17 research outputs found
Primary Cutaneous Apocrine Carcinoma of Sweat Glands: A Rare Case Report
Cutaneous apocrine gland carcinoma, a subtype of sweat gland carcinoma, is a very rare malignancy, and only few cases have been reported in the literature. Many of these carcinomas are indolent and slowly developing, but some are rapidly progressive. The treatment of choice is wide local excision with clear margins, with or without lymph node dissection. We report a case of a 67-year-old man who came to our hospital with an ulcerated nodule in the right axilla measuring 1 × 0.8 cm. Histological evaluation showed features of an apocrine gland carcinoma arising in an area of high apocrine gland density
Synchronous Primary Adenocarcinoma and Ancient Schwannoma in the Colon: An Unusual Case Report
Gastrointestinal schwannomas are uncommon stromal tumors of the intestinal tract and colon schwannomas are extremely rare. We report a rare case of ascending colon schwannoma with associated synchronous adenocarcinoma of the sigmoid colon. A 68-year-old man presented with a 20-day history of bleeding per rectum. Colonoscopy revealed a mass of 4.2 cm in diameter with endoluminal protrusion in the sigmoid colon and a second submucosal tumor in the ascending colon. Surgical intervention was suggested and ileo-hemicolectomy was done. Microscopically, the submucosal tumor of 4 cm in diameter showed features of schwannoma with degenerative change (ancient schwannoma). Lesional cells were positive for S100p and negative for actin, desmin, CD34, CD117, and pankeratin. The mass showed features of an invasive moderately differentiated adenocarcinoma. Colon schwannoma is a rare submucosal tumor, and the incidental occurrence with adenocarcinoma has not been well described in the literature
Assessment of algorithms for mitosis detection in breast cancer histopathology images
The proliferative activity of breast tumors, which is routinely estimated by counting of mitotic figures in hematoxylin and eosin stained histology sections, is considered to be one of the most important prognostic markers. However, mitosis counting is laborious, subjective and may suffer from low inter-observer agreement. With the wider acceptance of whole slide images in pathology labs, automatic image analysis has been proposed as a potential solution for these issues.
In this paper, the results from the Assessment of Mitosis Detection Algorithms 2013 (AMIDA13) challenge are described. The challenge was based on a data set consisting of 12 training and 11 testing subjects, with more than one thousand annotated mitotic figures by multiple observers. Short descriptions and results from the evaluation of eleven methods are presented. The top performing method has an error rate that is comparable to the inter-observer agreement among pathologists
Pathological non-response to chemotherapy in a neoadjuvant setting of breast cancer: an inter-institutional study
To identify markers of non-response to neoadjuvant chemotherapy (NAC) that could be used in the adjuvant setting. Sixteen pathologists of the European Working Group for Breast Screening Pathology reviewed the core biopsies of breast cancers treated with NAC and recorded the clinico-pathological findings (histological type and grade; estrogen, progesterone receptors, and HER2 status; Ki67; mitotic count; tumor-infiltrating lymphocytes; necrosis) and data regarding the pathological response in corresponding surgical resection specimens. Analyses were carried out in a cohort of 490 cases by comparing the groups of patients showing pathological complete response (pCR) and partial response (pPR) with the group of non-responders (pathological non-response: pNR). Among other parameters, the lobular histotype and the absence of inflammation were significantly more common in pNR (p < 0.001). By ROC curve analyses, cut-off values of 9 mitosis/2 mm(2) and 18 % of Ki67-positive cells best discriminated the pNR and pCR + pPR categories (p = 0.018 and < 0.001, respectively). By multivariable analysis, only the cut-off value of 9 mitosis discriminated the different response categories (p = 0.036) in the entire cohort. In the Luminal B/HER2- subgroup, a mitotic count < 9, although not statistically significant, showed an OR of 2.7 of pNR. A lobular histotype and the absence of inflammation were independent predictors of pNR (p = 0.024 and < 0.001, respectively). Classical morphological parameters, such as lobular histotype and inflammation, confirmed their predictive value in response to NAC, particularly in the Luminal B/HER2- subgroup, which is a challenging breast cancer subtype from a therapeutic point of view. Mitotic count could represent an additional marker but has a poor positive predictive value
A multicentre validation of Metasin: a molecular assay for the intraoperative assessment of sentinel lymph nodes from breast cancer patients
Aims:
Treatment strategies for breast cancer continue to evolve. No uniformity exists in the UK for the management of node‐positive breast cancer patients. Most centres continue to use conventional histopathology of sampled sentinel lymph nodes (SLNs), which requires delayed axillary clearance in up to 25% of patients. Some use touch imprint cytology or frozen section for intraoperative testing, although both have inherent sensitivity issues. An intraoperative molecular diagnostic approach helps to overcome some of these limitations. The aim of this study was to assess the clinical effectiveness of Metasin, a molecular method for the intraoperative evaluation of SLNs.
