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2. Grading of invasive breast carcinoma: the way forward

Author

C, van Dooijeweert, P J, van Diest, and I O, Ellis

Subjects
Pathologists, Artificial Intelligence, Humans, Mitosis, Reproducibility of Results, Breast Neoplasms, Female, Neoplasm Grading
Abstract

Histologic grading has been a simple and inexpensive method to assess tumor behavior and prognosis of invasive breast cancer grading, thereby identifying patients at risk for adverse outcomes, who may be eligible for (neo)adjuvant therapies. Histologic grading needs to be performed accurately, on properly fixed specimens, and by adequately trained dedicated pathologists that take the time to diligently follow the protocol methodology. In this paper, we review the history of histologic grading, describe the basics of grading, review prognostic value and reproducibility issues, compare performance of grading to gene expression profiles, and discuss how to move forward to improve reproducibility of grading by training, feedback and artificial intelligence algorithms, and special stains to better recognize mitoses. We conclude that histologic grading, when adequately carried out, remains to be of important prognostic value in breast cancer patients.

Published
2021

3. Tumor Infiltrating T Lymphocytes and Apoptosis in Colorectal Cancer

Author

Manal M S, Youssef, Emma C, Paish, J Clifford, Murray, Naglaa M, Farag, Khaled, Saleh, and I O, Ellis

Subjects
Male, Lymphocytes, Tumor-Infiltrating, T-Lymphocytes, In Situ Nick-End Labeling, Humans, Apoptosis, Female, Kaplan-Meier Estimate, Middle Aged, Colorectal Neoplasms, Immunohistochemistry, Aged
Abstract

Dysfunction of the immune system in colorectal cancer (CRC) can be due to a number of reasons including apoptosis of tumour infiltrating lymphocytes (TILs). The aims of this study was to investigate TILs in colorectal cancer and characterize apoptosis of TILs using terminal deoxynucleotidyl transferase dUTP nick end labeling (TUNEL) assay for detecting DNA fragments. We used monoclonal antibodies (mAbs) to T lymphocytes to detect TILs and double immunohistochemistry to assess apoptosis. T lymphocytes were detected in the immune infiltrate in CRC. TUNEL staining disclosed a high level of cell death among TILs. Apoptosis of T lymphocytes showed significant correlation with Dukes' stage (P = 0.02), lymphatic metastasis (P = 0.03), vascular metastasis (P = 0.01), lymph node metastasis (P = 0.02) and age of patient (P = 0.01). In conclusion, CRC may elude immunological surveillance by inducing apoptosis of TILs.

Published
2015

4. Apoptosis of T-cell subsets in colorectal cancer in vivo

Author

Manal M S, Youssef, Emma C, Paish, J Clifford, Murray, Naglaa M, Farag, Khaled, Saleh, and I O, Ellis

Subjects
Male, Caspase 3, T-Lymphocyte Subsets, Humans, Leukocyte Common Antigens, Apoptosis, Female, Neoplasm Metastasis, Colorectal Neoplasms, Neoplasm Proteins, Retrospective Studies
Abstract

Dysfunction of the immune system in colorectal cancer (CRC) can be due to a number of reasons including apoptosis of tumour infiltrating lymphocytes (TILs). The aims of this study were to characterize, phenotypically, the apoptosis of TILs in CRC, and define the association of these findings with prognostic indicators. We used double immunohistochemistry to assess the apoptosis of T-cell subsets. Monoclonal antibodies to T lymphocytes, T helper cells, cytotoxic T cells (CTLs), natural killer cells (NK), CD45 and CD45RO were used. Antibodies against cleaved caspase-3 as a marker of apoptosis were used. Apoptosis of T-cell subsets was detected in the immune infiltrate in CRC. Apoptosis of T lymphocytes showed significant correlation with lymphatic metastasis (P = 0.01), Dukes' stage (P = 0.019). Apoptotic T helper cells showed significant correlation with metastasis (P = 0.04), lymphatic metastasis (P = 0.02), death (P = 0.04) and recurrence (P = 0.04). For apoptosis of CTLs, there was a significant correlation with histological classification (P = 0.02), lymphatic metastasis (P = 0.04), vascular metastasis (P = 0.03) and lymph node metastasis (P = 0.04). A significant association was found between the apoptosis of NK cells and the histological classification (P = 0.04). A significant association was found between the apoptosis of cd45RO cells and the histological classification (P = 0.04). In conclusion, apoptosis of lymphocytes provides theoretical foundation for metastasis and counterattack of colon cancer.

Published
2015

5. Invasive breast carcinoma of no special type.

Author

E. A., Rakha, S., Masuda, K. H., Allison, F., Penault-Uorca, H., Bu, S. J., Schnitt, I. O., Ellis, H., Tsuda, M. P., Foschini, R., Horii, A., Vincent-Salomon, and W. T., Yang

Published
2019

7. E-cadherin as a prognostic indicator in primary breast cancer

Author

C Parker, R S Rampaul, S E Pinder, J A Bell, P M Wencyk, R W Blamey, R I Nicholson, J F R Robertson, and I O Ellis

Subjects
Adult, Cytoplasm, Cancer Research, Pathology, medicine.medical_specialty, Mammary gland, Breast Neoplasms, Biology, Cohort Studies, Immunoenzyme Techniques, Mice, Breast cancer, Predictive Value of Tests, Risk Factors, Biomarkers, Tumor, Carcinoma, medicine, Animals, Humans, Life Tables, Lymph node, Survival analysis, Aged, Retrospective Studies, Paraffin Embedding, Cell adhesion molecule, Cadherin, Antibodies, Monoclonal, Cancer, Regular Article, Middle Aged, Cadherins, Prognosis, medicine.disease, Survival Analysis, Neoplasm Proteins, cadherin, medicine.anatomical_structure, Oncology, immunohistochemistry, Cancer research, Female
Abstract

Epithelial cadherin (E-CD) is a member of the cadherin family of cell adhesion molecules and has been implicated as an invasion suppressor molecule in vitro and in vivo. We analysed 174 breast tumours from the Nottingham/Tenovus Breast Cancer Series immunohistochemically for E-CD expression using the mouse monoclonal antibody HECD-1 (Zymed Laboratories Inc.). In normal epithelial cells E-CD was strongly expressed at cell–cell boundaries. 66% of the breast cancers examined had reduced intensity of E-CD expression with 74% having significant reductions in the proportion of E-CD-positive tumour cells. Using a combined intensity/proportion score, significant associations were found between E-CD expression and tumour type (P ≤ 0.001). ER status (P = 0.026) and histological grade (P = 0.031). Expression of E-CD was not found to be related to recurrence, distant metastases, lymph node stage, vascular invasion, primary tumour size, prognostic group or survival. Thus E-CD expression in human breast cancer appears to have minimal prognostic value, but may have a role as a phenotypic marker. © 2001 Cancer Research Campaign http://www.bjcancer.com

Published
2001
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8. Sir Peter Freyer Memorial Lecture and Surgical Symposium 15th and 16th September, 1995

Author

J. Calleary, C. Tansey, J. McCormack, S. Kapur, J. Doyle, J. Flynn, A. J. Curran, D. Smyth, B. Kane, M. Toner, C. V. I. Timon, K. J. Cronin, J. O’Donoghue, F. X. Darmanin, J. McCann, F. Campbell, H. P. Redmond, C. Condron, D. Bouchier-Hayes, K. Aizaz, S. W. MacGowan, A. F. O’Donnell, D. A. Luke, E. McGovern, M. Morrin, F. Khan, P. V. Delaney, S. M. Lavelle, B. Kanagaratnam, V. Cuervas-Mons, A. Gauthier, C. Gips, R. Marques dos Santos, G. P. Molino, A. Theodossi, D. D. Tsiftsis, C. J. O. Boyle, T. J. Boyle, M. J. Kerin, D. M. Courtney, D. S. Quill, H. F. Given, D. F. O’Brien, E. J. Kelly, J. Kelly, D. Richardson, N. F. Fanning, R. Brennan, P. G. Horgan, F. B. V. Keane, S. Reid, C. Walsh, R. Patock, J. Hall, D. Evoy, M. Magd-Eldin, D. Curran, P. Keeling, N. Ade-Ajayi, L. Spitz, E. Kiely, D. Drake, N. Klein, D. M. O’Hanlon, D. Karat, K. Callanan, W. Crisp, S. M. Griffin, P. M. Murchan, B. Mancey-Jones, P. Sedman, C. J. Mitchell, J. Macfie, D. Scott, S. Raimes, C. J. O’Boyle, D. Maher, P. C. Willsher, J. F. R. Robertson, M. Hilaly, R. W. Blarney, S. G. Shering, S. Mitrovic, A. Rahim, E. W. McDermott, N. J. O’Higgins, C. A. Murphy, D. Morgan, C. W. Elston, I. O. Ellis, M. P. O’Sullivan, M. G. O’Riordain, J. P. Stack, M. K. Barry, J. T. Ennis, J. M. Fitzpatrick, T. F. Gorey, J. Kollis, H. Mullet, D. F. Smith, A. Zbar, M. J. Murray, E. W. M. McDermott, P. P. A. Smyth, N. Kapucouglu, S. Holmes, P. Holland, P. T. McCollum, A. da Silva, L. de Cossart, D. Hamilton, C. J. Kelly, K. Stokes, P. Broe, J. Crinnion, P. A. Grace, N. Morton, N. Ross, S. Naidu, P. Gervaz, R. J. Holdsworth, P. A. Stonebridge, A. O’Donnell, K. Carson, D. Phelan, S. McBrinn, D. McCarthy, H. Javadpour, J. McCarthy, M. Neligan, M. T. P. Caldwell, J. P. McGrath, P. J. Byrne, T. N. Walsh, P. Lawlor, C. Timon, R. C. Stuart, K. Murray, A. Carney, J. G. Johnston, B. Egan, P. R. O’Connell, J. Donoghue, A. Pollock, D. Hyde, D. Hourihan, W. A. Tanner, J. Donohue, N. Fanning, P. Horgan, A. Mahmood, K. Dave, J. Stewart, A. Cole, R. Hartley, T. G. Brennan, J. M. O’Donoghue, S. T. O’Sullivan, E. Beausang, J. Panchal, M. O’Shaughnessy, P. O’Grady, R. W. G. Watson, D. Johnstone, J. O’Donnell, E. McCarthy, N. Flynn, T. O’Dwyer, C. Curran, S. Duggan, S. Tierney, Z. Qian, P. A. Lipsett, H. A. Pitt, K. D. Lillemoe, J. Kollias, D. A. L. Morgan, I. S. Young, M. C. Regan, J. G. Geraghty, C. B. O. Suilleabhain, M. L. Rodrick, A. F. Horgan, J. A. Mannick, J. A. Lederer, T. P. J. Hennessy, M. Canney, K. Feeley, C. E. Connolly, H. Abdih, N. Finnegan, M. Da Costa, M. Shafii, A. J. Martin, D. Mulcahy, M. Dolan, M. Stephens, F. McManus, M. Walsh, D. P. O’Brien, J. P. Phillips, T. A. Carroll, D. O’Brien, D. Rawluk, T. Sullivan, K. Herbert, M. Kerins, M. O’Donnell, D. Lawlor, M. McHugh, G. Edwards, J. Rice, J. P. McCabe, J. Sparkes, S. Hayes, M. Corcoran, H. Bredin, D. O’Keeffe, J. Candon, E. D. Mulligan, T. H. Lynch, D. Mulvin, L. Vingers, J. M. Smith, H. Corby, K. Barry, I. Eardley, J. Frick, B. Goldwasser, P. Wiklund, E. Rogers, R. Weaver, P. T. Scardino, R. Kumar, P. Puri, A. B. Adeyoju, T. Lynch, J. Corr, T. E. D. McDermott, R. Grainger, J. Thornhill, M. Butler, D. Keegan, N. Hegarty, P. McCarthy, A. H. Mirza, M. O’Sullivan, P. Neary, T. P. F. O’Connor, D. McCormack, K. Cunningham, N. Cassidy, K. Mulhall, M. Murphy, A. Puri, B. Dhaif, P. D. Carey, R. J. Delicata, F. Abbasakoor, R. B. Stephens, A. J. Hussey, B. Garrihy, D. J. Nolan, O. J. McAnena, R. Fitzgerald, D. Watson, B. J. Coventry, P. Malycha, S. C. Ward, S. P. Y. Kwok, W. Y. Lau, J. W. Bergman, G. E. B. Hacking, C. Metreweli, A. K. C. Li, P. Madhavan, J. Donohoe, M. O’Donohue, D. A. McNamara, and M. K. O’Donohoe

