Purpose: Early breast cancer presents with a remarkable heterogeneity of outcomes.Undetected, microscopic lymph node tumor deposits may account for a significant fraction of this prognostic diversity. Thus, we systematically evaluated the presence of lymph node tumor cell deposits V0.2 mm in diameter [pN 0(i+) , nanometastases] and analyzed their prognostic effect. Experimental Design: Single-institution, consecutive patients with 8 years of median follow-up (n = 702) were studied. To maximize chances of detecting micrometastases and nanometastases, whole-axilla dissections were analyzed. pN 0 cases (n = 377) were systematically reevaluated by lymph node (n = 6676) step-sectioning and anticytokeratin immunohistochemical analysis. The risk of first adverse events and of distant relapse of bona fide pN 0 patients was compared with that of pN 0(i+) , pN 1mi , and pN 1 cases. Results: Minimal lymph node deposits were revealed in 13% of pN 0 patients.The hazard ratio for all adverse events of pN 0(i+) versus pN 0(iÀ) was 2.51 (P = 0.00019). Hazards of pN 1mi and pN 0(i+) cases were not significantly different. A multivariate Cox model showed a hazard ratio of 2.16 for grouped pN 0(i+) /pN 1mi versus pN 0(iÀ) (P = 0.0005). Crude cumulative incidence curves for metastatic relapse were also significantly different (Gray's test m 2 = 5.54, P = 0.019). Conclusion: Nanometastases are a strong risk factor for disease-free survival and for metastatic relapse. These findings support the inclusion of procedures for nanometastasis detection in tumor-node-metastasis staging.The tumor-node-metastasis (TNM) staging system for breast cancer (1) has proven invaluable in categorizing the extent of neoplastic disease, and as a basis to estimate prognosis and to direct treatment (2). However, this has not lead to the definition of tightly homogeneous prognostic classes, as considerable heterogeneity of outcomes can be observed among disease cases currently categorized as similar. This is particularly evident in the case of small breast tumors (2). We argued that a diverse extent of lymph node dissemination at early stages of disease may account for diverse disease recurrence dynamics. The principle that the macroscopic burden of metastatic cells (e.g., number of invaded lymph nodes) dictates different risks of disease recurrence has been recognized (1,3). This principle might be equally important at the low end of the spectrum, i.e., in the case of microscopic tumor cell deposits (1, 4).Serial sectioning coupled to immunohistochemical analysis has considerably improved the detection of small tumor cell clusters in lymph nodes (5 -10). Occult metastases can indeed be identified in up to 30% of cases previously classified as pN 0 (7 -9), in 14% to 20% of the cases by single lymph node sections (9, 10). Studies based on these procedures have shown that axillary lymph node microinvasion is a prognostic factor for breast cancer patients, and is associated with poorer diseasefree and overall survival (7, 8, 11 -13). As a consequenc...
Implementation of a multidisciplinary thoracic malignancy conference increased the 1-year survival rate of patients who underwent a surgical resection for NSCLC.
