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22 results on '"Woestenenk, R.M."'

1. PD-L1 siRNA-mediated silencing in acute myeloid leukemia enhances anti-leukemic T cell reactivity

Author

Ens, D. van, Mousset, C.M., Hutten, T.J.A., Waart, A.B. van der, Campillo-Davo, D., Heijden, S. van der, Vodegel, D., Fredrix, H., Woestenenk, R.M., Parga-Vidal, L., Jansen, J.H., Schaap, N.P.M., Lion, E., Dolstra, H., Hobo, W.A., Ens, D. van, Mousset, C.M., Hutten, T.J.A., Waart, A.B. van der, Campillo-Davo, D., Heijden, S. van der, Vodegel, D., Fredrix, H., Woestenenk, R.M., Parga-Vidal, L., Jansen, J.H., Schaap, N.P.M., Lion, E., Dolstra, H., and Hobo, W.A.

Abstract

Contains fulltext : 229284.pdf (Publisher’s version ) (Closed access), Acute myeloid leukemia (AML) is an immune-susceptible malignancy, as demonstrated by its responsiveness to allogeneic stem cell transplantation (alloSCT). However, by employing inhibitory signaling pathways, including PD-1/PD-L1, leukemia cells suppress T cell-mediated immune attack. Notably, impressive clinical efficacy has been obtained with PD-1/PD-L1 blocking antibodies in cancer patients. Yet, these systemic treatments are often accompanied by severe toxicity, especially after alloSCT. Here, we investigated RNA interference technology as an alternative strategy to locally interfere with PD-1/PD-L1 signaling in AML. We demonstrated efficient siRNA-mediated PD-L1 silencing in HL-60 and patients' AML cells. Importantly, WT1-antigen T cell receptor(+) PD-1(+) 2D3 cells showed increased activation toward PD-L1 silenced WT1(+) AML. Moreover, PD-L1 silenced AML cells significantly enhanced the activation, degranulation, and IFN-γ production of minor histocompatibility antigen-specific CD8(+) T cells. Notably, PD-L1 silencing was equally effective as PD-1 antibody blockade. Together, our study demonstrates that PD-L1 silencing may be an effective strategy to augment AML immune-susceptibility. This provides rationale for further development of targeted approaches to locally interfere with immune escape mechanisms in AML, thereby minimizing severe toxicity. In combination with alloSCT and/or adoptive T cell transfer, this strategy could be very appealing to boost graft-versus-leukemia immunity and improve outcome in AML patients.

Published
2020

2. TIGIT blockade enhances functionality of peritoneal NK cells with altered expression of DNAM-1/TIGIT/CD96 checkpoint molecules in ovarian cancer

Author

Maas, R.J.A., Hoogstad-van Evert, J.S. van, Meer, J.M.R. van der, Mekers, V.E., Rezaeifard, S., Korman, Alan J., Jonge, P.K. de, Woestenenk, R.M., Schaap, N.P.M., Massuger, L.F.A.G., Jansen, J.H., Hobo, W.A., Dolstra, H., Maas, R.J.A., Hoogstad-van Evert, J.S. van, Meer, J.M.R. van der, Mekers, V.E., Rezaeifard, S., Korman, Alan J., Jonge, P.K. de, Woestenenk, R.M., Schaap, N.P.M., Massuger, L.F.A.G., Jansen, J.H., Hobo, W.A., and Dolstra, H.

Abstract

Item does not contain fulltext

Published
2020

3. Single-cell analysis reveals that stochasticity and paracrine signaling control interferon-alpha production by plasmacytoid dendritic cells

Author

Wimmers, F., Subedi, Nikita, Buuringen, Nicole van, Heister, Daan, Vivie, Judith, Reinieren-Beeren, I.M.J., Woestenenk, R.M., Dolstra, H., Piruska, A., Jacobs, J.F.M., Figdor, C.G., Vries, I.J.M. de, Huck, W.T.S., Tel, J., Wimmers, F., Subedi, Nikita, Buuringen, Nicole van, Heister, Daan, Vivie, Judith, Reinieren-Beeren, I.M.J., Woestenenk, R.M., Dolstra, H., Piruska, A., Jacobs, J.F.M., Figdor, C.G., Vries, I.J.M. de, Huck, W.T.S., and Tel, J.