Subjects
business.industry, Medicine, General Medicine, business, Classics
Published
1995
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9. Hypoxia-induced EMAP-II transcription in colorectal cancer

Author

Manal M S, Youssef, Yee M, Heng, Desmond G, Powe, Jodie, Edgson, I O, Ellis, and Clifford, Murray

Subjects
Transcription, Genetic, Apoptosis, Adenocarcinoma, Lymphocyte Activation, Cell Hypoxia, Up-Regulation, Cell Line, Tumor, Human Umbilical Vein Endothelial Cells, Humans, Lymphocytes, RNA, Messenger, Mitogens, Colorectal Neoplasms, HT29 Cells, Microtubule-Associated Proteins
Abstract

Endothelial monocyte-activating polypeptide-II (p431EMAP-II) is a proinflammatory cytokine and a chemoattractant for mononuclear phagocytes and polymorphonuclear leucocytes, found in culture supernatants of many tumour cell lines. It was demonstrated that p43/EMAP-II induces apoptosis in mitogen-stimulated lymphocytes, and suggested that it may be a constituent of a novel immune evasion mechanism employed by tumour cells. Quantitative real-time reverse transcription- polymerase chain reaction (qRT-PCR) analysis for EMAP-II mRNA was performed for colorectal adenocarcinoma cell lines, DLD-1, HT 29; human umbilical vein endothelial cells (HUVEC); and normal colon under normal and hypoxic conditions. Under hypoxic conditions, EMAP-II transcript expression increased up to 22-fold over normoxia in tumour cells, while there was 1-fold increase due to hypoxia in HUVEC and no increase in normal colon. These results demonstrate that EMAP-II transcripts are upregulated in tumour cells in hypoxic conditions and support the notion that EMAP-II plays a complex and important role in human cancer.

Published
2012

10. Seventeenth Sir Peter Freyer memorial lecture and surgical symposium

Author

E. O’Broin, J. Donohoe, K. Mealy, M. Kerin, P. Gillen, W. A. Tanner, F. B. V. Keane, P. McCarthy, S. Rubesin, H. Herlinger, I. Laufer, M. T. P. Caldwell, P. Lawlor, P. J. Byrne, T. N. Walsh, T. P. J. Hennessy, A. J. Curran, P. Gormley, K. Barry, M. McGuire, P. Marks, A. Syed Asad, B. Lane, H. I. Browne, P. Keeling, M. K. Barry, C. J. Yeo, P. K. Sauter, K. D. Lillemoe, H. A. Pitt, J. L. Cameron, S. Sostre, D. A. O’Donovan, C. J. Kelly, D. M. Bouchier-Hayes, H. P. Redmond, P. Burke, W. S. Monkhouse, J. Burke, N. Williams, T. Gorey, N. H. Afdhal, A. I. Butt, M. H. Vazir, R. Sullivan, C. E. Connolly, H. C. Bredin, J. P. Sweeney, D. Greene, R. Harkin, J. Thornton, M. R. Butler, T. E. D. McDermott, R. Grainger, J. Thornhill, M. J. Kerin, J. Wilkie, J. R. T. Monson, S. Duggan, J. McCarthy, R. G. W. Watson, D. T. Croke, M. McDermott, D. Croke, P. B. V. Keane, R. W. G. Watson, R. O’Donnell, A. F. Horgan, D. S. O’Riordain, I. Saporoschetz, J. A. Mannick, M. L. Rodrick, D. M. Baker, J. A. Jones, J. S. Nguyen-Van-Tam, D. L. Morris, J. D. Hardcastle, R. J. C. Steele, J. B. Bourke, J. H. Lloyd, S. Brown, S. E. A. Attwood, J. McGrath, M. Regan, S. McCann, R. B. Stephens, A. T. Devitt, T. J. O’Sullivan, B. J. Hurson, M. C. Regan, M. Hurson, S. J. Kirk, H. L. Wasserkrug, A. Barbul, E. R. Naidu, Tracy Sullivan, M. Colreavy, S. Kaf Al-Ghazal, J. McCann, M. Rodrick, K. J. Cronin, P. Butler, M. McHugh, G. Edwards, J. G. Geoghegan, D. J. Hehir, W. O. Kirwan, M. P. Brady, J. A. O’Donnell, D. Evoy, S. T. O’Sullivan, C. M. Reardon, M. A. Stokes, F. Bergin, P. Mercer, D. Murphy, N. O’Higgins, P. M. Cannon, J. F. R. Robertson, I. O. Ellis, R. W. Blarney, D. L. Manning, R. I. Nicolson, E. Mulligan, P. Kent, J. Ennis, M. Dowling, P. Dervan, J. M. Fitzpatrick, T. F. Gorey, D. M. Sibbering, M. H. Galea, D. A. L. Morgan, A. P. Locker, C. W. Elston, R. W. Blamey, S. P. M. Cannon, S. O’Rourke, M. Galea, A. Evans, I. Ellis, S. Johnston, J. Byrne, P. Horgan, M. Kennedy, J. Callaghan, H. F. Given, E. Mooney, S. Donohue, D. M. O’Hanlon, R. Waldron, J. Johnston, M. Stokes, E. MeDermott, M. Sharp, M. Duffy, J. Murphy, G. T. McGreal, W. Kealy, M. Neligan, K. O’Malley, G. McEntee, F. Khan, M. Morrin, P. Delaney, N. Brindley, S. Dudeney, J. Drebin, J. Geraghty, P. Broe, M. Fynes, P. G. Horgan, P. R. O’Connell, B. Golden, F. Loughnane, S. Baldota, M. O’Donnell, S. Chen, P. W. Eustace, J. G. Johnston, T. Gaffney, S. El Tawil, F. Cunningham, E. Brazil, J. Reynolds, A. Ireland, O. Traynor, D. Little, M. Barry, F. Thornton, S. Sheehan, D. J. Bouchier-Hayes, P. Fitzgerald, P. Grace, Y. Gul, D. Waldron, M. Wali, M. P. Colgan, D. J. Moore, D. G. Shanik, J. MacNamara, V. P. Lynch, H. Abdih, W. Watson, J. D. Aloisi, T. J. Boyle, H. Kim Lyerly, C. Kelly, D. O’Donovan, W. Monkhouse, J. M. O’Donoghue, C. Curran, D. O’Hanlon, D. Maher, C. Homer, M. O’Brien, M. Caldwell, R. Sheehan, P. Crean, T. O’Brien, C. Grant, J. A. Van Heerden, J. A. Lynn, B. G. O’Donovan, D. S. Quill, C. P. Delaney, J. Phillips, J. A. McKeever, M. J. Earley, A. C. B. Hooper, S. K. Al-Ghazal, K. Khan, M. McKiernan, R. McQuillan, J. R. McCabe, D. O’Farrell, J. O’Byrne, B. O’Donovan, I. Rafi, M. Gilmore, F. Fitzgerald, R. Moran, D. O’Brien, C. Pidgeon, S. Young, D. Allcutt, D. Rawluk, D. P. O’Brien, J. P. Phillips, I. Beckingham, M. Hinwood, K. Rigg, M. Bishop, H. Rowley, T. P. O’Dwyer, I. J. Beckingham, J. S. O’Rourke, M. J. S. Dennis, P. R. F. Bell, M. L. Nicholson, N. Akhtar, M. O. Corcoran, T. H. Lynch, G. Connellan, D. Mulvin, B. Boyle, M. O’Donoghue, Y. El-Tayeb, J. O’Donoghue, L. Parke, D. A. Evoy, S. E. Attwood, P. W. N. Keeling, J. Doyle, J. R. Flynn, J. Hurley, A. E. Wood, C. Duncan, A. Quershi, A. Leahy, D. Hayes, H. Osborne, H. Mashali, and R. G. K. Watson

Subjects
business.industry, Medicine, General Medicine, business, Classics
Published
1994
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11. Expression profiling technology: its contribution to our understanding of breast cancer

Author

E A, Rakha, M E, El-Sayed, J S, Reis-Filho, and I O, Ellis

Subjects
Gene Expression Regulation, Neoplastic, Gene Expression Profiling, Humans, Breast Neoplasms, Female, Prognosis
Abstract

Breast cancer is a complex genetic disease characterized by the accumulation of multiple molecular alterations. Routine clinical management of breast cancer relies on clinical and pathological factors, however. These seem insufficient to reflect the whole clinical heterogeneity of tumours and are less than perfectly adapted to each patient. Recent advances in human genome research and high-throughput molecular technologies have made it possible to tackle the molecular complexity of breast cancer and have contributed to the realization that the biological heterogeneity of breast cancer has implications for treatment. Gene expression profiling of breast cancer has been performed using several approaches. This review will describe the details of gene expression profiling of breast cancer, the different approaches and the impact on clinical management.

