Neuroendocrine tumors: A European view

Buchanan, K. D.; Johnston, C.F.; O'Hare, M.M.T.; Ardill, Joy; Shaw, Christopher E.; Collins, J. S. A.; Watson, Ronald G.; Atkinson, A. B.; Hadden, David R.; Kennedy, T. L.; Sloan, James M.

doi:10.1016/0002-9343(86)90581-4

Cited by 150 publications

(68 citation statements)

References 12 publications

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“…This tumor register was established in 1978 by the Department of Medicine, the Queen's University understanding of the molecular genetics of cancer, and many of these advances have stemmed from studof Belfast. 1 Detailed clinicopathologic data on patients (including age, gender, symptoms, tumor location, tuies of cellular oncogenes and tumor-suppressor genes. Several oncogenes have been well studied over the mor size, and occurrence of metastases) were available, and each patient's clinical progress had been years and characterized with regard to their roles in the development of specific human tumors.…”

Section: Patientsmentioning

confidence: 99%

“…About one-third of PNTs fail to produce study, we have analyzed, by immunohistochemistry using monoclonal antibodies, the expression of five any hormone-related syndrome and are therefore described as nonfunctioning. 1 Carcinoid tumors are the dominant oncogenes-c-myc, bcl-2, c-erb B-2, c-erb B-3, and c-jun-in a retrospective series of 116 primost common of the gastrointestinal tract (GI) neuroendocrine neoplasms and account for 55-86% of all mary human GPNTs, including islet cell tumors of the pancreas and carcinoids of foregut, midgut, and hindsuch tumors. 3,4 According to the site of origin, carcinoid tumors have been classified as tumors of the foregut origin, and we have attempted to correlate this expression with the clinicopathologic outcome of the gut (bronchus, pancreas, stomach, and proximal duodenum), midgut (distal duodenum, jejunum, ileum, disease.…”

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confidence: 99%

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Oncogene expression in gastroenteropancreatic neuroendocrine tumors

Wang¹,

Johnston²,

Buchanan³

1997

Cancer

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Section: Patientsmentioning

confidence: 99%

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Oncogene expression in gastroenteropancreatic neuroendocrine tumors

Wang¹,

Johnston²,

Buchanan³

1997

Cancer

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“…1,2 The molecular mechanisms of neuroendocrine tumors are poorly understood but have been the focus of many recent reports. [3][4][5][6][7][8][9][10] The methylation of cytosine in CpG dinucleotides is an important epigenetic modification of DNA in the vertebrate genome.…”

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confidence: 99%

Hypomethylation of LINE-1 and Alu in well-differentiated neuroendocrine tumors (pancreatic endocrine tumors and carcinoid tumors)

et al. 2007

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Neuroendocrine tumors including carcinoid tumors and pancreatic endocrine tumors are uncommon, and the genetic alterations in these indolent tumors are not well characterized. We studied global hypomethylation by analyzing long interspersed nucleotide elements (LINE)-1 and Alu methylation using pyrosequencing in 35 neuroendocrine tumors and corresponding normal tissue. The tumor samples were less methylated than normal tissue at LINE-1 (P ¼ 0.04) and Alu (P ¼ 0.001). The mean relative tumor hypomethylation (difference in methylation between normal tissue and in tumor) was 11.5710.0 for LINE-1 and 5.876.4 for Alu, and were correlated with each other (correlation coefficient 0.6, P ¼ 0.001). Relative tumor hypomethylation of LINE-1 was higher in ileal carcinoid tumors than in non-ileal carcinoid tumors and pancreatic endocrine tumors (P ¼ 0.047), and tumors with lymph node metastasis (P ¼ 0.02), chromosome 18 loss (P ¼ 0.001) and RAS-association domain family 1, isoform A gene methylation (P ¼ 0.02). Alu methylation in tumors was inversely correlated with methylation of O 6 -methyl-guanine methyltransferase gene (P ¼ 0.02). Our study shows that hypomethylation is more common in carcinoid tumors than in pancreatic endocrine tumors and is associated with clinicopathologic features, and genetic and epigenetic alterations in these tumors, including lymph node metastasis.

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“…In this case, the derivative cells may dynamically undergo a caricatural differentiation that may resemble epithelial, glandular, or neuroendocrine cells. On the basis of different kinds and levels of molecular and genetic alterations, these cells may follow distinct differentiation pathways and may stop their distinct differentiation programmes at different stages of maturation (Buchanan et al, 1986;Hansson and Abrahamsson, 2003;Wright et al, 2003;Bishop, 2005;Long et al, 2005). Respiratory, gastroenteric, and urinary tracts, as well as the prostate, are physiologically under strict neurovegetative control, and so it is not surprising that the majority of neuroendocrine tumours arise in these anatomic sites.…”

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confidence: 99%

“…In some cases, they may be very difficult to recognise because there is no single marker to identify an undifferentiated neuroendocrine tumour; so, diagnosis must rely on the correct interpretation of pathological data (histology, immunohistochemistry, and sometimes electronic microscopy), biohumoral studies, blood/urinary tests, biological behaviour of the neoplasia, the natural history and the progression of the disease, and patients' symptoms (Wiedenmann and Huttner, 1989;Polak, 1993;Nicholson and Ryan, 2000;De Lellis, 2001;Bishop, 2005). Neuroendocrine tumours may arise with clinically different modalities and signs (paraneoplastic syndromes), which are often related to the different degrees of biological aggressiveness and to the different levels of production of specific hormones and peptides (Buchanan et al, 1986;Moertel, 1987). When well differentiated, they retain a low level of local and metastatic aggressiveness.…”

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Chemo-hormone therapy of non-well-differentiated endocrine tumours from different anatomic sites with cisplatinum, etoposide and slow release lanreotide formulation

et al. 2007

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We report the results of a phase II trial in patients with metastatic endocrine tumours from different sites, which aimed to evaluate the anti-tumour activity and toxicity of a cisplatinum and etoposide regimen administered in combination with the somatostatin agonist lanreotide given in slow release formulation. Between January 1999 and November 2003, 27 patients with histological diagnoses of endocrine tumours with different degrees of differentiation, excluding well differentiated carcinoid neoplasms, received intravenous (i.v.) administration of cisplatinum (30 mg m À2 ) and etoposide (100 mg m À2 ) on days 1 -3 and intramuscular administration of 60 mg lanreotide on day 1, in a 21-day cycle. All of the patients were evaluable for toxicity and response. The treatment was very well tolerated as no grade 4 toxicity was observed. Four patients achieved a complete response, six a partial response, 12 experienced disease stabilisation and five disease progression. The average time to progression and to survival were 9 and 24 months respectively. These results suggest that this chemo-hormone therapy regimen is well tolerated and active in patients with non-well differentiated endocrine tumours.

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Neuroendocrine tumors: A European view

Cited by 150 publications

References 12 publications

Oncogene expression in gastroenteropancreatic neuroendocrine tumors

Oncogene expression in gastroenteropancreatic neuroendocrine tumors

Hypomethylation of LINE-1 and Alu in well-differentiated neuroendocrine tumors (pancreatic endocrine tumors and carcinoid tumors)

Chemo-hormone therapy of non-well-differentiated endocrine tumours from different anatomic sites with cisplatinum, etoposide and slow release lanreotide formulation

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