Abstract

Contains fulltext : 194897.pdf (publisher's version ) (Open Access)

Published
2018

4. Increased Coexpression of PD-1, TIGIT, and KLRG-1 on Tumor-Reactive CD8(+) T Cells During Relapse after Allogeneic Stem Cell Transplantation

Author

Hutten, T.J.A., Norde, W.J., Woestenenk, R.M., Wang, Ruo Chen, Maas, F.M., Kester, Michel, Jansen, J.H., Schaap, N.P., Dolstra, H., Hobo, W.A., Hutten, T.J.A., Norde, W.J., Woestenenk, R.M., Wang, Ruo Chen, Maas, F.M., Kester, Michel, Jansen, J.H., Schaap, N.P., Dolstra, H., and Hobo, W.A.

Abstract

Contains fulltext : 191170.pdf (publisher's version ) (Closed access)

Published
2018

5. A Human Renal Proximal Tubule Cell Line with Stable Organic Anion Transporter 1 and 3 Expression Predictive for Antiviral-Induced Toxicity

Author

Nieskens, T.T., Peters, J.G.P., Schreurs, M.J., Smits, N., Woestenenk, R.M., Jansen, K., Made, T.K. van der, Röring, M., Hilgendorf, C., Wilmer, M.J., Masereeuw, R., Nieskens, T.T., Peters, J.G.P., Schreurs, M.J., Smits, N., Woestenenk, R.M., Jansen, K., Made, T.K. van der, Röring, M., Hilgendorf, C., Wilmer, M.J., and Masereeuw, R.

Abstract

Contains fulltext : 167165.pdf (publisher's version ) (Open Access)

Published
2016

6. CLEC12A-Mediated Antigen Uptake and Cross-Presentation by Human Dendritic Cell Subsets Efficiently Boost Tumor-Reactive T Cell Responses

Author

Hutten, T.J., Thordardottir, S., Fredrix, H., Janssen, L.D., Woestenenk, R.M., Tel, J., Joosten, B.H., Cambi, A., Heemskerk, M.H., Franssen, G.M., Boerman, O.C., Bakker, L.B., Jansen, J.H., Schaap, N.P., Dolstra, H., Hobo, W.A., Hutten, T.J., Thordardottir, S., Fredrix, H., Janssen, L.D., Woestenenk, R.M., Tel, J., Joosten, B.H., Cambi, A., Heemskerk, M.H., Franssen, G.M., Boerman, O.C., Bakker, L.B., Jansen, J.H., Schaap, N.P., Dolstra, H., and Hobo, W.A.

Abstract

Contains fulltext : 172057.pdf (publisher's version ) (Closed access), Potent immunotherapies are urgently needed to boost antitumor immunity and control disease in cancer patients. As dendritic cells (DCs) are the most powerful APCs, they are an attractive means to reinvigorate T cell responses. An appealing strategy to use the effective Ag processing and presentation machinery, T cell stimulation and cross-talk capacity of natural DC subsets is in vivo tumor Ag delivery. In this context, endocytic C-type lectin receptors are attractive targeting molecules. In this study, we investigated whether CLEC12A efficiently delivers tumor Ags into human DC subsets, facilitating effective induction of CD4(+) and CD8(+) T cell responses. We confirmed that CLEC12A is selectively expressed by myeloid cells, including the myeloid DC subset (mDCs) and the plasmacytoid DC subset (pDCs). Moreover, we demonstrated that these DC subsets efficiently internalize CLEC12A, whereupon it quickly translocates to the early endosomes and subsequently routes to the lysosomes. Notably, CLEC12A Ab targeting did not negatively affect DC maturation or function. Furthermore, CLEC12A-mediated delivery of keyhole limpet hemocyanin resulted in enhanced proliferation and cytokine secretion by keyhole limpet hemocyanin-experienced CD4(+) T cells. Most importantly, CLEC12A-targeted delivery of HA-1 long peptide resulted in efficient Ag cross-presentation by mDCs and pDCs, leading to strong ex vivo activation of HA-1-specific CD8(+) T cells of patients after allogeneic stem cell transplantation. Collectively, these data indicate that CLEC12A is an effective new candidate with great potential for in vivo Ag delivery into mDCs and pDCs, thereby using the specialized functions and cross-talk capacity of these DC subsets to boost tumor-reactive T cell immunity in cancer patients.