Published
2008

12. Adenomyoepithelioma of the breast; a case report and literature review

Author

R, Tait, S E, Pinder, I O, Ellis, and A D, Purushotham

Abstract

A case of adenomyoepithelioma of the breast is presented in order to illustrate some of the difficulties in achieving a pathological diagnosis of this lesion. Given the emerging evidence for adenomyoepithelioma to develop into malignancy, it is imperative that the histopathological features of this lesion are well described and recognized.

Published
2007

14. Expert opinion: Reporting needle core biopsies of breast carcinomas

Author

S A, Hoda, M, Harigopal, G C, Harris, S E, Pinder, A H S, Lee, and I O, Ellis

Subjects
Pathology, Surgical, Biopsy, Humans, Breast Neoplasms, Female, Adenocarcinoma, Medical Records
Abstract

Many breast carcinomas are now diagnosed in needle core biopsies, after either mammographic detection or symptomatic presentation. There is dispute, however, about the range of information that should be included in the diagnostic report of these small and possibly unrepresentative samples. Is it sufficient to simply report the presence of carcinoma, in situ or invasive? Or should the histopathologist give a more detailed report including features of prognostic and predictive significance? If so, what is the evidence that the further information is, first, of clinical benefit and, second, not unreliable because of sampling variability? To address the question "What should be included in reports of needle core biopsies of breast carcinomas?" contributions were invited from authors in the USA and the UK.

Published
2003

15. Excision biopsy findings of patients with breast needle core biopsies reported as suspicious of malignancy (B4) or lesion of uncertain malignant potential (B3)

Author

A H S, Lee, H E, Denley, S E, Pinder, I O, Ellis, C W, Elston, P, Vujovic, R D, Macmillan, and A J, Evans

Subjects
Predictive Value of Tests, Biopsy, Needle, Carcinoma, Humans, Mass Screening, Breast Neoplasms, Female, Breast, Mammography
Abstract

The UK National Health Service Breast Screening Programme has proposed five categories for reporting breast needle core biopsies. The majority of cores are reported as benign (B1), normal (B2) or malignant (B5). The predictive value of the two borderline categories suspicious of malignancy (B4) and lesion of uncertain malignant potential (B3) was studied.Over a 2-year period a total of 3822 breast needle core biopsies were performed, with 2997 from symptomatic patients and 825 from women undergoing mammographic screening, including 43 B4 reports (40 patients) and 120 B3 reports (116 lesions in 115 patients). The frequencies of B4 (2.5% versus 0.7%) and B3 cores (7.3% versus 2.0%) were both higher in screening than in symptomatic patients. B4 was most commonly used for small fragments of atypical cells separate from the main core or focal atypical intraductal proliferations. The criteria for calling a core B3 were: atypical intraductal epithelial proliferations (including foci that in excision specimens would be classified as atypical ductal hyperplasia), lobular neoplasia, radial scar, papillary lesion, fibroepithelial lesion with cellular stroma and spindle cell proliferations. Excision biopsies were performed in 39 patients with B4 core and 96 with B3 core. Invasive carcinoma or ductal carcinoma in situ was seen in 33 of the patients with B4 (85%) and in 29 of those with B3 cores (25%). Some categories of B3 core were associated with a higher rate of malignancy (40% for atypical intraductal epithelial proliferations and 46% for lobular neoplasia).The positive predictive value for carcinoma is high following a B4 core (86%). The lesion should be excised, but definitive cancer treatment is not appropriate. In some cases a definite diagnosis of malignancy can be made on repeat core. The B3 group is more heterogeneous and has a lower rate of malignancy on further biopsy (25%). The majority of B3 lesions require excision. All these patients should be discussed at multidisciplinary meetings.

Published
2003

17. Neuroendocrine differentiation and prognosis in breast adenocarcinoma

Author

A, Miremadi, S E, Pinder, A H S, Lee, J A, Bell, E C, Paish, P, Wencyk, C W, Elston, R I, Nicholson, R W, Blamey, J F, Robertson, and I O, Ellis

Subjects
Adult, Synaptophysin, Breast Neoplasms, Adenocarcinoma, Middle Aged, Prognosis, Immunohistochemistry, Survival Analysis, Carcinoma, Neuroendocrine, Phosphopyruvate Hydratase, Chromogranins, Chromogranin A, Humans, Female, Aged, Follow-Up Studies
Abstract

Neuroendocrine differentiation has been detected, and its prognostic value studied, in a number of common human carcinomas. To date there are few detailed studies examining its relevance in breast carcinoma. In this study we evaluate the frequency and prognostic importance of neuroendocrine differentiation in breast adenocarcinoma.The presence of neuroendocrine differentiation, defined as positive reactivity for three markers, neuron-specific enolase (NSE), chromogranin A and/or synaptophysin, has been evaluated in 99 patients with primary operable breast cancer using standard immunocytochemical techniques. A consecutive cohort of patients were selected from the Nottingham/Tenovus series. Comprehensive patient and tumour records have been maintained, and patients were followed up according to a defined protocol. Eighteen cases were positive for NSE, 10 for chromogranin A and 13 for synaptophysin. Eleven percent were positive with more than one neuroendocrine marker. No significant association was found between neuroendocrine differentiation and tumour size, grade, stage or the prevalence of vascular invasion. There was no significant difference in either overall or disease-free survival between patients with or without neuroendocrine differentiation.In this study we confirm that neuroendocrine differentiation can be identified in a subset (10-18%) of human breast carcinomas. This phenomenon appears to have no relationship to established prognostic factors or patient outcome.

Published
2002

18. An audit of 'equivocal' (C3) and 'suspicious' (C4) categories in fine needle aspiration cytology of the breast

Author

R A, Deb, P, Matthews, C W, Elston, I O, Ellis, and S E, Pinder

Subjects
Breast Diseases, Medical Audit, Predictive Value of Tests, Biopsy, Needle, Humans, Breast Neoplasms, Female, Breast, Follow-Up Studies
Abstract

We have audited the frequency of use and outcome of the "equivocal/atypia probably benign" (C3) and "suspicious of malignancy" (C4) category for breast cytology in our Unit. A total of 14 935 cytological specimens were reported by at least one of the three pathologists with a special interest in breast pathology, according to five categories of the NHSBSP guidelines for cytology reporting, 1992; 3.7% (555 cases) and 3.9% (587 cases) of cases were classified as equivocal (C3) and suspicious (C4), respectively, giving a total rate (C3 + C4) of 7.6%. Of the C3 cases, 68% were subsequently benign and 32% were malignant. Of the C4 cases, 19% were subsequently benign and 81% malignant. The commonest benign lesions in both categories were fibroadenomas (7.6% of C3 and 19.8% of C4), fibrocystic change (14.3% of C3 and 12.5% of C4), radial scars (6.2% of C3 and 10.4% of C4) and papillomas (6.2% of C3 and 6.3% of C4). Of the malignant lesions (particularly those classified as C3), a high proportion were low grade or special type cancers. The categories of atypia probably benign (C3) and suspicious of malignancy (C4) in breast cytology provide a strategy for classification of problematic or uncertain cases; this maintains the predictive value of the benign (C2) and malignant (C5) categories, and allows separation of these difficult cases into clinically useful groups with differing probabilities of malignancy.

Published
2001

19. Mitotic counting in surgical pathology: sampling bias, heterogeneity and statistical uncertainty

Author

F B, Thunnissen, A W, Ambergen, M, Koss, W D, Travis, T J, O'Leary, and I O, Ellis

Subjects
Genetic Heterogeneity, Pathology, Surgical, Data Interpretation, Statistical, Neoplasms, Mitotic Index, Humans, Mitosis, Selection Bias
Abstract

Mitotic counting in surgical pathology: sampling bias, heterogeneity and statistical uncertainty Although several articles on the methodological aspects of mitotic counting have been published, the effects of macroscopic sampling and tumour heterogeneity have not been discussed in any detail. In this review the essential elements for a standardized mitotic counting protocol are described, including microscopic calibration, specific morphological criteria, macroscopic selection, counting procedure, effect of biological variation, threshold, and the setting of an area of uncertainty ('grey area'). We propose that the use of a standard area for mitotic quantification and of a grey area in mitotic counting protocols will facilitate the application of mitotic counting in diagnostic and prognostic pathology.

Published
2001

20. Phosphorylation of ERK1/2 mitogen-activated protein kinase is associated with poor response to anti-hormonal therapy and decreased patient survival in clinical breast cancer

Author

J M, Gee, J F, Robertson, I O, Ellis, and R I, Nicholson

Subjects
Adult, Antineoplastic Agents, Hormonal, MAP Kinase Signaling System, Breast Neoplasms, Disease-Free Survival, Statistics, Nonparametric, Predictive Value of Tests, Antineoplastic Combined Chemotherapy Protocols, Humans, Phosphorylation, Aged, Proportional Hazards Models, Aged, 80 and over, Mitogen-Activated Protein Kinase 1, Middle Aged, Prognosis, Immunohistochemistry, Survival Rate, Tamoxifen, Drug Resistance, Neoplasm, Case-Control Studies, Multivariate Analysis, Goserelin, Female, Mitogen-Activated Protein Kinases, Biomarkers
Abstract

It is believed that growth factor phosphorylation cascades interact closely with oestrogen receptor (ER) signaling to regulate breast cancer growth, and that alterations in these pathways may underlie resistance to anti-hormones such as tamoxifen. There is an increasing body of experimental evidence implicating the mitogen-activated protein kinase extracellular signal-regulated-kinases ERK1 and ERK2 (ERK1/2 MAPK) in these events. The present study is the first to address the relationship between ERK1/2 MAPK phosphorylation (p-MAPK) and response to anti-hormonal agents in clinical breast cancer (n = 90). Immunocytochemical analysis using a phosphorylation state-specific ERK1/2 MAPK antibody revealed 72% of breast tumors to have considerable nuclear p-MAPK immunostaining (designated p-MAPK positive), whereas staining was barely detectable or absent in the remaining 28% (designated p-MAPK negative). Comparison with staining in normal breast material obtained from reduction mammoplasty patients (n = 10) demonstrated an increased frequency of higher intensity p-MAPK immunostaining cells within carcinomas (p = 0.002). Significant relationships were revealed between p-MAPK positivity and poorer quality (p = 0.001) and shortened duration (p = 0.006) of anti-hormonal response, as well as with decreased survival time from the initiation of therapy (p = 0.022). These associations were retained in ER positive disease (p = 0.013, p = 0.037 and p = 0.048 respectively), where multivariate analysis demonstrated p-MAPK status to be a significantly independent predictor for response duration (p = 0.034) and patient survival (p = 0.029). Phosphorylated ERK1/2 MAP kinase is thus potentially prognostic for prediction of response to anti-hormonal agents and survival, data providing further evidence that ERK1/2 MAP kinase plays a role in circumvention of anti-hormonal response in breast cancer.

