tissue microarray
در نشریات گروه پزشکی-
Background
Gastric cancer is the fourth leading cause of cancer-related deaths in the world. The identification of gastric cancer subtypes related to recognizable microbial agents may play a pivotal role in the targeted prevention and treatment of this cancer. The current study is conducted to define the frequency of Epstein-Barr virus (EBV) infection in gastric cancers of four major provinces, with different incidence rates of gastric cancers, in Iran.
MethodsParaffin blocks of 682 cases of various types of gastric cancer from Tehran, South and North areas of Iran were collected. Twelve tissue microarray (TMA) blocks were constructed from these blocks. Localization of EBV in tumors was assessed by in situ hybridization (ISH) for EBV-encoded RNA (EBER). Chi-squared test was used to evaluate the statistical significance between EBV-associated gastric cancer (EBVaGC) and clinicopathologic tumor characteristics.
ResultsFourteen out of 682 cases (2.1%) of gastric adenocarcinoma were EBER-positive. EBER was positive in 8 out of 22 (36.4%) of medullary carcinomas and 6 out of 660 (0.9%) of non-medullary type, which was a statistically significant difference (P<0.001). The EBVaGCs were more frequent in younger age (P=0.009) and also showed a trend toward the lower stage of the tumor (P=0.075).
ConclusionEBV-associated gastric adenocarcinoma has a low prevalence in Iran. This finding can be due to epidemiologic differences in risk factors and exposures, and the low number of gastric medullary carcinomas in the population. It may also be related to gastric tumor heterogeneity not detected with the TMA technique.
Keywords: Gastric Cancer, Epstein-Barr Virus, Iran, Tissue Microarray -
Background & Objective
Talin-1 is a constituent of the multiprotein adhesion complexes that play main role in the formation of tumors and migration in different types of malignancies. The present study aimed to assess expression and prognostic significance of the talin-1 protein in ovarian serous carcinoma (OSC) patients.
MethodsThe expression of talin-1 in mRNA and its protein levels were investigated for ovarian cancer (OC) by using bioinformatics tools, including Gene Expression Profiling Interactive Analysis 2 (GEPIA2), Gene Expression Database of Normal and Tumor Tissue 2 (GENT2), and The University of ALabama at Birmingham CANcer data analysis Portal (UALCAN) databases. Thereafter, immunohistochemical (IHC) staining was used to study the expression patterns of the talin-1 protein using 46 paraffin-embedded OSC tissue specimens, 25 benign tumors, and 20 normal tissues, which were assembled in tissue microarrays (TMAs). We also assessed the potential association between the expression of the talin-1 protein, various clinicopathological parameters, and survival outcomes.
ResultsOur IHC examination for talin-1 was significantly overexpressed in OSC tissues compared to benign tumors and normal tissues. The Kaplan-Meier survival analysis has also indicated statistically significant differences in terms of disease-specific survival (DSS) and progression-free survival (PFS) between the patients with high and low expression levels of talin-1, respectively.
ConclusionThe talin-1 protein was overexpressed in OSC tissues, and a high expression level of talin-1 was found to be significantly associated with tumor aggressiveness and poorer DSS or PFS. Therefore, talin-1 may serve as a molecular marker of cancer progression and a novel prognostic biomarker in these patients.
Keywords: Cancer progression, Ovarian serous carcinoma, Prognosis, Talin-1, Tissue microarray -
Background & Objective
Tissue microarray (TMA) is a method of harvesting small tissue cores from a number of donor paraffin tissue blocks and arraying them in a recipient paraffin block. It has numerous advantages and applications but is expensive. This study aimed to develop a simple yet efficient method of manual, small-format TMA block construction.
MethodsDisposable skin punch biopsy needles were used to manually core out 4-mm cylinders from the archival donor blocks comprising tissue from 60 thyroidectomy specimens. These cores were oriented in the embedding cassette in accordance with the grid design. The molten wax was slowly dispensed and allowed to be set. Sectioning, mounting, and hematoxylin and eosin (H&E) staining were performed by a conventional method. Immunohistochemical studies, using HBME-1, CK19, and S100 antibodies, were also performed on these tissue array sections.
ResultsThere was no core loss during processing. Technical issues like core tilt and floatation were easily tackled. Morphological identification, histological typing, and immunohistochemical analysis could be satisfactorily performed in these TMA sections. Donor blocks did not break after punching.
ConclusionThis TMA construction method is simple, feasible, easily reproducible, and time-saving. It can serve as an excellent cost-effective alternative for resource-poor laboratories for carrying out immunohistochemical studies.
