showed a good performance of ddPCR, especially when 4ml plasma was used in combination with a semi-automated cfDNA extraction method (Maxwell). A good correlation between mutation status obtained by plasma-based ddPCR and tissue-based NGS analysis was obtained, assuming that this technology can be safely used in diagnostic practice when tumour tissue is not available.In conclusion, our results demonstrated the need for standardised criteria to determine aCT administration for luminal early-stage breast cancer patients in Belgium. In addition, we showed that MGS testing assists in therapeutic decision-making, and can reduce aCT administration in clinical high-risk patients. The decentralisation of MGS testing in local laboratories equipped with state-of-the-art technologies for molecular diagnostics can improve access to MGS testing while complying with privacy regulations and reducing the costs of the test. This decentralisation, and the use of inexpensive statistical models predictive for MGS outcome, could further improve the selection for aCT administration and MGS testing in patients with luminal early-stage breast cancer. Finally, we provided evidence for the clinical application of the highly sensitive ddPCR as a useful screening method to detect PIK3CA hotspot mutations in patients with metastatic luminal breast cancer for which no representative tumour tissue is available.
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A significant effort is being made in the identification of prognostic markers to improve the risk stratification of invasive micropapillary breast carcinoma (IMPC). Expression of BCL-2is normally associated an improved overall prognosis. However, it remains unclear whether this applies also to IMPC. Recently, it was observed that tumor-infiltrating lymphocytes (TILs) in IMPC are a negative prognostic influence. The aim of this study is to evaluate the reproducibility in the assessment of BCL-2 expression and stromal TILs measurement in IMPC. Secondly we aim at validate BCL-2 expression and stromal TILs measurement as independent prognostic markers in IMPC. A total of 132 female patients with IMPC were included in the study for retrospective analysis and pathology review was performed on all cases. A tissue micro array (TMA) was created to evaluate the amount of BCL-2 using immunohistochemical staining with an BCL-2 antibody. The results were graded independently by 2 different readers in a semiquantative manner. We also examined these patients on the percentage of TILs by 3 different observers, following the guidelines as set by Salgado et al. Afterwards these results were compared to assess reproducibility of the different scoring system between readers. Subsequently TILs scores were compared to breast cancer surrogate subtypes, Lymphovascular invasion (LVI), perineural invasion (PNI) and tertiary lymphoid aggregates (TLA) status. We observed an excellent correlation between the BCL-2 scores of the 2 readers. We were able to determine that the readers had an ICC of 0.776 on resection specimens (RS) and an ICC of 0.753 on core needle biopsies (CNB). When we compared the TILs scores on a CNB and a RS in the same patient, we found a poor correlation for reader 1 and 2. We did find a good correlation for CNB and RS in reader 3 with an ICC of 0.803. The ANOVA test shows that there is a significant difference in the scores for each breast cancer surrogate subtype with a p-value of 0.026 (α = 0.05). We could not establish a significant difference in TIL scoring for patients with LVI vs. patients without LVI and no significant difference between the patients with PNI and without PNI (p = 0.36). However we did find a significant difference in TIL scores between patients with TLA (19.89%) and the group without TLA (14.65%) with a p value of 0.02. we ascertained a significant correlation between the presence of LVI and the presence of TLA in our patient group In this study we were able to determine BCL-2 staining as a highly reproducible test, independent of the interpreter’s experience level. TILs score was also found to be a reproducible test for RS and CNB, with potential for further research to be done and guidelines to be created about how to standardize TIL grading in IMPC specifically. We found a significant difference in TILs scoring between different breast cancer surrogate subtypes. No significant correlation was found between TILs score and the presence of LVI nor between the TIL score and PNI, however a significant correlation between TIL score and TLA was found. We also observed a strong relationship between the presence of LVI and TLA. The next step will be to evaluate the value of BCL-2 and TILs as independent prognostic factors.