Published
2016

7. Apoptosis-Related Gene Expression Profiling in Hematopoietic Cell Fractions of MDS Patients

Author

Langemeijer, S.M.C., Mariani, N., Knops, R., Gilissen, C.F., Woestenenk, R.M., Witte, T.J. de, Huls, G.A., Reijden, B.A. van der, Jansen, J.H., Langemeijer, S.M.C., Mariani, N., Knops, R., Gilissen, C.F., Woestenenk, R.M., Witte, T.J. de, Huls, G.A., Reijden, B.A. van der, and Jansen, J.H.

Abstract

Contains fulltext : 168172.pdf (publisher's version ) (Open Access), Although the vast majority of patients with a myelodysplastic syndrome (MDS) suffer from cytopenias, the bone marrow is usually normocellular or hypercellular. Apoptosis of hematopoietic cells in the bone marrow has been implicated in this phenomenon. However, in MDS it remains only partially elucidated which genes are involved in this process and which hematopoietic cells are mainly affected. We employed sensitive real-time PCR technology to study 93 apoptosis-related genes and gene families in sorted immature CD34+ and the differentiating erythroid (CD71+) and monomyeloid (CD13/33+) bone marrow cells. Unsupervised cluster analysis of the expression signature readily distinguished the different cellular bone marrow fractions (CD34+, CD71+ and CD13/33+) from each other, but did not discriminate patients from healthy controls. When individual genes were regarded, several were found to be differentially expressed between patients and controls. Particularly, strong over-expression of BIK (BCL2-interacting killer) was observed in erythroid progenitor cells of low- and high-risk MDS patients (both p = 0.001) and TNFRSF4 (tumor necrosis factor receptor superfamily 4) was down-regulated in immature hematopoietic cells (p = 0.0023) of low-risk MDS patients compared to healthy bone marrow.

Published
2016

8. Chromosomal abnormalities in hepatic cysts point to novel polycystic liver disease genes

Author

Wills, E.S., Cnossen, W.R., Veltman, J.A., Woestenenk, R.M., Steehouwer, M., Salomon, J., Morsche, R.H.M. te, Huch, M., Hehir-Kwa, J.Y., Banning, M.J., Pfundt, R.P., Roepman, R., Hoischen, A., Drenth, J.P.H., Wills, E.S., Cnossen, W.R., Veltman, J.A., Woestenenk, R.M., Steehouwer, M., Salomon, J., Morsche, R.H.M. te, Huch, M., Hehir-Kwa, J.Y., Banning, M.J., Pfundt, R.P., Roepman, R., Hoischen, A., and Drenth, J.P.H.