Published
2001

21. Sentinel node biopsy for breast cancer may have little to offer four-node-samplers. results of a prospective comparison study

Author

R D, Macmillan, D, Barbera, D J, Hadjiminas, R S, Rampaul, A H, Lee, S E, Pinder, I O, Ellis, R W, Blamey, and J G, Geraghty

Subjects
Clinical Protocols, Sentinel Lymph Node Biopsy, Axilla, Humans, Breast Neoplasms, False Positive Reactions, Female, Prospective Studies, Sensitivity and Specificity, Mastectomy
Abstract

The aims of the study were to determine how often four node axillary sampling (4NAS) encompasses the sentinel node (SN) and to compare the relative sensitivity of 4NAS with sentinel node biopsy (SNB) for axillary node staging. 200 patients with breast cancer were preoperatively injected with 27 MBq 99m-Tc-labelled colloid adjacent to the tumour. At operation, standard 4NAS was performed. Each node was counted ex vivo using a probe. A search was then made to find a node with higher counts in vivo directed by the probe. If found, it was excised. Each node was submitted separately to pathology. A SN was identified in 191 patients (96%). The SN was contained in the 4NAS in 153 patients (80%) and identified separately in 38 patients (20%). Of 60 node-positive patients, 49 were positive by 4NAS and SNB, the SN was not identified in 2 and in 8 the SN was falsely negative compared with 4NAS. For 1 patient, the SN was positive and the 4NAS negative. SNB performed using radiolabelled colloid has no advantage over 4NAS when nodes are assessed by standard histological technique.

Published
2001

22. Biological and clinical associations of c-jun activation in human breast cancer

Author

J M, Gee, A F, Barroso, I O, Ellis, J F, Robertson, and R I, Nicholson

Subjects
MAP Kinase Signaling System, Proto-Oncogene Proteins c-jun, Breast Neoplasms, Oncogene Proteins v-erbB, Immunohistochemistry, Survival Analysis, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, Transcription Factor AP-1, Receptors, Estrogen, Humans, Female, Cell Division, Signal Transduction
Abstract

Sub-units and regulators of the activating protein-1(AP-1) complex have been implicated in breast-cancer biology, therapeutic response and prognosis. This study has immunocytochemically examined the impact of c-jun-protein activation on biological and clinical parameters in human primary breast cancers, employing an antibody specific for the serine 63-phosphorylated c-jun protein. Substantial nuclear immunostaining was commonly apparent, indicative of an activated c-jun pool, with associations with MAP-kinase-signalling elements, e.g., transforming growth factor-alpha (p = 0.04), epidermal growth factor receptor (p = 0.08), phosphorylated erk 1/2 MAP kinase (p = 0.001) and phosphorylated jun kinase (p = 0.05) Little association was noted with c-fos protein, perhaps indicating alternative AP-1 partners for c-jun with a diversity of cellular end-points. This may explain the lack of relationship with proliferation and grade, the imperfect association between increased c-jun activation and poorer survival (p = 0.061), and the apparent relationship with distant metastasis (p = 0.05). While increased c-jun activation related to poorer quality (p = 0.09) and shortened duration of endocrine response in oestrogen-receptor-positive patients (p = 0.018), no generalized effects on oestrogen-regulated gene products were noted, indicating that AP-1 influences on oestrogen-receptor/oestrogen-response element transactivation are unlikely to explain endocrine insensitivity. These data reinforce our belief that elevated AP-1 signalling influences aspects of the breast-cancer phenotype.

Published
2001

23. A possible divergent role for the oestrogen receptor alpha and beta subtypes in clinical breast cancer

Author

J M, Knowlden, J M, Gee, J F, Robertson, I O, Ellis, and R I, Nicholson

Subjects
Receptors, Estrogen, Estrogen Receptor alpha, Estrogen Receptor beta, Humans, Breast Neoplasms, Female, RNA, Messenger, RNA, Neoplasm, Immunohistochemistry, Polymerase Chain Reaction, Neoplasm Staging
Abstract

We have examined the relative levels of oestrogen receptor beta (ERbeta) mRNA in 94 breast cancer specimens using a semi-quantitative RT-PCR procedure. We correlated its expression with ERalpha and various clinical, pathological and biochemical features of the disease. The level of ERbeta mRNA expression in these samples was found to be much lower than ERalpha. Although ERalpha mRNA species were found to be most frequently associated with histological grade I and II tumours, displaying tubular differentiation, low grades of nuclear pleomorphism and low mitotic activity, such features were not characteristic of ERbeta positive samples. Indeed, application of the Spearman rank correlation test revealed that there was an inverse association between ERbeta normalised levels and ERalpha protein HScore. Also ERbeta mRNA positive cancers were more frequently EGFR protein positive than their negative counterparts (p = 0.016), a feature normally associated with endocrine-insensitive disease. Our data suggest that although ERbeta levels are most likely lower than ERalpha, they may influence the biological behaviour of breast cancers containing low levels of ERalpha.

Published
2001

25. Gamma linolenic acid with tamoxifen as primary therapy in breast cancer

Author

F S, Kenny, S E, Pinder, I O, Ellis, J M, Gee, R I, Nicholson, R P, Bryce, and J F, Robertson

Subjects
Antineoplastic Agents, Hormonal, Biopsy, Administration, Oral, Breast Neoplasms, Middle Aged, Disease-Free Survival, Tamoxifen, Proto-Oncogene Proteins c-bcl-2, Receptors, Estrogen, Humans, Female, Neoplasm Metastasis, gamma-Linolenic Acid, Aged, Neoplasm Staging
Abstract

Gamma linolenic acid (GLA) has been proposed as a valuable new cancer therapy having selective anti-tumour properties with negligible systemic toxicity. Proposed mechanisms of action include modulation of steroid hormone receptors. We have investigated the effects of GLA with primary hormone therapy in an endocrine-sensitive cancer. Thirty-eight breast cancer patients (20 elderly Stage I-II, 14 locally advanced, 4 metastatic) took 8 capsules of oral GLA/day (total = 2.8 g) in addition to tamoxifen 20 mg od (T+GLA). Quality and duration of response were compared with matched controls receiving tamoxifen 20 mg od alone (n = 47). Serial tumour biopsies were taken to assess changes in oestrogen receptor (ER) and bcl-2 expression during treatment. GLA was well tolerated with no major side effects. T+GLA cases achieved a significantly faster clinical response (objective response vs. static disease) than tamoxifen controls, evident by 6 weeks on treatment (p = 0.010). There was significant reduction in ER expression in both treatment arms with T+GLA objective responders sustaining greater ER fall than tamoxifen counterparts (6-week biopsy p = 0.026; 6-month biopsy p = 0.019). We propose GLA as a useful adjunct to primary tamoxifen in endocrine-sensitive breast cancer. The effects of GLA on ER function and the apparent enhancement of tamoxifen-induced ER down-regulation by GLA require further investigation.

Published
2000

26. Metaplastic carcinoma of the breast arising within complex sclerosing lesion: a report of five cases

Author

H, Denley, S E, Pinder, P H, Tan, C S, Sim, R, Brown, T, Barker, J, Gearty, C W, Elston, and I O, Ellis

Subjects
Carcinoma, Adenosquamous, Sclerosis, Humans, Breast Neoplasms, Female, Middle Aged, Neoplasm Metastasis, Aged
Abstract

This study presents a series of five cases in which metaplastic carcinoma, predominantly low-grade adenosquamous carcinoma, of the breast is seen arising within a background of a complex sclerosing lesion. This association has been recognized previously but has not been documented in detail. This study describes the characteristics of the components present in each case and discusses the existing literature. This observation adds further evidence to support an association between some types of invasive breast carcinoma and sclerosing lesions of the breast.Four of these cases were received as referral cases for opinion. The fifth was received as part of the routine surgical workload within our own institution. Two patients presented following mammographic screening and three symptomatically; their mean age was 62 years (range 49-68). The mean lesion size was 16 mm (range 7-24). All five lesions showed features of a complex sclerosing lesion/radial scar in the form of central sclerosis with elastosis and radiating benign entrapped tubules. One had associated benign papillary structures and two had focal benign squamous metaplasia. Four cases showed coexisting but distinct areas of low-grade adenosquamous carcinoma with glandular and squamous epithelial differentiation in a spindle cell background. One case had associated undifferentiated spindle cell carcinoma. Detailed immunophenotypic characteristics of two cases are presented.This series illustrates a postulated but previously unconfirmed association between an unusual form of metaplastic breast carcinoma (adenosquamous carcinoma) and complex sclerosing lesions. The mechanisms of induction of breast carcinoma are poorly understood but these observations further emphasize the potential for sclerosing lesion of the breast to be associated with, and possibly give rise to, invasive carcinoma of different types. The precise nature of the interaction between the pathological processes remains unclear.

