Your search keyword '"Bockstal M"' showing total 5 results

1. Adenoid cystic carcinoma of the Bartholin gland is not HPV-related: A case report and review of literature

Author

Nieuwenhuyzen-de Boer, G.M., Dasgupta, S. (Shatavisha), Ewing, P.C. (Patricia), Bockstal, M. (Mieke) van, Nieuwenhuyzen-de Boer, G.M., Dasgupta, S. (Shatavisha), Ewing, P.C. (Patricia), and Bockstal, M. (Mieke) van

Abstract

Adenoid cystic carcinoma (ACC) of the Bartholin gland is a rare gynaecological entity. Despite its slow growth and inconspicuous presentation, vulvar ACC has a propensity for perineural invasion and is therefore associated with high local recurrence rates. We report a case of vulvar ACC in a 61-year-old woman with a prolonged swelling of the Bartholin gland. This patient presented with pulmonary metastases at the moment of histological diagnosis. The vulvar and the pulmonary lesions showed identical histology. Despite a history of human papilloma virus (HPV)-related usual type vulvar intra-epithelial neoplasia and cervical squamous cell carcinoma, the vulvar ACC was negative for both p16 immunoh

Published

2020

2. Granular dot-like staining with MLH1 immunohistochemistry is a clone-dependent artefact

Author

Dasgupta, S. (S.), Ewing, P.C. (Patricia), Groenendijk, F.H. (F. H.), Stam, O. (O.), Biermann, K. (Katharina), Doukas, M. (M.), Dubbink, H.J. (Erik Jan), Velthuysen, M.L.F. (Loes) van, Dinjens, W.N.M. (Winand), Bockstal, M. (Mieke) van, Dasgupta, S. (S.), Ewing, P.C. (Patricia), Groenendijk, F.H. (F. H.), Stam, O. (O.), Biermann, K. (Katharina), Doukas, M. (M.), Dubbink, H.J. (Erik Jan), Velthuysen, M.L.F. (Loes) van, Dinjens, W.N.M. (Winand), and Bockstal, M. (Mieke) van

Abstract

Immunohistochemistry (IHC) for DNA mismatch repair proteins MLH1, PMS2, MSH2, and MSH6 is used for microsatellite instability (MSI) screening in colorectal carcinoma (CRC) and endometrial carcinoma (EC). Loss of PMS2, with retained MLH1 staining occurs in germline mutations of PMS2 gene, and is an indication for genetic testing. We report a pitfall of immunohistochemical interpretation in an EC, initially regarded as MLH1-positive and PMS2-negative. Review of the MLH1-IHC (M1-clone) revealed a granular, dot-like, nuclear staining. On repeating the MLH1-IHC with a different clone (ES05-clone), complete negativity was noted, and on molecular testing, MLH1 promotor methylation was detected. The dot-like pattern was therefore adjudged a clone-dependent artefact. On reviewing the archived MLH1-IHC slides, we observed the same dot-like pattern in two CRCs; in both cases the M1-clone had been used. Awareness of this artefact may prevent reporting errors, and unnecessary referrals for germline mutation testing.

Published

2019

3. EXclusion of non-Involved uterus from the Target Volume (EXIT-trial): An individualized treatment for locally advanced cervical cancer using modern radiotherapy and imaging techniques

Author

Vandecasteele, K. (Katrien), Tummers, P. (Philippe), Bockstal, M. (Mieke) van, De Visschere, P. (Pieter), Vercauteren, T. (Tom), Gersem, W. (Werner) de, Denys, H. (Hannelore), Naert, E. (Eline), Makar, A. (A.), Neve, W. (Wilfried) de, Vandecasteele, K. (Katrien), Tummers, P. (Philippe), Bockstal, M. (Mieke) van, De Visschere, P. (Pieter), Vercauteren, T. (Tom), Gersem, W. (Werner) de, Denys, H. (Hannelore), Naert, E. (Eline), Makar, A. (A.), and Neve, W. (Wilfried) de

Abstract

Background: Definitive chemoradiotherapy is standard of care in locally advanced cervical cancer (LACC). Both toxicity and local relapse remain major concerns in this treatment. We hypothesize that a magnetic resonance imaging (MRI) based redefining of the radiotherapeutic target volume will lead to a reduction of acute and late toxicity. In our center, chemoradiotherapy followed by hysterectomy was implemented successfully in the past. This enables us to assess the safety of reducing the target volume but also to explore the biological effects of chemoradiation on the resected hysterectomy specimen. Methods: The EXIT-trial is a phase II, single arm study aimed at LACC patients. This study evaluates whether a MRI-based exclusion of the non-tumor-bearing parts of the uterus out of the target volume results in absence of tumor in the non-high doses irradiated part of the uterus in the hysterectomy specimen. Secondary endpoints include a dosimetric comparison of dose on normal tissue when comparing study treatment plans compared to treatment of the whole uterus at high doses; acute and chronic toxicity, overall survival, local relapse- and progression-free survival. In the translational part of the study, we will evaluate the hypothesis that the baseline apparent diffusion coefficient (ADC) values of diffusion weighted MRI and its evolution 2 weeks after start of CRT, for the whole tumor as well as for intra-tumoral regions, is prognostic for residual tumor on the hysterectomy specimen. Discussion: Although MRI is already used to guide target delineation in brachytherapy, the EXIT-trial is the first to use this information to guide target delineation in external beam radiotherapy. Early therapy resistance prediction using DW-MRI opens a window for early treatment adaptation or further dose-escalation on tumors/intratumoral regions at risk for treatment failure.

