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14 results on '"Meijers, R.W.J."'

2. NTRK rearrangements in a subset of NF1-related malignant peripheral nerve sheath tumors as novel actionable target.

Author

Hiemcke-Jiwa, L.S., Meister, M.T., Martin, E., Dierselhuis, M.P., Haveman, L.M., Meijers, R.W.J., Tops, B.B.J., Wesseling, P., Diest, P.J. van, Gorp, J.M. van, Hehir, J.Y., Belzen, I.A.E.M. van, Bonenkamp, J.J., Noesel, M.M. van, Flucke, U.E., Kester, L.A., Hiemcke-Jiwa, L.S., Meister, M.T., Martin, E., Dierselhuis, M.P., Haveman, L.M., Meijers, R.W.J., Tops, B.B.J., Wesseling, P., Diest, P.J. van, Gorp, J.M. van, Hehir, J.Y., Belzen, I.A.E.M. van, Bonenkamp, J.J., Noesel, M.M. van, Flucke, U.E., and Kester, L.A.

Abstract

01 januari 2023, Item does not contain fulltext

Published
2023

3. Formalin-Fixed, Paraffin-Embedded-Targeted Locus Capture: A Next-Generation Sequencing Technology for Accurate DNA-Based Gene Fusion Detection in Bone and Soft Tissue Tumors.

Author

Stelloo, E., Meijers, R.W.J., Swennenhuis, J.F., Allahyar, A., Hajo, K., Cangiano, M., Leng, W.W.J. de, Helvert, S. van, Meulen, J. van der, Creytens, D., Kempen, L.C. van, Cleton-Jansen, A.M., Bovee, J.V.M.G., Laat, W. de, Splinter, E., Feitsma, H., Stelloo, E., Meijers, R.W.J., Swennenhuis, J.F., Allahyar, A., Hajo, K., Cangiano, M., Leng, W.W.J. de, Helvert, S. van, Meulen, J. van der, Creytens, D., Kempen, L.C. van, Cleton-Jansen, A.M., Bovee, J.V.M.G., Laat, W. de, Splinter, E., and Feitsma, H.

Abstract

Contains fulltext : 296779.pdf (Publisher’s version ) (Open Access), Chromosomal rearrangements are important drivers in cancer, and their robust detection is essential for diagnosis, prognosis, and treatment selection, particularly for bone and soft tissue tumors. Current diagnostic methods are hindered by limitations, including difficulties with multiplexing targets and poor quality of RNA. A novel targeted DNA-based next-generation sequencing method, formalin-fixed, paraffin-embedded-targeted locus capture (FFPE-TLC), has shown advantages over current diagnostic methods when applied on FFPE lymphomas, including the ability to detect novel rearrangements. We evaluated the utility of FFPE-TLC in bone and soft tissue tumor diagnostics. FFPE-TLC sequencing was successfully applied on noncalcified and decalcified FFPE samples (n = 44) and control samples (n = 19). In total, 58 rearrangements were identified in 40 FFPE tumor samples, including three previously negative samples, and none was identified in the FFPE control samples. In all five discordant cases, FFPE-TLC could identify gene fusions where other methods had failed due to either detection limits or poor sample quality. FFPE-TLC achieved a high specificity and sensitivity (no false positives and negatives). These results indicate that FFPE-TLC is applicable in cancer diagnostics to simultaneously analyze many genes for their involvement in gene fusions. Similar to the observation in lymphomas, FFPE-TLC is a good DNA-based alternative to the conventional methods for detection of rearrangements in bone and soft tissue tumors.

Published
2023

5. Multicenter Comparison of Molecular Tumor Boards in The Netherlands: Definition, Composition, Methods, and Targeted Therapy Recommendations

Author

Koopman, B., Groen, H.J.M., Ligtenberg, M.J.L., Grünberg, K., Monkhorst, K., Langen, A.J. de, Boelens, M.C., Paats, M.S., Thüsen, J.H. von der, Dinjens, W.N., Solleveld, N., Wezel, T. van, Gelderblom, H., Hendriks, L.E., Speel, E.M., Theunissen, T.E.J., Kroeze, L., Mehra, N., Piet, B., Wekken, A.J. van der, Elst, A. Ter, Timens, W., Willems, S.M., Meijers, R.W.J., Leng, W.W.J. de, Lindert, A.S.R. van, Radonic, T., Hashemi, S.M., Heideman, D. A. M., Schuuring, E., Kempen, L.C. van, Koopman, B., Groen, H.J.M., Ligtenberg, M.J.L., Grünberg, K., Monkhorst, K., Langen, A.J. de, Boelens, M.C., Paats, M.S., Thüsen, J.H. von der, Dinjens, W.N., Solleveld, N., Wezel, T. van, Gelderblom, H., Hendriks, L.E., Speel, E.M., Theunissen, T.E.J., Kroeze, L., Mehra, N., Piet, B., Wekken, A.J. van der, Elst, A. Ter, Timens, W., Willems, S.M., Meijers, R.W.J., Leng, W.W.J. de, Lindert, A.S.R. van, Radonic, T., Hashemi, S.M., Heideman, D. A. M., Schuuring, E., and Kempen, L.C. van