Published
2000

27. Immunohistochemical analysis reveals a tumour suppressor-like role for the transcription factor AP-2 in invasive breast cancer

Author

J M, Gee, J F, Robertson, I O, Ellis, R I, Nicholson, and H C, Hurst

Subjects
Cell Nucleus, Cyclin-Dependent Kinase Inhibitor p21, Receptor, ErbB-2, Blotting, Western, Antibodies, Monoclonal, Breast Neoplasms, Immunohistochemistry, Proto-Oncogene Mas, Statistics, Nonparametric, Neoplasm Proteins, DNA-Binding Proteins, Transcription Factor AP-2, Cyclins, Humans, Female, Genes, Tumor Suppressor, Enzyme Inhibitors, Transcription Factors
Abstract

This paper describes the generation and characterization of a monoclonal antibody specific for two members of the AP-2 family of transcription factors, AP-2alpha and AP-2beta, and its subsequent application to archival primary breast tumour material. Nuclear localization of AP-2 was found in all expressing cases, but in general levels of immunostaining were low, with only 17 per cent of the 86 tumours examined showing very high expression levels. Nevertheless, data analysis of the whole patient series allowed the identification of significant relationships between levels of AP-2 and other important breast markers. Thus, expression of AP-2alpha/beta was found to correlate significantly with expression of both ER ( p=0.036*) and the universal cell-cycle inhibitor p21(cip) ( p=0.03*), but was inversely related to levels of the proto-oncogene ErbB2 ( p=0.008*). AP-2-positive tumours also showed a low rate of proliferation, with significantly reduced mitotic count and a lower tumour grade. There was no significant relationship with clinical parameters, but samples with adjacent normal tissue indicated that loss of the AP-2 marker was associated with disease progression from normal breast through to invasive disease. This was confirmed by examining separate series of pure normal and pure DCIS samples, both of which expressed significantly higher levels of AP-2 ( p=0.0001* in each case) than the invasive tumours. Overall, these findings implicate AP-2alpha/beta as having a role akin to that of a tumour suppressor in breast cancer.

Published
2000

29. A critical appraisal of existing classification systems of epithelial hyperplasia and in situ neoplasia of the breast with proposals for future methods of categorization: where are we going?

Author

I O, Ellis, S E, Pinder, A H, Lee, and C W, Elston

Subjects
Chromosome Aberrations, Carcinoma, Intraductal, Noninfiltrating, Hyperplasia, Terminology as Topic, Disease Management, Humans, Breast Neoplasms, Breast, Precancerous Conditions, Carcinoma in Situ
Abstract

Current classification systems for borderline lesions of the breast including epithelial hyperplasia, atypical hyperplasia, and ductal carcinoma in situ fall short of the ideal. They present pathologists with problems of recognition or clear distinction and clinicians with difficult management choices. In addition, recent evidence indicates that different pathogenetic lesions are present in some categories. This article presents a brief critical appraisal of the existing classifications and offers suggestions for revision using a model of pathogenetic lineage.

Published
1999

30. Ductal carcinoma in situ of the human breast: clinico-pathological aspects

Author

S E, Pinder, A J, Evans, and I O, Ellis

Subjects
Clinical Trials as Topic, Antineoplastic Agents, Hormonal, Biopsy, Carcinoma, Ductal, Breast, Breast Neoplasms, Combined Modality Therapy, Tamoxifen, Chemotherapy, Adjuvant, Humans, Female, Breast, Neoplasm Recurrence, Local, Carcinoma in Situ, Mammography, Randomized Controlled Trials as Topic
Abstract

The apparent increase of incidence of DCIS is related to the development of mammographic screening programs and requires an effort of diagnostic, classification and treatment revision. The same natural history of the DCIS is still poorly known, and the phases of its evolution are supposed essentially on epidemiologic and statistics bases. The efforts for a classification are aimed to the search of a prognostic meaning: nuclear grading and possible invasive evolution; association of nuclear grading and necrosis. Both are correlated with local recurrence and free interval. The finding of micro-calcifications is the basis of the instrumental mammographic diagnosis; the possible isolated and unique finding encourages choices of conservative surgery. But as the less large lesions are as a rule of higher grade than those more extended, there are the treatment can be puzzling. As a consequence in fact the former are exposed to wider resections than the last ones. The DCIS is also characterized in its post-surgical evolution from the borders of the excision, from the pathologic classification, from the nuclear degree and from the dimensions of the lesion. In the more favourable conditions the surgical excision represents an adequate treatment. The radiotherapy finds his role in the more elevated degrees and in the case of incomplete excision, also if only presumptive. The alternative is the reoperation and the mastectomy.

Published
1999

31. p21(WAF1) expression and endocrine response in breast cancer

Author

R A, McClelland, J M, Gee, L, O'Sullivan, D M, Barnes, J F, Robertson, I O, Ellis, and R I, Nicholson

Subjects
Adult, Aged, 80 and over, Cell Nucleus, Cyclin-Dependent Kinase Inhibitor p21, Breast Neoplasms, Middle Aged, Immunohistochemistry, Survival Analysis, Ki-67 Antigen, Receptors, Estrogen, Cyclins, Biomarkers, Tumor, Humans, Female, Tumor Suppressor Protein p53, Aged
Abstract

An immunocytochemical assay for the p53-regulated protein product of the WAF1/Cip1 gene, p21(WAF1) (p21), was developed and applied to archival primary breast tumour material from 91 patients whose subsequent recurrent disease was treated with assessable courses of endocrine therapy. Nuclear localization of p21 protein was observed in 76 (82.4 per cent) cases. Status cut-offs were established and 29 (31.9 per cent) were deemed negative, 39 (42.9 per cent) weakly positive, and 23 (25.3 per cent) strongly positive. p21 status was inversely correlated with p53 protein (p=0.047) but did not relate to oestrogen receptor (ER) status, response to endocrine therapy, or time to further disease progression (TTP). Highly p21-positive patients had a significantly improved overall survival time (p=0. 020). Co-assessment of p21 and p53 subgroups revealed p21+/p53- patients to have good survival characteristics, whilst p21-/p53+ patients did poorly (p=0.008). The p21-/p53- patients overall did intermediately well, but Ki67-defined cellular proliferation analysis of these revealed two subclasses: those with high proliferation and poor survival times resembling the p21-/p53+ phenotype, and those with less proliferative tumours with good survival, similar to the p21+/p53- group. The significance of these results is discussed in the light of recent research concerning the role of p21 and p53 in breast cancer aetiology.

Published
1999

32. An immunohistochemical examination of the expression of E-cadherin, alpha- and beta/gamma-catenins, and alpha2- and beta1-integrins in invasive breast cancer

Author

M A, Gonzalez, S E, Pinder, P M, Wencyk, J A, Bell, C W, Elston, R I, Nicholson, J F, Robertson, R W, Blamey, and I O, Ellis

Subjects
Adult, Integrin beta1, Integrin alpha2, Breast Neoplasms, Middle Aged, Cadherins, Prognosis, Neoplasm Proteins, Immunoenzyme Techniques, Cytoskeletal Proteins, Desmoplakins, Antigens, CD, Biomarkers, Tumor, Trans-Activators, Humans, Female, Neoplasm Invasiveness, Cell Adhesion Molecules, alpha Catenin, beta Catenin, Aged, Proportional Hazards Models
Abstract

This study examines the expression of the cell-cell adhesion molecules E-cadherin and its associated proteins, the catenins and the matrix-cell adhesion molecules beta1- and alpha2-integrins, in primary invasive breast carcinoma. Expression was assessed immunohistochemically on frozen sections by semi-quantitative scoring of the intensity and proportion of immunoreactivity in 55 cases. Associations with each other and with other histological and prognostic features and survival were sought. There was a significant association between loss of E-cadherin expression and loss of alpha- and beta/gamma-catenin immunostaining. In 20 per cent of cases, membranous immunoreactivity with E-cadherin antibody was absent. Absent cytoplasmic expression of alpha- and beta/gamma-catenins was seen in 24 and 22 per cent of breast cancers, respectively. The intensity of reactivity with E-cadherin showed a significant association with histological grade (p=0.002) and tumour type (p0.001). Lobular carcinomas frequently showed loss of expression of E-cadherin, as reported elsewhere; loss of catenin expression was also found in these tumours. alpha-catenin intensity also showed a relationship with grade (p=0.008) and with oestrogen receptor (ER) status (p=0.006). beta/gamma-catenin expression was not associated with other known prognostic factors. Forty-nine per cent and 42 per cent of cases showed no membrane immunostaining with beta1- and alpha2-integrin, respectively, and co-ordinated loss of beta1- and alpha2-integrin expression was found. Both beta1- and alpha2-integrin expression were associated with histological grade (p=0.003 and p=0.031, respectively) and beta1 immunoreactivity with tumour type (p=0.010). None of the variables examined showed a statistically significant association with tumour size or lymph node stage, or with overall survival, although a trend was seen (p=0.087) towards poorer survival of patients with tumours with absent or weak expression of beta1-integrin. The expression of these markers is of biological interest, but appears to be of little additional use in predicting clinical behaviour.

Published
1999

33. BRCA1 expression levels predict distant metastasis of sporadic breast cancers

Author

L T, Seery, J M, Knowlden, J M, Gee, J F, Robertson, F S, Kenny, I O, Ellis, and R I, Nicholson

Subjects
Receptors, Estrogen, BRCA1 Protein, Reverse Transcriptase Polymerase Chain Reaction, Humans, Breast Neoplasms, Female, RNA, Messenger, Neoplasm Metastasis, Prognosis
Abstract

The role of BRCA1 in progression of sporadic breast cancers has to date been equivocal, although preliminary studies on small numbers of samples have suggested an association between expression levels of this gene and acquisition of an invasive phenotype. We have further reasoned that loss of oestrogen receptor positivity may have a detrimental effect on BRCA1 expression. In order to test this hypothesis and extend earlier investigations we have applied a sensitive RT-PCR procedure to determine the associations between BRCA1 expression and a variety of clinical parameters in a sample cohort derived from sporadic breast tumour specimens. We have established that BRCA1 and ER mRNA expression are closely associated (p=0.013), indicating a possible functional relationship between these 2 genes. We have further identified an association between low levels of BRCA1 expression and acquisition of distant metastasis in sporadic disease (p=0.019). In light of our findings, we suggest that suppression of BRCA1 has a role to play in progression of a significant fraction of sporadic breast cancers and may additionally prove to be a useful, novel, prognostic marker for this disease type.