Aims-To determine cell proliferation in infiltrating breast carcinomas. Methods-Using the MIB-1 monoclonal antibody, the proliferation index was measured in paraffin wax sections of 871 breast cancers. The MIB-1 proliferation index was compared with other markers of disease progression: size, lymph node status, histotype, oestrogen and progesterone receptor status, expression of p53 and Neu, and DNA ploidy. AUl parameters were measured using image analysis. In 347 tumours, the MIB-1 and Ki-67 proliferation indexes were compared. Follow up data were available for 170 cases (median 66.5 months). Results-Of the tumours, 314 (36%) had a high proliferation index. The MIB-1 proliferation index was correlated directly with size, nodal status, overexpression of p53 and Neu, and the DNA index; and inversely with oestrogen and progesterone receptor status. The correlation between MIB-1 and Ki-67 proliferation indexes was statistically significant. In patients with pT1 tumours, a low proliferation index correlated with a longer relapse-free interval and overall survival; node negative patients with a low proliferation index had a longer overall survival. Conclusions-The MIB-1 proliferation index is a reliable, practical and useful method ofmeasuring proliferative activity and is an important predictor of clinical behaviour. ( Clin Pathol 1996;49:926-930) Keywords: breast cancer, MIB-1, proliferative activity, image analysis, overall survival.Use of immunocytochemistry to measure tumour proliferation preserves both cytological and architectural features and can be used to detect proliferation related nuclear antigens, one of the most important of which is Ki-67. The Ki-67 nuclear antigen is expressed by dividing cells in all phases of the cell cycle except Go 1 and has been established as an independent prognostic marker in breast cancer. Unfortunately, detection of Ki-67 is limited to frozen tissue only. However, several antibodies are available for quantifying cell proliferation in paraffin wax embedded specimens, including antibodies directed against proliferating cell nuclear antigen (PCNA) and the Ki-Sl and MIB-1 monoclonal antibodies."'' MIB-1, in particular, recognises Ki-67 nuclear antigen, permitting the assessment of growth fraction on small tumours, formalin fixed tissue and retrospective studies on archival material.The aim of the present study was to measure the MIB-1 proliferation index in 871 infiltrating breast carcinomas. The results were compared with other markers of prognosis: oestrogen and progesterone receptor status, overexpression of c-erbB-2/Neu and p53, the DNA index, and the Ki-67 proliferation index. The clinical usefulness of the MIB-1 proliferation index was also evaluated in 170 patients (median follow up 66.5 months). MethodsParaffin wax blocks of 871 infiltrating primary breast cancers were retrieved from the archives. The clinicopathological details of the patients studied are presented in table 1. The mean age of the patients was 61 years; 277 (31.8%) were pre-menopausal and 507...
Biological Profile of in Situ Breast Cancer Investigated by Immunohistochemical Technique
In 74 in situ breast cancers an immunohistochemical study for estrogen (ER) and progesterone (PR) receptors, proliferation index (PI), and c-erbB-2, p53, and bcl-2 overexpression was performed. Cases were categorized as ductal carcinoma in situ (DCIS) comedo: 24.3% of cases; DCIS non comedo: 27% of cases; DCIS cribriform: 5.4% of cases; lobular carcinoma in situ (LCIS): 16.3% of cases; mixed carcinoma in situ: 27% of cases. Quantitation of immunohistochemical results was obtained with an image analysis computerized system (CAS 200). The cutoff values used were: 10% of positive area for ER, PR, NEU, and bcl-2; 5% of positive area for p53; 13% of PI for proliferative activity. DCIS cribriform and LCIS displayed a higher positivity for ER (92.6 and 93.8% of cases); DCIS cribriform and DCIS non comedo a higher for PR (89 and 75.3%); DCIS comedo presented the highest values for PI (65.4%), NEU (72.8%), and p53 expression (37.3%). All DCIS cribriform and DCIS non comedo and 99.6% of LCIS expressed bcl-2. The results underscore the importance of biological characterization of breast carcinoma in situ with the aim to define lesions natural history.
Background:In primary breast cancers dichotomic classification of E-cadherin expression, according to an arbitrary cutoff, may be inadequate and lead to loss of prognostic significance or contrasting prognostic indications. We aimed to assess the prognostic value of high and low E-cadherin levels in a consecutive case series (204 cases) of unilateral node-negative non-lobular breast cancer patients with a 8-year median follow-up and that did not receive any adjuvant therapy after surgery.Methods:Expression of E-cadherin was investigated by immunohistochemistry and assessed according to conventional score (0, 1+, 2+, 3+). Multiple correspondence analysis was used to visualise associations of both categorical and continuous variables. The impact of E-cadherin expression on patients outcome was evaluated in terms of event-free survival curves by the Kaplan–Meier method and proportional hazard Cox model.Results:Respect to intermediate E-cadherin expression values (2+), high (3+) or low (0 to 1+) E-cadherin expression levels had a negative prognostic impact. In fact, both patients with a low-to-nil (score 0 to 1+) expression level of E-cadherin and patients with a high E-cadherin expression level (score 3+) demonstrated an increased risk of failure (respectively, hazard ratio (HR)=1.71, confidence interval (CI)=0.72–4.06 and HR=4.22, CI=1.406–12.66) and an interesting association with young age.Conclusions:The findings support the evidence that high expression values of E-cadherin are not predictive for a good prognosis and may help to explain conflicting evidence on the prognostic impact of E-cadherin in breast cancer when assessed on dichotomic basis.
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