Abstract

Item does not contain fulltext, BACKGROUND: Molecular tumor boards (MTBs) provide rational, genomics-driven, patient-tailored treatment recommendations. Worldwide, MTBs differ in terms of scope, composition, methods, and recommendations. This study aimed to assess differences in methods and agreement in treatment recommendations among MTBs from tertiary cancer referral centers in The Netherlands. MATERIALS AND METHODS: MTBs from all tertiary cancer referral centers in The Netherlands were invited to participate. A survey assessing scope, value, logistics, composition, decision-making method, reporting, and registration of the MTBs was completed through on-site interviews with members from each MTB. Targeted therapy recommendations were compared using 10 anonymized cases. Participating MTBs were asked to provide a treatment recommendation in accordance with their own methods. Agreement was based on which molecular alteration(s) was considered actionable with the next line of targeted therapy. RESULTS: Interviews with 24 members of eight MTBs revealed that all participating MTBs focused on rare or complex mutational cancer profiles, operated independently of cancer type-specific multidisciplinary teams, and consisted of at least (thoracic and/or medical) oncologists, pathologists, and clinical scientists in molecular pathology. Differences were the types of cancer discussed and the methods used to achieve a recommendation. Nevertheless, agreement among MTB recommendations, based on identified actionable molecular alteration(s), was high for the 10 evaluated cases (86%). CONCLUSION: MTBs associated with tertiary cancer referral centers in The Netherlands are similar in setup and reach a high agreement in recommendations for rare or complex mutational cancer profiles. We propose a "Dutch MTB model" for an optimal, collaborative, and nationally aligned MTB workflow. IMPLICATIONS FOR PRACTICE: Interpretation of genomic analyses for optimal choice of target therapy for patients with cancer is becoming in

Published
2021

6. Multicenter Comparison of Molecular Tumor Boards in The Netherlands: Definition, Composition, Methods, and Targeted Therapy Recommendations

Author

Koopman, B. (Bart), Groen, H.J.M. (Henk), Ligtenberg, M.J. (Marjolijn), Grünberg, K. (Katrien), Monkhorst, K. (Kim), de Langen, A.J. (Adrianus J.), Boelens, M.C. (Mirjam C.), Paats, M.S. (Marthe), Thusen, J.H. (Jan) von der, Dinjens, W.N.M. (Winand), Solleveld, N. (Nienke), Wezel, T. (Tom) van, Gelderblom, H. (Hans), Hendriks, L.E. (Lizza E.), Speel, E.J. (Ernst-Jan), Theunissen, T.E. (Tom E.), Kroeze, L.I. (Leonie I.), Mehra, N. (Niven), Piet, B. (Berber), van der Wekken, A.J. (Anthonie J.), ter Elst, A. (Arja), Timens, W. (Wim), Willems, S.M. (Stefan Martin), Meijers, R.W.J. (Ruud), Leng, W.W.J. (Wendy) de, van Lindert, A.S.R. (Anne S.R.), Radonic, T. (Teodora), Hashemi, S.M.S. (Sayed M.S.), Heideman, D.A.M. (Danielle), Schuuring, E. (Ed), Kempen, L.C. (Leon), Koopman, B. (Bart), Groen, H.J.M. (Henk), Ligtenberg, M.J. (Marjolijn), Grünberg, K. (Katrien), Monkhorst, K. (Kim), de Langen, A.J. (Adrianus J.), Boelens, M.C. (Mirjam C.), Paats, M.S. (Marthe), Thusen, J.H. (Jan) von der, Dinjens, W.N.M. (Winand), Solleveld, N. (Nienke), Wezel, T. (Tom) van, Gelderblom, H. (Hans), Hendriks, L.E. (Lizza E.), Speel, E.J. (Ernst-Jan), Theunissen, T.E. (Tom E.), Kroeze, L.I. (Leonie I.), Mehra, N. (Niven), Piet, B. (Berber), van der Wekken, A.J. (Anthonie J.), ter Elst, A. (Arja), Timens, W. (Wim), Willems, S.M. (Stefan Martin), Meijers, R.W.J. (Ruud), Leng, W.W.J. (Wendy) de, van Lindert, A.S.R. (Anne S.R.), Radonic, T. (Teodora), Hashemi, S.M.S. (Sayed M.S.), Heideman, D.A.M. (Danielle), Schuuring, E. (Ed), and Kempen, L.C. (Leon)