Published
1999

34. Endocrine response and resistance in breast cancer: a role for the transcription factor Fos

Author

J M, Gee, P C, Willsher, F S, Kenny, J F, Robertson, S E, Pinder, I O, Ellis, and R I, Nicholson

Subjects
Time Factors, Antineoplastic Agents, Hormonal, Breast Neoplasms, Endocrine System, Immunohistochemistry, Survival Analysis, Tamoxifen, Ki-67 Antigen, Biomarkers, Tumor, Disease Progression, Mitotic Index, Humans, Female, Proto-Oncogene Proteins c-fos, Aged
Abstract

We have previously demonstrated that elevated Fos expression may be important in de novo endocrine resistance in breast cancer. However, changes in Fos expression during endocrine response and subsequently on acquisition of resistance are unknown. This study immunocytochemically monitors Fos protein within sequential biopsies from primary human breast cancer patients obtained pre-treatment (T1), during tamoxifen therapy (T2, T3) and on disease progression (T5), examining in parallel proliferation [i.e., MIBI (Ki67) immunostaining, mitotic activity], cellularity and endocrine response. Significantly diminished Fos, proliferation and cellularity were observed after 6 weeks of therapy in patients exhibiting a better quality and/or duration of response, while modest Fos increases and a maintained proliferation and cellularity were seen in poorer responders. Decreases in Fos, proliferation and cellularity at 6 months similarly hallmarked better responders. We confirmed a significant association between de novo resistance and elevated Fos and proliferation. Additionally, however, these parameters increased at the time of disease relapse over pre-treatment and "on therapy" values. Our data indicate that tamoxifen response involves a reduction in both tumor cell proliferation and cell survival, potentially entailing diminished Fos protein expression in better-responding patients. Our data are also supportive of elevated Fos expression being involved in the departure from endocrine control inherent in both primary and acquired resistance.

Published
1999

35. Use of reverse transcription-polymerase chain reaction methodology to detect estrogen-regulated gene expression in small breast cancer specimens

Author

J M, Knowlden, J M, Gee, S, Bryant, R A, McClelland, D L, Manning, R, Mansel, I O, Ellis, R W, Blamey, J F, Robertson, and R I, Nicholson

Subjects
Transcription, Genetic, Reverse Transcriptase Polymerase Chain Reaction, Tumor Suppressor Proteins, Proteins, Breast Neoplasms, Estrogens, Immunohistochemistry, Gene Expression Regulation, Neoplastic, Receptors, Estrogen, Biomarkers, Tumor, Humans, Female, Trefoil Factor-1, RNA, Messenger, Receptors, Progesterone
Abstract

We describe the development and use of a sensitive reverse transcription-PCR (RT-PCR) procedure to detect novel estrogen-regulated gene expression in small clinical breast cancer samples, in which such study would be extremely difficult by any other molecular or immunocytochemical means. Assay optimization for pLIV1, estrogen receptors (ERs), progesterone receptors, and pS2 gene products was carried out on 50 primary breast cancers for which comparative Northern analysis and immunocytochemical data were available. Using 27 amplification cycles and a 0.5 microM primer concentration, varying expressions of the gene products were recorded simultaneously with a constant densitometric signal for a coamplified endogenous control gene (alpha-actin). Good concordances were subsequently observed between pLIV1 status generated by RT-PCR and both Northern analysis (P = 0.002) and ER status by immunocytochemistry (P = 0.0244). Agreement was also noted between ER (P = 0.002), progesterone receptor (P = 0.0005), and pS2 (P = 0. 0023) RT-PCR and immunocytochemical methodologies. The RT-PCR assays were then applied to 10 needle core trucut biopsies in which similar relationships were obtained. Our results justify the future use of this RT-PCR methodology to examine new estrogen-regulated genes in small breast cancer samples, and it is envisaged that this technology will prove invaluable in many future breast cancer studies.

Published
1998

37. The importance of the histologic grade of invasive breast carcinoma and response to chemotherapy

Author

S E, Pinder, S, Murray, I O, Ellis, H, Trihia, C W, Elston, R D, Gelber, A, Goldhirsch, J, Lindtner, H, Cortés-Funes, E, Simoncini, M J, Byrne, R, Golouh, C M, Rudenstam, M, Castiglione-Gertsch, and B A, Gusterson

Subjects
Antimetabolites, Antineoplastic, Antineoplastic Agents, Hormonal, Breast Neoplasms, Disease-Free Survival, Cohort Studies, Antineoplastic Combined Chemotherapy Protocols, Humans, Neoplasm Invasiveness, Antineoplastic Agents, Alkylating, Cyclophosphamide, Mastectomy, Proportional Hazards Models, Carcinoma, Estrogen Antagonists, Prognosis, Postmenopause, Survival Rate, Tamoxifen, Methotrexate, Premenopause, Chemotherapy, Adjuvant, Prednisone, Female, Fluorouracil, Lymph Nodes, Forecasting
Abstract

Histologic grade is well recognized for its prognostic significance in cases of primary operable invasive breast carcinoma; however, the majority of studies in which grade has been assessed have been based on single-center trials. In addition, the role of grade in predicting response to chemotherapy has not been examined in many previous studies.The authors assessed the value of Nottingham histologic grade (NHG) in a group of 465 patients enrolled in a multicenter, randomized International Breast Cancer Study Group clinical trial of adjuvant chemotherapy for patients with lymph node (LN) positive and LN negative primary breast carcinoma (formerly named Ludwig Trial V).NHG was a predictor of overall survival for both LN negative and LN positive patients (P=0.045 and P0.001, respectively). NHG was associated with a poorer prognosis for both LN positive and LN negative patients, with hazard ratios of 1.651 (P0.001) and 1.437 (P=0.045), respectively, for an increase of one grade. Among LN negative patients, this survival disadvantage was observed only for those who received perioperative chemotherapy. For LN positive patients, an increase of one grade resulted in a significant overall survival disadvantage regardless of whether prolonged or perioperative chemotherapy was given. For LN negative patients grouped by grade, there was no observed difference in overall or disease free survival according to whether perioperative chemotherapy or no adjuvant therapy was given. However, LN positive patients with Grade 3 tumors had a significantly greater overall and disease free survival benefit from prolonged chemotherapy than from perioperative chemotherapy (P=0.016 and P=0.013, respectively); LN positive patients with Grade 1 or 2 disease in both treatment arms had comparable overall and disease free survival. A strong correlation between the previously utilized Bloom-Richardson grading system (BRG) and NHG was observed (P0.001 and kappa=82%) and no apparent differences in overall and disease free survival were observed between the two systems. NHG did, however, identify a greater proportion of tumors as Grade 1, and BRG identified a greater proportion of breast carcinomas as Grade 3.This multicenter clinical study confirms the value of histologic grade, and the authors propose that this technique be used to identify Grade 3, LN positive patients who will benefit from prolonged rather than perioperative chemotherapy.

Published
1998

38. Tumour cell membrane laminin expression is associated with basal-like phenotype and poor survival in Nigerian breast cancer.

Author

A. O. J., AGBOOLA, H. O., EBILI, V. O., IYAWE, A. A. F., BANJO, B. S., SALAMI, E. A., RAKHA, C., NOLAN, I. O., ELLIS, and A. R., GREEN

Abstract

Introduction: Laminin is a glycoprotein with diverse functions in carcinogenesis including cell proliferation, invasion, metastases and epithelial-mesenchymal transition (EMT). In breast cancer (BC) laminin expression is speculated to be associated with unfavourable clinicopathological and molecular characteristics. We hypothesize that laminin expression would contributed to the aggressive nature of basal like and triple negative BC phenotype observed in Black women. Methods: The expression of laminin was determined in a well-characterised Nigerian cohort of 255 BC using tissue microarray and immunohistochemistry. Laminin expression was compared with clinical, pathological and survival characteristics. Results: Laminin was expressed in 146 (57.3%) cases and significantly correlated with younger age at diagnosis (p=0.005), premenopausal status (p=0.003), expression of EGFR (p=0.002), ID4 and MTA1, basal cytokeratin 5/6, p53, and triple negative tumours (all p<0.001). In addition, there was an inverse association of laminin expression with E-cadherin (p=0.03), ER and PgR (all p<0.001) and a trend with BRCA1 (p=0.05). Univariate survival analysis showed tumours positive for laminin had significantly poorer breast cancer specific survival (BCSS, p=0.009) and disease free interval (p=0.03), but not associated in Cox multivariate analysis. Conclusion: This study demonstrates that laminin expression may have important roles in the aggressive nature observed in the basal-like and triple negative molecular subtype of Nigerian BC women. [ABSTRACT FROM AUTHOR]

Published
2016

39. Male breast cancer: pathological and immunohistochemical features

Author

P C, Willsher, I H, Leach, I O, Ellis, J A, Bell, C W, Elston, J B, Bourke, R W, Blamey, and J F, Robertson

Subjects
Male, Time Factors, Receptor, ErbB-2, Mucin-1, Breast Neoplasms, Prognosis, Immunohistochemistry, Survival Analysis, Breast Neoplasms, Male, ErbB Receptors, Receptors, Estrogen, Biomarkers, Tumor, Humans, Female, Neoplasm Invasiveness, Tumor Suppressor Protein p53, Receptors, Progesterone, Follow-Up Studies, Retrospective Studies
Abstract

male breast cancer is uncommon and studies regarding the potential clinical relevance of the histopathological and immunohistochemical features are infrequently reported.We investigated the biological characteristics of forty-one male patients with invasive breast cancer by assessing histopathological and multiple immunohistochemical features.The majority were no special type (ductal) (37/41), lobular cancer was not seen. 73% were histological grade 3, 93% were positive for oestrogen receptor and 73% for progesterone receptor. The proportion of cancers positive for c-ebB-2 (45%), EGFR (20%), p53 (58%), MiB1 (40%), NCRC11 (78%), were similar to reports for female breast cancer. Nonsignificant associations between poor survival outcome and grade 3 tumours, and positive tissue staining for MiB1 and p53 were seen.While there ar similarities in the biological features of breast cancer in males and females, some differences were identified. Male breast cancer is more likely to be grade 3 tumours and hormone receptor positive.

Published
1997

40. Quality assurance in DNA image analysis on diploid cells

Author

F B, Thunnissen, I O, Ellis, and U, Jutting

Subjects
Quality Control, Liver, Fibroadenoma, Leukocytes, Humans, Breast Neoplasms, DNA, Diploidy, Image Cytometry
Abstract

DNA image analysis is presently performed in many laboratories. Before general extrapolation of results between different laboratories, validation has to be performed for interlaboratory studies on DNA image analysis. The aim of this study was to establish the performance of different DNA image analysis instruments when measuring different diploid cells. On three separate parts of the same object slide, human liver cells, white blood cells, and imprints of a breast fibroadenoma were sampled. In this quality assurance interlaboratory study, 13 laboratories participated voluntarily. Two slides were sent to each participating laboratory: one Feulgen and one unstained to be stained according the participating laboratory in-house procedure. The features integrated optical density (IOD) and object AREA were recorded for each nucleus. For calculation of the results, the average IOD value of liver diploid cells was set at 2c. A striking difference was observed between the different presumed diploid cell types, from almost 1c to 3c. This variation was not dependent on central or in-house staining. Although in-house calibration was performed for each image analysis system, a surprisingly large variation existed in the reported object AREA, irrespective of the cell type. These results clearly demonstrate that measurements performed in one laboratory cannot be extrapolated to the outcome of others and support the need for standardization. The use of external control cells works well for comparison of instruments. In conclusion, in DNA image analysis quality control is necessary, standardization is obligatory, and the use of an internal control for determination of the diploid peak in a histogram of patient samples is recommended.

