Your search keyword '"Karrenbeld, A"' showing total 11 results

1. Locoregional Residual Esophageal Cancer after Neo-adjuvant Chemoradiotherapy and Surgery Regarding Anatomic Site and Radiation Target Fields: A Histopathologic Evaluation Study.

Author

Faiz, Zohra, Kats-Ugurlu, Gursah, Mui, Véronique E. M., Karrenbeld, Arend, Burgerhof, Hans G. M., Plukker, John T. M., and Muijs, Christel T.

Abstract

Objective: Neoadjuvant chemoradiotherapy followed by surgery establishes a considerable pathologic complete response (pCR) in EC. The aim was to determine site of residual tumor and its prognostic impact. Summary Background Data: High rates of residual tumor in the adventitial region even inside the radiation fields will influence current decision-making. Methods: We evaluated resection specimens with marked target fields from 151 consecutive EC patients treated with carboplatin/paclitaxel and 41.4Gy between 2009 and 2018. Results: In radically resected (R0) specimens 19.8% (27/136) had a pCR (ypT0N0) and 14% nearly no response (tumor regression grade: tumor regression grade 4–5). Residual tumor commonly extended in or restricted to the adventitia (43.1%; 47/109), whereas 7.3% was in the mucosa (ypT1a), 16.5% in the submucosa (ypT1b) and 6.4% only in lymph nodes (ypT0N+). Macroscopic residues in R0-specimens of partial responders (tumor regression grade 2-3: N = 90) were found in- and outside the gross tumor volume (GTV) in 33.3% and 8.9%, and only microscopic in- and outside the clinical target volume in 58.9% and 1.1%, respectively. Residual nodal disease was observed proximally and distally to the clinical target volume in 2 and 5 patients, respectively. Disease Free Survival decreased significantly if macroscopic tumor was outside the GTV and in ypT2-4aN+. Conclusions: After neoadjuvant chemoradiotherapy, pCR and ypT1aN0 were seen in a limited number of R0 resected specimens (19.8% and 7.3%, respectively), whereas 6.4% had only nodal disease (yT0N+). Disease Free Survival decreased significantly if macroscopic residue was outside the GTV and in responders with only nodal disease. Therefore, we should be cautious in applying wait and see strategies. [ABSTRACT FROM AUTHOR]

Published

2022

2. Diffuse enteritis after colectomy for ulcerative colitis: two case reports and review of the literature.

Author

Corporaal S, Karrenbeld A, van der Linde K, Voskuil JH, Kleibeuker JH, and Dijkstra G

Published

2009

3. Impact of the Number of Histologically Examined Lymph Nodes on Prognosis in Colon Cancer.

Author

Kelder, Wendy, Inberg, Bas, Schaapveld, Michael, Karrenbeld, Arend, Grond, Joris, Wiggers, Theo, and Plukker, John T.

Published

2009

4. High-grade dysplasia in sporadic fundic gland polyps: a case report and review of the literature.

Author

Jalving, Mathilde, Koornstra, Jan J, Götz, Jan M, van der Waaij, Laurens A, de Jong, Steven, Zwart, Nynke, Karrenbeld, Arend, and Kleibeuker, Jan H

Published

2003

5. Prognostic Significance of K-ras and TP53 Mutations in the Role of Adjuvant Chemotherapy on Survival in Patients with Dukes C Colon Cancer.

Author

Bleeker, W. A., Hayes, V. M., Karrenbeld, A., Hofstra, R. M. W., Verlind, E., Hermans, J., Poppema, S., Buys, C. H. C. M., and Plukker, J. Th. M.