Abstract

Background: Molecular tumor boards (MTBs) provide rational, genomics-driven, patient-tailored treatment recommendations. Worldwide, MTBs differ in terms of scope, composition, methods, and recommendations. This study aimed to assess differences in methods and agreement in treatment recommendations among MTBs from tertiary cancer referral centers in The Netherlands. Materials and Methods: MTBs from all tertiary cancer referral centers in The Netherlands were invited to participate. A survey assessing scope, value, logistics, composition, decision-making method, reporting, and registration of the MTBs was completed through on-site interviews with members from each MTB. Targeted therapy recommendations were compared using 10 anonymized cases. Participating MTBs were asked to provide a treatment recommendation in accordance with their own methods. Agreement was based on which molecular alteration(s) was considered actionable with the next line of targeted therapy. Results: Interviews with 24 members of eight MTBs revealed that all participating MTBs focused on rare or complex mutational cancer profiles, operated independently of cancer type–specific multidisciplinary teams, and consisted of at least (thoracic and/or medical) oncologists, pathologists, and clinical scientists in molecular pathology. Differences were the types of cancer discussed and the methods used to achieve a recommendation. Nevertheless, agreement among MTB recommendations, based on identified actionable molecular alteration(s), was high for the 10 evaluated cases (86%). Conclusion: MTBs associated with tertiary cancer referral centers in The Netherlands are similar in setup and reach a high agreement in recommendations for rare or complex mutational cancer profiles. We propose a “Dutch MTB model” for an optimal, collaborative, and nationally aligned MTB workflow. Implications for Practice: Interpretation of genomic analyses for optimal choice of target therapy for patients with cancer is becoming in

Published
2020
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7. Comel-Netherton syndrome: A local skin barrier defect in the absence of an underlying systemic immunodeficiency

Author

Stuvel, K. (Kira), Heeringa, J.J. (Jorn), Dalm, V.A.S.H. (Virgil), Meijers, R.W.J. (Ruud), Hoffen, E. (Els) van, Gerritsen, S.A.M. (Susan A. M.), Zelm, M.C. (Menno) van, Pasmans, S.G.M.A. (Suzanne), Stuvel, K. (Kira), Heeringa, J.J. (Jorn), Dalm, V.A.S.H. (Virgil), Meijers, R.W.J. (Ruud), Hoffen, E. (Els) van, Gerritsen, S.A.M. (Susan A. M.), Zelm, M.C. (Menno) van, and Pasmans, S.G.M.A. (Suzanne)

Abstract

Background: Comel-Netherton syndrome (NS) is a rare autosomal disease, characterized by severe skin disease, hair shaft defects, atopic diathesis, and increased susceptibility for skin infections. Since patients with NS suffer from recurrent infections, it has been hypothesized that an underlying immunodeficiency attributes to this. Here, we studied clinical and immunological characteristics of the cohort of NS patients in the Netherlands in order to identify whether potential immunodeficiencies result in the increased risk of infectious complications. Methods: Phenotypes were scored for severity of skin condition, specific hair shaft defects, atopy, and recurrent infections. Patients’ blood samples were collected for quantification of serum immunoglobulin (Ig) levels, specific antibodies against Streptococcus pneumoniae, and allergen-specific IgE, as well as detailed immunophenotyping of blood leukocyte and lymphocyte subsets by flow cytometry. Results: A total of 14 patients were included with age range 3-46 years and varying degrees of skin involvement. All patients presented with atopic symptoms (food allergy, n = 13; hay fever, n = 10; asthma, n = 7). Recurrent skin infections were common, particularly in childhood (n = 12). Low levels of specific antibodies against S pneumoniae were found in 10 of 11 evaluated patients. Detailed immunological analysis was performed on 9 adult patients. Absolute numbers of lymphocyte subsets and serum immunoglobulin levels were all within normal ranges. Conclusion: Multidisciplinary evaluation of our national cohort showed no evidence for a severe, clinically relevant systemic immunodeficiency. Therefore, we conclude that in Dutch NS patients the increased risk of infections most likely results from the skin barrier disruption and that increased allergen penetration predisposes to allergic sensitization.