Abstract

Contains fulltext : 167652.pdf (publisher's version ) (Closed access), Autosomal dominant polycystic liver disease (ADPLD) is caused by variants in PRKCSH, SEC63, and LRP5, whereas autosomal dominant polycystic kidney disease is caused by variants in PKD1 and PKD2. Liver cyst development in these disorders is explained by somatic loss-of-heterozygosity (LOH) of the wild-type allele in the developing cyst. We hypothesize that we can use this mechanism to identify novel disease genes that reside in LOH regions. In this study, we aim to map abnormal genomic regions using high-density SNP microarrays to find novel PLD genes. We collected 46 cysts from 23 patients with polycystic or sporadic hepatic cysts, and analyzed DNA from those cysts using high-resolution microarray (n=24) or Sanger sequencing (n=22). We here focused on regions of homozygosity on the autosomes (>3.0 Mb) and large CNVs (>1.0 Mb). We found frequent LOH in PRKCSH (22/29) and PKD1/PKD2 (2/3) cysts of patients with known heterozygous germline variants in the respective genes. In the total cohort, 12/23 patients harbored abnormalities outside of familiar areas. In individual ADPLD cases, we identified germline events: a 2q13 complex rearrangement resulting in BUB1 haploinsufficiency, a 47XXX karyotype, chromosome 9q copy-number loss, and LOH on chromosome 3p. The latter region was overlapping with an LOH region identified in two other cysts. Unique germline and somatic abnormalities occur frequently in and outside of known genes underlying cysts. Each liver cyst has a unique genetic makeup. LOH driver gene BUB1 may imply germline causes of genetic instability in PLD.

Published
2016

9. Addition of 10-Day Decitabine to Fludarabine/Total Body Irradiation Conditioning is Feasible and Induces Tumor-Associated Antigen-Specific T Cell Responses

Author

Cruijsen, M.J., Hobo, W.A., Velden, W.J.F.M. van der, Bremmers, M.E.J., Woestenenk, R.M., Bar, B.M., Falkenburg, J.H.F., Kester, M., Schaap, N.P., Jansen, J.H., Blijlevens, N.M., Dolstra, H., Huls, G.A., Cruijsen, M.J., Hobo, W.A., Velden, W.J.F.M. van der, Bremmers, M.E.J., Woestenenk, R.M., Bar, B.M., Falkenburg, J.H.F., Kester, M., Schaap, N.P., Jansen, J.H., Blijlevens, N.M., Dolstra, H., and Huls, G.A.

Abstract

Contains fulltext : 172843.pdf (publisher's version ) (Closed access)

Published
2016

10. Longevity and composition of cellular immune responses following experimental Plasmodium falciparum malaria infection in humans

Author

Teirlinck, A.C., McCall, M.B.B., Roestenberg, M., Scholzen, A., Woestenenk, R.M., Mast, Q. de, Ven, A.J.A.M. van der, Hermsen, C.C., Luty, A.J.F., and Sauerwein, R.W.

Subjects
Immune Regulation [NCMLS 2], Pathogenesis and modulation of inflammation Infection and autoimmunity [N4i 1], Poverty-related infectious diseases Infectious diseases and international health [N4i 3], Auto-immunity, transplantation and immunotherapy [N4i 4]
Abstract