Keywords: Core flotation, Core tilt, skin punch biopsy needles, Tissue microarray -
BackgroundThe VEGF is essential in the process of tissue remodeling and angiogenesis. Limited data is available on the expression and regulation of VEGF and its receptors in the human endometrium. The aim of this study was evaluation of expression patterns of VEGF and Flk-1 in human endometrium during the menstrual cycle.MethodsSixty paraffin-embedded blocks of endometrial tissues from the patients with normal menstrual cycles were obtained. Tissue samples were assembled into tissue microarray slides and classified by histological dating into five phases: the proliferative (n=14), peri-ovulatory (n=9), early-secretory (n=12), mid-secretory (n=11) and late-secretory (n=14) phases. Immunohistochemical staining was performed using VEGF or Flk-1 monoclonal antibodies. The intensity of immunostain-ing was evaluated by the semi-quantitative scoring method (HSCORE). Kruskal-Wallis one-way analysis of variance and Scheff’s post-hoc test were used for statistical analysis. A p-value of <0.05 was considered statistically significant.ResultsVEGF and Flk-1 were expressed in the three components of the endometrium at various phases of the menstrual cycle. In the stroma, the expression of VEGF varied among the phases (p<0.05). The expression of Flk-1 in the luminal and glandular epithelium revealed stronger intensity of immunostaining as compared with the stroma at the different phases (p<0.05). The level of Flk-1 expression also showed significant differences among the phases in the glandular epithelium with greatest expression at late-secretory phase (p<0.05).ConclusionTemporal and spatial distribution of VEGF and Flk-1 expression in the three components of human endometrium during menstrual cycle suggests the functional role of angiogenesis in the remodeling process of endometrial tissue.Keywords: Endometrium, Flk, 1, Menstrual cycle, Tissue microarray, VEGF
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سابقه و هدفمننژیوم شایع ترین تومور سیستم عصبی مرکزی است و با توجه به اهمیت بیماری و گزارشی از همراه بودن آن با مارکرهای ki 67 و p 53 و گزارش تنها یک مورد از وضعیت آن در کشور و به منظور تعیین پروگنوز بهتر مننژیوم با استفاده از مارکرهای ki 67 و p53 این تحقیق روی مراجعین بیمارستان شهدای تجریش در سال های 1375 تا 1390 انجام شد.روش بررسیتحقیق با روش مقطعی روی کلیه نمونه های با تشخیص قطعی مننژیوم انجام گرفت. تشخیص قطعی با پاتولوژی بوده و طبقه بندی مننژیوم بر حسب گرید آنها و مطابق با معیار گریدینگ سال 2007 سازمان بهداشت جهانی با روش ریزآرایه بافتی بر روی بلوک های پارافینی انجام گرفت، به این ترتیب که روی تنها یک اسلاید شیشه ای تعداد زیادی از قطعات سوزنی تومورهای با گریدهای مختلف از روی بلوک های پارافینی قرار گرفت و مارکرهای ki67 و p53 با روش ایمونوهیستوشیمی بررسی گردید. میزان رنگ آمیزی دو مارکر بر اساس تعیین درصد سلول های رنگ شده و شدت رنگ آمیزی با مارکر توصیفی بررسی گردید.یافته هااز 89 تومور واجد شرایط، 82/43% گرید یک، 94/44% گرید دو، 37/3% گرید سه، 49/4% گروه مننژیوم با نمای آتیپیک و 37/3% مننژیوم با تهاجم به مغز بودند. میانگین p53 در گرید یک 28/31، در گرید دو 77/57، در گرید سه 60، در مننژیوم با نمای آتیپیک 5/47 و در مننژیوم با تهاجم به مغز 65 بود (087/0=p). در مورد شاخص ki 67، میانگین آن در گرید یک 46/7، در گرید دو 5/33، در گرید سه 5/22، در مننژیوم با نمای آتیپیک 78/10 و در موارد با تهاجم به مغز 20 بود (032/0=p).نتیجه گیریبه نظر می رسد که ارتباطی بین ki 67 و گرید مننژیوم وجود داشته باشد. انجام مطالعات تحلیلی و متعاقب آن بررسی-های تجربی را توصیه می نماییم.
کلید واژگان: مننژیوم، ki 67، p53، تکنیک ریز آرایه بافتیBackgroundMeningioma is the most common CNS tumor; association of this tumor with specific markers P53، Ki67 has been reported in some studies. This study was done with the aim of determining the frequency of these markers in patients presenting with meningioma in a teaching hospital in Tehran.Materials And MethodsThis cross-sectional study was done on samples obtained from all patients operated for meningioma in Shohadae Tajrish Hospital from 1996 to 2011. Meningiomas were graded in accordance with the WHO grading system. This method was performed by tissue microarray on paraffin embedded blocks of the samples; several pin-size samples were placed on a single glass slide and immune-histo-chemistry study was done for Ki67 and P53 markers.ResultsStudy done on 89 paraffin embedded blocks of meningiomas revealed that 43. 82% were grade 1، 44. 94% grade 2، 3. 37% grade 3، and 4. 49% of meningiomas had atypical features while 3. 37% had invaded the brain. Expression of P53 was seen in 31. 28% of meningiomas in grade 1، 57. 77% in grade 2، 60% in grade 3، 47. 5% in tumors with atypical features and in 65% of tumors invading the brain (P= 0. 087(. Expression of Ki67 was observed in 7. 46% of grade 1، 33. 5% of grade 2، 22. 5% of grade 3، 10. 78% of meningiomas with atypical features and 20% of tumors invading the brain (P= 0. 032).ConclusionIt seems that there is a relationship between the grade of meningiomas and expression of Ki67 in tumor cells.Keywords: Meningioma, Ki67, P53, Tissue microarray
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