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ABSTRACT Non-Hodgkin lymphoma type marginal zone lymphomas (MZLs) are B-cell lymphomas with an indolent behaviour. Chronic antigen stimulation is a predisposing condition to achieve a MZL, as already reported in patients with chronic infections or autoimmune disorders. This retrospective study focuses on patients with a primary tumor who develop simultaneously or later in time a MZL. Patients with a malignant tumor are also exposed to chronic antigen stimulation, which might be another predisposing factor to develop a MZL. We provide a descriptive overview of patients with a MZL who present with multiple primary malignant tumors (MPMTs) over a period of 15 years. From October 2003 up to October 2018 272 patients were diagnosed with a MZL at our tertiary referral hospital. 86 patients (31.6%) with a MZL had MPMTs, which is much higher compared to the incidence of MPMTs in the general population. 60 patients (22.0%) developed a MZL after an initial primary tumor, of which 22 patients (36.7%) received a diagnosis of MZL in the first 6 months after the primary tumor. Chronic tumor antigen driven stimulation should be considered as a possible inducer of MZL based upon these results, alongside chronic infections and autoimmune disorders.
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Literature review HER2 is known to be overexpressed in approximately 15% to 20% of all breast cancers. To guarantee proper high quality testing in daily clinical practice, ASCO/CAP have developed guidelines. Three different versions have been written since 2007, aiming to generalize and standardize analytical aspects and interpretation of HER2 testing. The Latest version, published in 2018, aims to optimize identification of HER2 positive patients. Although proven to be fit for purpose for identification of this specific subgroup of patients, It remains unclear whether these guidelines are the golden standard for identification of a new group of patient, so called HER-low. Recently,multiple different therapy options have been approved by the FDA for HER2-low patients. The 2018 ASCO/CAP guideline also updated its recommendation regarding FISH reflex testing. Reflex testing for HER2 IHC 3+ cases would no longer be supported by guidelines. Objectives According to recent guidelines published in 2018 by ASCO/CAP, in situ hybridization diagnostic tests with the aim to validate IHC 3+ cases are no longer recommended. These changes imply that pathologists are no longer able to rely on ISH methods to validate their initial evaluation concerning HER2 IHC 3+ cases. Given this paradigmatic switch in the interpretation of the HER2 IHC, research is needed to assess whether current ASCO/CAP guidelines are still fit for purpose to correctly identify this novel category of patients. In this scenario Belgian pathologists will have to be proficient in accurately scoring the lower range of HER2 protein expression and distinguish HER2-LOW patients from HER2 true negative ones. Materials and methods Based on a consensus provided by expert pathologists, we performed a modified Delphi study and Cases able to reach a consensus score were eligible for inclusion in a HER2 training scheme. A training scheme was designed to include 42 cases of which 32 would have to be scored by participants themselves. 61 participants were included in the study. Results Out of 102 total cases scored according to the ASCO/CAP guidelines of 2007 and 2018, in a first round of consensus, experts were able to reach a consensus for 41 and 24 cases respectively. In general we observed a reduction in the size of the HER2 IHC 1+ subgroup when comparing results obtained from both guidelines.. using the ASCO/CAP 2007 guidelines our participants reached an accuracy of 78.9% of all assessments (N=473). Using the ASCO/CAP 2018 guidelines accuracy was found to be 74.1% meaning 1405 out of 1897 cases evaluated using the ASCO/CAP 2018 guidelines were concordant with the consensus score. For both guidelines, scoring accuracy was found to be approaching 100% for HER2 IHC 3+ while scoring accuracy for HER2 LOW was found to be below 80%. Across all cohorts, all assessments and both guidelines, deviating results were found to be dominated by overestimation. Breast pathology experience, familiar primary method/assay of scoring, screen resolution as well as type of laboratory affiliated with participants did no significantly influence obtained data. conclusion While current guidelines have proven to be fit for purpose with the aim of identifying patients to be HER2 positive or negative, using these guidelines to correctly identify HER2 LOW patients will not be desirable due to the extent of discordant results.
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