Published

2018

4. Dichotomous histopathological assessment of ductal carcinoma in situ of the breast results in substantial interobserver concordance

Author

Bockstal, M. (Mieke) van, Baldewijns, M. (Marcella), Colpaert, C. (Cécile), Dano, H. (Hélène), Floris, O.A.M., Galant, C. (Christine), Lambein, K. (K.), Peeters, D. (Dieter), Van Renterghem, S. (Sofie), Van Rompuy, A.-S. (Anne-Sophie), Verbeke, S.L.J. (Sofie), Verschuere, S. (Stephanie), Van Dorpe, J. (Jo), Bockstal, M. (Mieke) van, Baldewijns, M. (Marcella), Colpaert, C. (Cécile), Dano, H. (Hélène), Floris, O.A.M., Galant, C. (Christine), Lambein, K. (K.), Peeters, D. (Dieter), Van Renterghem, S. (Sofie), Van Rompuy, A.-S. (Anne-Sophie), Verbeke, S.L.J. (Sofie), Verschuere, S. (Stephanie), and Van Dorpe, J. (Jo)

Abstract

Aims: Robust prognostic markers for ductal carcinoma in situ (DCIS) of the breast require high reproducibility and thus low interobserver variability. The aim of this study was to compare interobserver variability among 13 pathologists, in order to enable the identification of robust histopathological characteristics. Methods and results: One representative haematoxylin and eosin-stained slide was selected for 153 DCIS cases. All pathologists independently assessed nuclear grade, intraductal calcifications, necrosis, solid growth, stromal changes, stromal

Published

2018

5. APOBEC3G expression correlates with T-cell infiltration and improved clinical outcomes in high-grade serous ovarian carcinoma

Author

Leonard, B. (Brandon), Starrett, G.J. (Gabriel J.), Maurer, M.J. (Matthew J.), Oberg, A.L. (Ann L.), Van Bockstal, M. (Mieke), Van Dorpe, J. (Jo), De Wever, O. (Olivier), Helleman, J. (Jozien), Sieuwerts, A.M. (Anieta), Berns, P.M.J.J. (Els), Martens, J.W.M. (John), Anderson, B.D. (Brett D.), Brown, W.L. (William L.), Kalli, K.R. (Kimberly R.), Kaufmann, S.H. (Scott H.), Harris, R.S. (Reuben), Leonard, B. (Brandon), Starrett, G.J. (Gabriel J.), Maurer, M.J. (Matthew J.), Oberg, A.L. (Ann L.), Van Bockstal, M. (Mieke), Van Dorpe, J. (Jo), De Wever, O. (Olivier), Helleman, J. (Jozien), Sieuwerts, A.M. (Anieta), Berns, P.M.J.J. (Els), Martens, J.W.M. (John), Anderson, B.D. (Brett D.), Brown, W.L. (William L.), Kalli, K.R. (Kimberly R.), Kaufmann, S.H. (Scott H.), and Harris, R.S. (Reuben)

Abstract

__Purpose:__ APOBEC3 DNA cytosine deaminase family members normally defend against viruses and transposons. However, deregulated APOBEC3 activity causes mutations in cancer. Because of broad expression profiles and varying mixtures of normal and cancer cells in tumors, including immune cell infiltration, it is difficult to determine where different APOBEC3s are expressed. Here, we ask whether correlations exist between APOBEC3 expression and T-cell infiltration in high-grade serous ovarian cancer (HGSOC), and assess whether these correlations have prognostic value. __Experimental Design:__ Transcripts for APOBEC3G, APOBEC3B, and the T-cell markers, CD3D, CD4, CD8A, GZMB, PRF1, and RNF128 were quantified by RT-qPCR for a cohort of 354 HGSOC patients. Expression values were correlated with each other and clinical parameters. Two additional cohorts were used to extend HGSOC clinical results. Immunoimaging was used to colocalize APOBEC3G and the T-cell marker CD3. TCGA data extended expression analyses to additional cancer types. __Results:__ A surprising positive correlation was found for expression of APOBEC3G and several T cell genes in HGSOC. Immunohistochemistry and immunofluorescent imaging showed protein colocalization in tumor-infiltrating T lymphocytes. High APOBEC3G expression correlated with improved outcomes in multiple HGSOC cohorts. TCGA data analyses revealed that expression of APOBEC3D and APOBEC3H also correlates with CD3D across multiple cancer types. __Conclusions:__ Our results identify APOBEC3G as a new candidate biomarker for tumor-infiltrating T lymphocytes and favorable prognoses for HGSOC. Our data also highlight the complexity of the tumor environment with respect to differential APOBEC family gene expression in both tumor and surrounding normal cell types. Clin Cancer Res; 22(18); 4746-55.

Published

2016