Published
1997

41. High levels of allele loss at the FHIT and ATM genes in non-comedo ductal carcinoma in situ and grade I tubular invasive breast cancers

Author

S, Man, I O, Ellis, M, Sibbering, R W, Blamey, and J D, Brook

Subjects
Heterozygote, Tumor Suppressor Proteins, Carcinoma, Ductal, Breast, Proteins, Breast Neoplasms, Cell Cycle Proteins, Ataxia Telangiectasia Mutated Proteins, DNA, Neoplasm, Adenocarcinoma, Protein Serine-Threonine Kinases, Polymerase Chain Reaction, Sensitivity and Specificity, Acid Anhydride Hydrolases, Neoplasm Proteins, DNA-Binding Proteins, Cell Transformation, Neoplastic, Chromosomes, Human, Humans, Female, Neoplasm Invasiveness, Alleles, Carcinoma in Situ, Gene Deletion, Microsatellite Repeats
Abstract

Fifty-four grade 1 tubular breast cancers and nine non-comedo ductal carcinoma in situ samples have been analyzed for loss of heterozygosity using a series of microsatellite markers. Markers mapping to regions of the genome for which loss of heterozygosity has been documented previously in higher-grade breast cancers were selected for this analysis. Even within this group of good prognostic early breast cancers, genetic events are very common. The highest levels of loss were observed for D3S1300, which maps within an intron of the recently identified FHIT gene. High levels of loss were also observed within the ATM gene. These findings indicate that allele loss at FHIT and ATM may be an important early event in the development of sporadic breast cancer.

Published
1996

42. The significance of p53 autoantibodies in the serum of patients with breast cancer

Author

P C, Willsher, S E, Pinder, L, Robertson, R I, Nicholson, I O, Ellis, J A, Bell, R W, Blamey, J A, Green, and J F, Robertson

Subjects
Antibodies, Neoplasm, Humans, Breast Neoplasms, Female, Tumor Suppressor Protein p53, Prognosis, Autoantibodies, Neoplasm Staging
Abstract

Serum p53 autoantibodies were studied in 82 patients with Stage 1 or 2 breast cancer using an ELISA assay. Tissue expression of p53 in these patients was also examined. High levels of serum p53 autoantibodies were detected in 48% (39/82) patients, while 23% (19/82) were tissue positive. Patients with high serum p53 autoantibodies levels were not significantly different to those with low levels with respect to, tissue p53, tumour grade, size, stage or oestrogen receptor status. Tissue immunoreactivity for p53 was significantly associated with tumour grade and negative oestrogen receptor status. Patients in both groups were followed for a median of over five years but the presence of p53 autoantibodies in serum was not prognostic with respect to disease free interval or survival. In this study detection of p53 autoantibodies in serum does not correlate with any of the usual tumour related prognostic factors, nor does it correlate with clinical outcome.

Published
1996

44. The radiological appearances of invasive cribriform carcinoma of the breast. Nottingham Breast Team

Author

J A, Stutz, A J, Evans, S, Pinder, I O, Ellis, L J, Yeoman, A R, Wilson, and D M, Sibbering

Subjects
Humans, Breast Neoplasms, Female, Ultrasonography, Mammary, Adenocarcinoma, Middle Aged, Aged, Mammography
Abstract

Invasive cribriform carcinoma (ICC) of the breast is characterized by a cribriform histological architecture. It is rare, accounting for 0.6% of breast cancers in Nottingham and has an excellent prognosis. Its radiological features have not been previously described. Preoperative mammograms were available in eight cases (6 symptomatic, 2 screen-detected) and preoperative ultrasound examinations in four. The tumour was mammographically occult in four (50%) cases. The four tumours which were visible on mammography all showed as a large (20-35 mm) spiculated mass and two contained a few flecks of punctate calcification. The ultrasound appearances were not entirely typical of breast carcinoma. Three of four showed an ill-defined, inhomogeneous solid mass, but without the distal acoustic attenuation found in 60-97% of other forms of breast carcinoma. We conclude that ICC has imaging characteristics distinct from tubular carcinoma, which is its closest histological analogue.

Published
1994

45. Correlations between the mammographic features of ductal carcinoma in situ (DCIS) and C-erbB-2 oncogene expression. Nottingham Breast Team

Author

A J, Evans, S E, Pinder, I O, Ellis, D M, Sibbering, C W, Elston, D N, Poller, and A R, Wilson

Subjects
Receptor, ErbB-2, Carcinoma, Ductal, Breast, Biomarkers, Tumor, Humans, Breast Neoplasms, Breast, Immunohistochemistry, Mammography
Abstract

C-erbB-2 oncogene expression is found in 60% of DCIS cases. C-erbB-2 expression in DCIS has been shown to correlate with comedo subtype, large cell size, lymphoid infiltrate, nuclear pleomorphism, multinucleation and high mitotic rate. These findings have led to the suggestion that the subgroup of DCIS that expresses c-erbB-2 may be a biologically definable category with prognostic significance. The purpose of this study was to identify any differences in the mammographic appearances between DCIS which expresses c-erbB-2 and DCIS that does not express this oncogene.C-erbB-2 staining characteristics and preoperative mammograms were available for review in 126 patients with pure DCIS. All the mammograms were reviewed by a radiologist knowing the patient had DCIS but without any further pathological or immunohistochemical information.C-erbB-2 positive DCIS showed the following features more commonly than c-erbB-2 negative disease: calcification (65 of 71 (92%) vs 28 of 39 (72%), P0.01), ductal distribution of calcification (51 of 65 (78%) vs 16 of 28 (57%), P0.05), rod-shaped calcification (53 of 65 (82%) vs 15 of 28 (54%), P0.01) and granular calcification (63 of 65 (97%) vs 24 of 28 (86%), P0.05). C-erbB-2 negative DCIS more commonly showed an abnormal mammogram without calcification than c-erbB-2 positive disease (11 of 39 (28%) vs 6 of 71 (8%), P0.01).We have demonstrated significant differences in the mammographic features of c-erbB-2 positive and negative disease. As c-erbB-2 expression has been shown to correlate with aggressive histological features, the differences in the mammographic appearances between c-erbB-2 positive and c-erbB-2 negative DCIS may be of practical value.

Published
1994

46. Transforming growth factor-alpha and endocrine sensitivity in breast cancer

Author

R I, Nicholson, R A, McClelland, J M, Gee, D L, Manning, P, Cannon, J F, Robertson, I O, Ellis, and R W, Blamey

Subjects
Nuclear Proteins, Breast Neoplasms, Transforming Growth Factor alpha, Immunohistochemistry, Neoplasm Proteins, ErbB Receptors, Tamoxifen, Ki-67 Antigen, Receptors, Estrogen, Biomarkers, Tumor, Goserelin, Humans, Female, Menopause
Abstract

The expression of transforming growth factor-alpha (TGF-alpha) has been evaluated in 51 breast cancers of known responsiveness to endocrine therapy using immunohistochemistry. High levels of TGF-alpha were observed in 65% of tumors and showed no relationship with tumor estrogen receptor or epidermal growth factor receptor status or Ki67 immunostaining. TGF-alpha levels did, however, relate to the endocrine sensitivity of the disease, with unresponsive tumors frequently showing high levels of TGF-alpha immunoreactivity. This relationship was observed in estrogen receptor-positive disease and was independent of the epidermal growth factor receptor status of the tumor. No quantitative association between TGF-alpha and Ki67 immunostaining was observed in any of the subcategories of tumors. These data infer a role for TGF-alpha in the development of endocrine insensitivity in estrogen receptor-positive breast cancer by mechanisms which appear independent of tumor growth fraction, as determined by Ki67 immunostaining.

Published
1994

47. Ideas in pathology. Ductal carcinoma in situ of the breast: a proposal for a new simplified histological classification association between cellular proliferation and c-erbB-2 protein expression

Author

D N, Poller, M J, Silverstein, M, Galea, A P, Locker, C W, Elston, R W, Blamey, and I O, Ellis

Subjects
Ploidies, Receptor, ErbB-2, Carcinoma, Ductal, Breast, Breast Neoplasms, DNA, Neoplasm, Prognosis, ErbB Receptors, Immunoenzyme Techniques, Necrosis, Proto-Oncogene Proteins, Biomarkers, Tumor, Humans, Female, Carcinoma in Situ, Cell Division
Abstract

The diagnosis of ductal carcinoma in situ of the breast (DCIS) has become common with the advent of breast screening programs.Proliferation indices (S-phase fraction) were studied in 76 cases of pure DCIS. Tumors were classified according to conventional criteria and also according to a novel simplified classification based on cellular necrosis and morphology. This new classification defines three distinct tumor groups: pure comedo in 19 (25.0%) cases, DCIS with necrosis (non-pure comedo) in 21 (27.6%) patients, and DCIS without necrosis in 36 (47.4%) of cases, the latter group comprising largely classical cribriform or micropapillary architectural subtypes.Flow cytometric DNA analysis showed a significantly higher S-phase fraction in comedo DCIS than in the subgroup of DCIS tumors without necrosis (P0.01 [anova]). A preliminary analysis of disease recurrence and disease-free survival in a large series of 391 cases of pure DCIS showed that of 181 cases of pure comedo DCIS there were 19 local recurrences at the 7-year stage (82% 7-year disease-free survival), with 5 local recurrences in 51 cases of DCIS with necrosis (non-pure comedo) (85% 7-year disease-free survival) and only 6 local recurrences in the 159 cases of the DCIS-without-necrosis subgroup (94% 7-year disease-free survival). The chi 2 value for the frequency of disease recurrence of all cases of DCIS with necrosis (i.e., combining the groups of comedo DCIS and DCIS with necrosis (non-pure comedo)) as compared to DCIS without histological evidence of necrosis was 5705 (df = 2; P = 0.0001), and the chi 2 for disease-free survival of types of DCIS with necrosis as compared to cases without necrosis was 178 (df = 2; P = 0.0001). This analysis indicates that the histological presence of necrosis appears to be a relatively powerful predictor of increased disease recurrence and poorer disease-free survival after treatment for DCIS.Necrosis in DCIS in the absence of pure classical comedo morphology is a feature of more biologically aggressive in situ breast cancer with an intermediate proliferative fraction as compared with the high proliferative fraction of pure comedo DCIS and the low proliferative fraction of DCIS without necrosis. There was no significant difference in DNA ploidy (diploid or aneuploid) between the subgroups as assessed by chi 2 analysis. Further larger studies are required to establish if DCIS with necrosis (non-pure comedo) also shows a greater tendency to local recurrence after breast conservation treatment than do subtypes of DCIS without necrosis. DCIS with necrosis (non-pure comedo) should be adopted as a distinct histological subgroup of DCIS in future clinical studies of in situ mammary carcinoma.