Published
2020
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8. One-fits-all pretreatment protocol facilitating Fluorescence in Situ Hybridization on formalin-fixed paraffin-embedded, fresh frozen and cytological slides

Author

Richardson, S.O. (Shivanand O.), Huibers, M.M.H. (Manon M. H.), Weger, R.A. (Roel) de, Leng, W.W.J. (Wendy) de, Hinrichs, J.W.J. (John W.J.), Meijers, R.W.J. (Ruud W. J.), Willems, S.M. (Stefan Martin), Peeters, T.L.M.G. (Ton L. M. G.), Richardson, S.O. (Shivanand O.), Huibers, M.M.H. (Manon M. H.), Weger, R.A. (Roel) de, Leng, W.W.J. (Wendy) de, Hinrichs, J.W.J. (John W.J.), Meijers, R.W.J. (Ruud W. J.), Willems, S.M. (Stefan Martin), and Peeters, T.L.M.G. (Ton L. M. G.)

Abstract

Background: The Fluorescence In Situ Hybridization (FISH) technique is a very useful tool for diagnostic and prognostic purposes in molecular pathology. However, clinical testing on patient tissue is challenging due to variables of tissue processing that can influence the quality of the results. This emphasizes the necessity of a standardized FISH protocol with a high hybridization efficiency. We present a pretreatment protocol that is easy, reproducible, cost-effective, and facilitates FISH on all types of patient material simultaneously with good quality results. During validation, FISH analysis was performed simultaneously on formalin-fixed paraffin-embedded, fresh frozen and cytological patient material in combination with commercial probes using our optimized one-fits-all pretreatment protocol. An optimally processed sample is characterized by strong specific signals, intact nuclear membranes, non-disturbing autofluorescence and a homogeneous DAPI staining. Results: In our retrospective cohort of 3881 patient samples, overall 93% of the FISH samples displayed good quality results leading to a patient diagnosis. All FISH were assessed on quality aspects such as adequacy and consistency of signal strength (brightness), lack of background and / or cross-hybridization signals, and additionally the presence of appropriate control signals were evaluated to assure probe accuracy. In our analysis 38 different FISH probes from 3 commercial manufacturers were used (Cytocell, Vysis and ZytoLight). The majority of the patients in this cohort displayed good signal quality and barely non-specific background fluorescence on all tissue types independent of which commercial probe was used. Conclusion: The optimized one-fits-all FISH method is robust, reliable and reproducible to deliver an accurate result for patient diagnostics in a lean workflow and cost-effective manner. This protocol can be used for widespread application in cancer and non-cancer diagnostics and research.

Published
2019
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9. Lo of CD28 on peripheral T cells decreases the risk for early acute rejection after kidney transplantation

Author

Dedeoğlu, B. (Burç), Meijers, R.W.J. (Ruud), Klepper, M. (Mariska), Heelink, D.A. (Dennis A.), Baan, C.C. (Carla), Litjens, N.H.R. (Nicolle), Betjes, M.G.H. (Michiel), Dedeoğlu, B. (Burç), Meijers, R.W.J. (Ruud), Klepper, M. (Mariska), Heelink, D.A. (Dennis A.), Baan, C.C. (Carla), Litjens, N.H.R. (Nicolle), and Betjes, M.G.H. (Michiel)

Abstract

Background End-stage renal disease patients have a dysfunctional, prematurely aged peripheral T-cell system. Here we hypothesized that the degree of premature T-cell ageing before kidney transplantation predicts the risk for early acute allograft rejection (EAR). Methods 222 living donor kidney transplant recipients were prospectively analyzed. EAR was defined as biopsy proven acute allograft rejection within 3 months after kidney transplantation. The differentiation status of circulating T cells, the relative telomere length and the number of CD31+ naive T cells were determined as T-cell ageing parameters. Results Of the 222 patients analyzed, 30 (14%) developed an EAR. The donor age and the historical panel reactive antibody score were significantly higher (p = 0.024 and p = 0.039 respectively) and the number of related donor kidney transplantation was significantly lower (p = 0.018) in the EAR group. EAR-patients showed lower CD4+CD28null T-cell numbers (p<0.01) and the same trend was observed for CD8+CD28null T-cell numbers (p = 0.08). No differences regarding the other ageing parameters were found. A multivariate Cox regreion analysis showed that higher CD4+CD28null T-cell numbers was aociated with a lower risk for EAR (HR: 0.65, p = 0.028). In vitro, a significant lower percentage of alloreactive T cells was observed within CD28null T cells (p<0.001). Conclusion Immunological ageing-related expansion of highly differentiated CD28null T cells is aociated with a lower risk for EAR.