Abstract

PURPOSE: Mutations in K-ras and TP53 genes are common in colorectal cancer. They affect biologic behavior and might influence chemotherapy susceptibility in these tumors. We investigated whether the survival of patients with Dukes C colon cancer treated with adjuvant chemotherapy is influenced by K-ras and TP53 mutations. METHODS: Mutation screening of the hot spots of the K-ras gene and of the evolutionarily conserved regions of the TP53 gene was performed by denaturing gradient gel electrophoresis technique in formalin-fixed paraffin-embedded specimens of 55 consecutive patients with Dukes C colon cancer treated with adjuvant 5-fluorouracil-based chemotherapy. The median follow-up was 47 (range, 32-66) months. RESULTS: Alterations in the mutation hot spots of K-ras were found at codon 12 (n = 11) and 13 (n = 4) in 15 of the 55 carcinomas (27 percent). No mutation was found at codon 61. Mutations of a probably causative nature in the evolutionarity conserved regions (exons 5-8) of the TP53 gene were found in 24 tumors (44 percent). K-ras and TP53 mutations were found equally in the group with recurrent disease (7/26 (26 percent) and 12/27 (44 percent), respectively) and in the group without recurrences (8/28 (24 percent) and 12/28 (43 percent), respectively). Cancer-specific survival did not differ significantly between patients with K-ras or TP53 or both mutated and nonmutated tumors, respectively (log-rank test: K-ras, P = 0.72 and TP53, P = 0.77: K-ras and TP53, P = 0.8). Also, potentially aggressive K-ras codon 12 and 13 mutations had the same survival as tumors without these mutations (log-rank test; P = 0.73). CONCLUSIONS: Patients with K-ras or TP53 or both mutated Dukes C colon tumors have the same survival as nonmutated tumors when treated with adjuvant chemotherapy. These data suggest that mutations in K-ras or TP53 alone are not prognostic indicators in patients with Dukes C colon cancer receiving adjuvant 5-Fluorouracil-based therapy. [ABSTRACT FROM AUTHOR]

Published

2001

6. Comprehensive TP53-Denaturing Gradient Gel Electrophoresis Mutation Detection Assay Also Applicable to Archival Paraffin-Embedded Tissue.

Author

Hayes, Vanessa M., Bleeker, Wim, Verlind, Edwin, Timmer, Tineke, Karrenbeld, Arend, Plukker, John T., Marx, Munro P., Hofstra, Robert M. W., and Buys, Charles H. C. M.

Published

1999

7. Clinical relevance of transforming growth factor α, epidermal growth factor receptor, p53, and Ki67 in colorectal liver metastases and corresponding primary tumors.

Author

De Jong, Koert P., Stellema, Rudi, Karrenbeld, Arend, Koudstaal, Jan, Gouw, Annette S., Sluiter, Wim J., Peeters, Paul M. J. G., Slooff, Maarten J. H., and De Vries, Elisabeth G. E.

Published

1998

8. Colonic epithellal cell proliferation throughout the colon is not affected by supplementary calcium or resistant starch in adenoma patients.

Author

van Gorkom, B. A.P., Karrenbeld, A., van der Meer, R., de Vries, E. G.E., and Kleibeuker, J. H.

Published

1999

9. Sennoside laxatives induce apoptosis of colonlc epithelial cells by a p53, p21/WAF mediated pathway.

Author

van Gorkom, B. A.P., Karrenbeld, A., de Vries, E. G.E., and Kleibeuker, J. H.

Published

1998

10. High frequency of hMSH6 mutations in patients with MSI-low tumors.

Author

Berends, M. J.W., Wu, Y., Sijmons, R. H., Hollema, H., Karrenbeld, A., van der Zee, A. G.J., Buys, C. H.C.M., Hofstra, R. M.W., and Kleibeuker, J. H.

Published

1998

11. Epithelial cell proliferative activity of Barrett's esophagus.

Author

Peters, F. T. M., Ganesh, S., Kuipers, E. J., de Jager-Krikken, A., Karrenbeld, A., Harms, G., Sluiter, W. J., Koudstaal, J., Klinkenberg-Knol, E. C., Lamers, C. B. H. W., and Kleibeuker, J. H.

Published

1998