Methods and results:
RNA from 3296 lymph nodes from 1836 patients undergoing SLN assessment was analysed with Metasin. Alternate slices of tissue were examined in parallel by histology. Cases deemed to be discordant were analysed by protein gel electrophoresis. There was concordance between Metasin and histology in 94.1% of cases, with a sensitivity of 92% [95% confidence interval (CI) 88–94%] and a specificity of 97% (95% CI 95–97%). Positive and negative predictive values were 88% and 98%, respectively. Over half of the discordant cases (4.4%) were ascribed to tissue allocation bias (TAB).
Conclusions:
Clinical validation of the Metasin assay suggests that it is sufficiently sensitive and specific to make it fit for purpose in the intraoperative setting
p63 expression in benign and malignant breast lesions
The p63 gene encodes six protein isoforms.
The transactivating isoforms have similar actions with
p53, while the N-isoforms inhibit transcription activation
by p53 and transactivating isoforms. p63 is expressed in
stratified epithelia and in basal cells of the prostate and
salivary glands. In mammary epithelium p63 has been
shown to be expressed only in the myoepithelial layer. In
the present study we investigated the immunohistochemical
expression of p63, in benign and
malignant breast lesions, and compared it with known
myoepithelial cell markers. Our material consisted of
140 benign and 126 malignant breast lesions. We used
the antibodies anti-p63, anti-a-smooth muscle actin,
anti-S-100 protein and anti-cytokeratin 14. In all benign
lesions, p63 immunoreactivity was noted in the
myoepithelial cell layer surrounding the luminal
epithelial cells. A less continuous peripheral rim of
myoepithelial cells was also highlighted with p63-
staining in all situ carcinomas. All invasive breast
carcinomas were devoided of peripheral p63 staining.
Interestingly, strong nuclear p63 immunoreactivity was
noted in a small fraction (5-15%) of epithelial cells in all
cases of papillomatosis, in 62.5% of in situ ductal
papillary-type carcinomas and in 33.3% of invasive
papillary carcinomas. Comparable staining was observed
with S-100. The stromal cells were unreactive to p63.
Our findings suggest that p63 is a sensitive and specific
myoepithelial marker, and may be included in
immunohistochemical panels aiming to identify
myoepithelial cells in problematic breast lesions.
Regarding papillary neoplasms, it is possible that tumor
cells acquire and exhibit at least in part a myoepithelial
differentiation program
Expression of vascular endothelial growth factor (VEGF) and association with microvessel density in small-cell and non-small-cell lung carcinomas
Recent studies have demonstrated that tumor
angiogenesis is a prognostic factor for various malignant
neoplasms. Specifically, in non-small-cell lung
carcinomas (NSCLCs) most reports show an association
between neovascularization and vascular endothelial
growth factor (VEGF) expression as well as the presence
of metastases and survival, although a few reports do not
agree with these findings. Angiogenesis is not clearly
characterized in small-cell lung carcinomas (SCLCs),
since they are rarely treated by surgery, and thus the
available tissue for biological characterization is sparse.
The aim of the present study was to investigate
angiogenesis and the expression of VEGF in lung
tumors. We examined 88 non-small-cell and 39 smallcell
lung carcinomas. Angiogenesis was estimated by
determining microvessel counts, with the use of anti-
CD31 and anti-factor VIII antibodies and expression of
VEGF was also evaluated immunohistochemically. Our
data showed that in NSCLCs angiogenesis was more
prominent in poorly-differentiated neoplasms and
correlated with VEGF expression, therefore it is at least
in part mediated by the latter. Interestingly, in SCLCs a
higher vascularization was noted. However, there was no strong association with VEGF expression. Thus, smallcell
lung carcinoma may represent a suitable neoplasm
for testing antiangiogenic drugs in combination with
chemotherapy. Nevertheless, antiangiogenic therapy
should not be targeted specifically to the VEGF pathway,
since in SCLCs other mediators of angiogenesis may be
important as well