Published
2016
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12. Cytomegalovirus contributes partly to uraemia-associated premature immunological ageing of the T cell compartment

Author

Meijers, R.W.J. (Ruud), Litjens, N.H.R. (Nicolle), Wit, E.A. (Elly) de, Langerak, A.W. (Anton), Spek, A. (Ashley) van der, Baan, C.C. (Carla), Weimar, W. (Willem), Betjes, M.G.H. (Michiel), Meijers, R.W.J. (Ruud), Litjens, N.H.R. (Nicolle), Wit, E.A. (Elly) de, Langerak, A.W. (Anton), Spek, A. (Ashley) van der, Baan, C.C. (Carla), Weimar, W. (Willem), and Betjes, M.G.H. (Michiel)

Abstract

Cytomegalovirus (CMV) infection has been implicated in accelerated T cell ageing. End-stage renal disease (ESRD) patients have a severely immunologically aged T cell compartment but also a high prevalence of CMV infection. We investigated whether CMV infection contributes to T cell ageing in ESRD patients. We determined the thymic output by the T cell receptor excision circle (TREC) content and percentage of CD31+ naïve T cells. The proliferative history of the T cell compartment by determination of the relative telomere length (RTL) and the T cell differentiation status was determined by immunophenotyping. It appeared that CMV infection did not affect thymic output but reduced RTL of CD8+ T cells in ESRD patients. Moreover, increased T cell differentiation was observed with higher percentages of CD57+ and CD28null CD4+ and CD8+ memory T cells. These CD28null T cells had significantly shorter telomeres compared to CD28+ T cells. Therefore we concluded that CMV infection does not affect the decreased thymic output but increases T cell differentiation as observed in ESRD-related premature T cell ageing.

Published
2013
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13. Uremia causes premature ageing of the T cell compartment in end-stage renal disease patients

Author

Meijers, R.W.J. (Ruud), Litjens, N.H.R. (Nicolle), Wit, E.A. (Elly) de, Langerak, A.W. (Anton), Spek, A. (Ashley) van der, Baan, C.C. (Carla), Weimar, W. (Willem), Betjes, M.G.H. (Michiel), Meijers, R.W.J. (Ruud), Litjens, N.H.R. (Nicolle), Wit, E.A. (Elly) de, Langerak, A.W. (Anton), Spek, A. (Ashley) van der, Baan, C.C. (Carla), Weimar, W. (Willem), and Betjes, M.G.H. (Michiel)

Abstract

Background: End-stage renal disease (ESRD) patients treated with renal replacement therapy (RRT) have premature immunologically aged T cells which may underlie uremia-associated immune dysfunction. The aim of this study was to investigate whether uremia was able to induce premature ageing of the T cell compartment. For this purpose, we examined the degree of premature immunological T cell ageing by examining the T cell differentiation status, thymic output via T cell receptor excision circle (TREC) content and proliferative history via relative telomere length in ESRD patients not on RRT.Results: Compared to healthy controls, these patients already had a lower TREC content and an increased T cell differentiation accompanied by shorter telomeres. RRT was able to enhance CD8 + T cell differentiation and to reduce CD8 + T cell telomere length in young dialysis patients. An increased differentiation status of memory CD4 + T cells was also noted in young dialysis patients.Conclusion: Based on these results we can conclude that uremia already causes premature immunological ageing of the T cell system and RRT further increases immunological ageing of the CD8 + T cell compartment in particular in young ESRD patients.

Published
2012
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14. A killer on the road: Circulating CD4 +CD28null T cells as cardiovascular risk factor in ESRD patients

Author

Betjes, M.G.H. (Michiel), Meijers, R.W.J. (Ruud), Wit, L.E.A. (Elly) de, Litjens, N.H.R. (Nicolle), Betjes, M.G.H. (Michiel), Meijers, R.W.J. (Ruud), Wit, L.E.A. (Elly) de, and Litjens, N.H.R. (Nicolle)

Abstract

Chronic kidney disease (CKD) is associated with a sharp increase in the risk for cardiovascular disease, which can only be partially explained by known classical risk factors. However, there is a well-established association with increased systemic inflammation. In the last decade, an unique cytotoxic CD4 + T cell population has been identified, which can be recognized by the loss of the costimulatory cell surface marker CD28, hence their name CD4 +CD28null T cells. These cells are highly proinflammatory, have the functional features of professional killer lymphocytes and can expand from less than 1% to over 50% of the total CD4 + T cell population. In this review, we show that these cells probably play an important role in destabilizing atherosclerotic plaques and could explain, at least in part, the association of cardiovascular disease with an increased inflammatory milieu in CKD patients.

Published
2012
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