Published
1994

48. Seventeenth sir peter freyer memorial lecture and surgical symposium

Author

D. O’Gradaigh, P. J. Byrne, P. Gillen, P. Lawlor, T. N. Walsh, T. P. J. Hennessy, S. T. O’Sullivan, G. C. O’Sullivan, W. O. Kirwan, H. Li, M. T. P. Caldwell, S. Hone, S. E. A. Attwood, I. P. Kelly, T. P. Corrigan, E. Mulligan, M. J. Kerin, N. N. Williams, K. J. Cronin, M. El Sadar, P. Dervan, J. M. Fitzpatrick, T. F. Gorey, M. Maher, D. Hehir, A. Horgan, R. Stuart, J. A. O’Donnell, M. P. Brady, J. M. O’Donoghue, J. R. Flynn, J. Doyle, M. Gallagher, K. Connolly, M. Barry, M. G Davies, M. West, E. O’Broin, J. A. Connolly, D. Long, M. F. Shine, F. Lennon, K. J. Dawson, J. R. Novell, A. K. Burroughs, K. Rolles, W. P. Joyce, J. Dolan, J. Hyland, O. Traynor, M. Bennett, O. Tighe, H. Mulcahy, D. O’Donoghue, D. Bouchier-Hayes, D. T. Croke, G. Santos, G. Khoury, M. C. Winslet, A. A. M. Lewis, E. Beausang, K. Mealy, L. Joyce, M. McNicholls, D. McErlean, M. A. Stokes, K. Barry, R. Sullivan, J. Byrne, J. Callaghan, T. O’Gorman°, H. F. Given, M. S. Dudeney, M. P. Redmond, J. M. Deasy, V. K. Young, R. G. K. Watson, G. O’Kane, K. Murphy, C. McDowell, K. Khan, S. K. Al-Ghazal, J. McCann, R. C. Stuart, M. O’Connor, J. McCabe, J. O’Byrne, D. O’Farrell, M. Walsh, J. O’Beirne, S. O’Flannagan, A. McGuinness, O. Brady, W. Quinlan, J. P. McCabe, B. Curtin, M. Stephens, J. Stack, P. McCarthy, M. Schnall, H. Pollack, T. H. Lynch, B. Waymont, J. A. Dunn, M. A. Hughes, D. M. A. Wallace, T. E. D. McDermott, R. Grainger, E. Rogers, M. Corcoran, H. Bredin, H. Grimes, D. Lanigan, C. Roobottom, P. A. Dubbins, R. G. Choa, T. Creagh, M. R. Butler, K. J. O’Flynn, R. P. MacDonagh, D. G. Thomas, K. Dawson, J. Aitken, B. Cooke, S. P. Parbhoo, P. M. Cannon, S. C. Low, A. Dixon, I. O. Ellis, C. W. Elston, R. W. Blarney, E. D. Mulligan, K. Cronin, A. Stack, J. Ennis, F. Abbaskoor, M. K. O’Donoghue, G. Fulton, W. A. Tanner, F. B. V. Keane, B. V. Joseph, F. O. Cunningham, M. Dowling, E. Conveney, J. G. Geraghty, P. Byrne, G. Clarke, J. Duffy, N. O’Higgins, D. O’Hanlon, P. G. Horgan, D. O’Brien, C. Phelan, P. Given, P. Kent, S. Sheehan, M. P. Colgan, D. Moore, G. Shanik, P. Murphy, R. Vashisht, M. Sian, P. Franks, M. K. O’Malley, Y. Gul, D. Waldron, W. P. Hederman, H. P. Singh, S. Dias, T. Aherne, D. J. Hehir, J. A. McKeever, C. A. Bannon, D. Mehigan, T. V. Keaveney, T. F. Browne, U. M. Sivananthan, M. R. Rees, S. Whittaker, G. A. Davies, R. Vashisght, E. Sharp, A. Coady, A. Sterpetti, R. M. Greenhalgh, D. P. O’Brien, D. B. Gough, M. C. Regan, I. E. Efron, S. I. Kirk, M. Hurson, H. L. Wasserkrug, A. Barbul, S. Haynes, J. Thornton, J. Sparkes, A. D. K. Hill, C. J. Kelly, J. Gallagher, L. Modyka, H. P. Redmond, J. M. Daly, O. M. Austin, R. J. Cunney, P. A. Grace, C. Curran, J. O’Donoghue, M. Abernathy, N. Sharpe, M. Lucy, E. W. D. McDermott, P. M. Mercer, N. J. O’Higgins, G. Murugasu, A. Groeschel, M. Carmody, J. Donohue, D. H. Osborne, M. McLaughlin, J. Devlin, J. P. Phillips, Y. Ellias, M. Tahir, J. McKeever, M. Tighe, V. Lynch, M. Ahmed, P. P. A. Smyth, A. M. Hetherton, P. Horgan, M. Little, D. S. Quill, C. O. Duncan, M. O’Donnell, J. A. E. Hobby, D. Little, M. Murphy, P. Burke, P. Broe, M. McKiernan, S. J. Kirk, J. Crowe, P. MacMathuna, J. Lennon, T. Corrigan, R. O’Connell, A. Browne, A. Quershi, A. Leahy, G. Courtney, P. Grace, H. Osborne, D. J. Buckley, M. Goggin, T. A. Farrell, J. Geraghty, F. K. Keeling, P. R. O’Connell, H. Naama, E. Moore, E. Barry, C. Duffy, P. Hogan, G. Nee, M. Fahy, D. P. Kenny, V. Ellias, E. Gibney, W. Joyce, E. Gaffney, J. McMahon, M. McCabe, P. Kelly, M. Leader, C. I. Timon, P. Gullane, I. Dardick, I. McCarthy, N. F. Couse, M. Morrin, and P. V. Delaney

Subjects
General Medicine
Published
1994
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49. Consistency of histopathological reporting of breast lesions detected by screening: findings of the U.K. National External Quality Assessment (EQA) Scheme. U. K. National Coordinating Group for Breast Screening Pathology

Author

J P, Sloane, R, Ellman, T J, Anderson, C L, Brown, J, Coyne, N S, Dallimore, J D, Davies, D, Eakins, I O, Ellis, and C W, Elston

Subjects
Observer Variation, Hyperplasia, Quality Assurance, Health Care, Carcinoma, Ductal, Breast, Breast Neoplasms, United Kingdom, Diagnosis, Differential, Breast Diseases, Humans, Mass Screening, Female, Neoplasm Invasiveness, Breast, Precancerous Conditions, Carcinoma in Situ
Abstract

The aim of the scheme was to determine consistency of histopathological reporting in the United Kingdom National Breast Screening Programme. This external quality assessment scheme involved 51 sets of 12 slides which were circulated to 186-251 pathologists at intervals of 6 months for 3 years. Participants recorded their diagnoses on standard reporting forms, which were submitted to the U.K. National Cancer Screening Evaluation Unit for analysis. A high level of consistency was achieved in diagnosing major categories of breast disease including invasive carcinoma and the important borderline lesions, radial scar and ductal carcinoma in situ (DCIS), the latter exceeding a national target set prior to the onset of the scheme. Atypical hyperplasia (AH) was reported with much less consistency although, where it was the majority opinion, over 86% of diagnoses were of benign disorders and only 14% were of DCIS. Inconsistency was encountered in subtyping and measuring DCIS, the former apparently due to current uncertainties about classification and the latter to poor circumscription, variation in size in different sections and merging with zones of AH. Reporting prognostic features of invasive carcinomas was variable. Measurement of size was achieved with adequate consistency except in a small number of very poorly circumscribed tumours. Grading and subtyping were inconsistent although the latter was not specifically tested and will be the subject of future study. Members of the National Coordinating Group achieved greater uniformity than the remainder of the participants in all diagnostic categories, but both groups experienced similar types of problem. Our findings suggest that participation in the scheme improves diagnostic consistency. In conclusion, consistency in diagnosing invasive carcinoma and radial scar is excellent, and good in DCIS, but improvements are desirable in diagnosing atypical hyperplasia, classifying DCIS and reporting certain prognostic features of invasive tumours. Such improvements will require further research, the development of improved diagnostic criteria and the dissemination of clearer guidelines.

Published
1994

50. Expression of tumour-associated antigens in breast cancer primary tissue compared with serum levels

Author

P M, Cannon, I O, Ellis, R W, Blamey, J, Bell, C W, Elston, and J F, Robertson

Subjects
Immunoenzyme Techniques, Antigens, Neoplasm, Biomarkers, Tumor, Antibodies, Monoclonal, Humans, Breast Neoplasms, Female, Middle Aged
Abstract

The level of expression of six breast cancer-associated antigens or markers (CEA, NCRC-11, HMFG1, HMFG2, D8 and DF3) in primary tumour tissue and patients' serum has been compared. Two-hundred-and-forty-five consecutive patients with newly-diagnosed breast cancer had tumour biopsy and serum samples taken prior to any anti-cancer therapy (Stage I and II disease n = 100, Stage III disease n = 60, Stage IV disease n = 85). No correlations were found between the level of tumour tissue staining and serum levels of the same antigens. Those samples from patients with Stage IV disease were also analysed separately but again no correlations were observed. Therefore the staining pattern of the primary tumour for these antigens is not a predictor of which tumour marker will be elevated in the serum.

Published
1993

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