Contains fulltext : 98063.pdf (Publisher’s version ) (Open Access) Cellular responses to Plasmodium falciparum parasites, in particular interferon-gamma (IFNgamma) production, play an important role in anti-malarial immunity. However, clinical immunity to malaria develops slowly amongst naturally exposed populations, the dynamics of cellular responses in relation to exposure are difficult to study and data about the persistence of such responses are controversial. Here we assess the longevity and composition of cellular immune responses following experimental malaria infection in human volunteers. We conducted a longitudinal study of cellular immunological responses to sporozoites (PfSpz) and asexual blood-stage (PfRBC) malaria parasites in naive human volunteers undergoing single (n = 5) or multiple (n = 10) experimental P. falciparum infections under highly controlled conditions. IFNgamma and interleukin-2 (IL-2) responses following in vitro re-stimulation were measured by flow-cytometry prior to, during and more than one year post infection. We show that cellular responses to both PfSpz and PfRBC are induced and remain almost undiminished up to 14 months after even a single malaria episode. Remarkably, not only 'adaptive' but also 'innate' lymphocyte subsets contribute to the increased IFNgamma response, including alphabetaT cells, gammadeltaT cells and NK cells. Furthermore, results from depletion and autologous recombination experiments of lymphocyte subsets suggest that immunological memory for PfRBC is carried within both the alphabetaT cells and gammadeltaT compartments. Indeed, the majority of cytokine producing T lymphocytes express an CD45RO(+) CD62L(-) effector memory (EM) phenotype both early and late post infection. Finally, we demonstrate that malaria infection induces and maintains polyfunctional (IFNgamma(+)IL-2(+)) EM responses against both PfRBC and PfSpz, previously found to be associated with protection. These data demonstrate that cellular responses can be readily induced and are long-lived following infection with P. falciparum, with a persisting contribution by not only adaptive but also (semi-)innate lymphocyte subsets. The implications hereof are positive for malaria vaccine development, but focus attention on those factors potentially inhibiting such responses in the field. 01 december 2011

Published
2011

11. 1,25-Dihydroxyvitamin D3 inhibits proliferation but not the suppressive function of regulatory T cells in the absence of antigen-presenting cells

Author

Khoo, A.L., Joosten, I., Michels, M., Woestenenk, R.M., Preijers, F.W.M.B., He, X., Netea, M.G., Ven, A.J.A.M. van der, and Koenen, H.J.P.M.

Subjects
Pathogenesis and modulation of inflammation [N4i 1], Auto-immunity, transplantation and immunotherapy Immune Regulation [N4i 4], Immune Regulation [NCMLS 2], Poverty-related infectious diseases [N4i 3], hemic and immune systems, chemical and pharmacologic phenomena, Auto-immunity, transplantation and immunotherapy [N4i 4]
Abstract

Contains fulltext : 96559.pdf (Publisher’s version ) (Closed access) Vitamin D3 is known to induce regulatory T (Treg) cells by rendering antigen-presenting cells tolerogenic, its direct effect on human naturally occurring Treg cells is unclear. Here, we investigated if and how 1,25-dihydroxyvitamin D(3) [1,25(OH)2D3] can directly affect the proliferation and function of human naturally occurring Treg cells in vitro. First, we demonstrated that these Treg cells express vitamin D receptors that were up-regulated following anti-CD3/CD28-bead stimulation. 1,25(OH)2D3 inhibited proliferation of Treg cells even when exogenous interleukin-2 was provided. Treg cells were more susceptible to the inhibitory effect of 1,25(OH)2D3 than conventional T cells(.) 1,25(OH)2D3 neither affected the anergic state nor the suppressive function of Treg cells but induced a subtle increase in interleukin-10-secreting cells. The cell-division-inhibiting effect of 1,25(OH)2D3 on Treg cells was also demonstrated in vivo by supplementing vitamin D-deficient HIV-1-infected patients with 2000 IU cholecalciferol (vitamin D3). Increased serum 1,25(OH)2D3 levels were associated with a drop in the number and percentage of Treg cells, which may be attributed to a decrease in the proliferating Foxp3+ Treg cell population. In conclusion, 1,25(OH)2D3 directly affects Treg cell growth and promotes interleukin-10 production without apparent effects on activation status and suppressive phenotype whereas in vivo, high serum 1,25(OH)2D3 levels are associated with reduced Treg cell proliferation and a reduced number of Treg cells. 01 december 2011

Published
2011

12. Enhanced cellular uptake of albumin-based lyophilisomes when functionalized with cell-penetrating peptide TAT in HeLa cells

Author

Bracht, E. van, Versteegden, L.R.M., Stolle, S., Verdurmen, W.P.R., Woestenenk, R.M., Raave, R., Hafmans, T., Oosterwijk, E., Brock, R.E., Kuppevelt, T.H. van, Daamen, W.F., Bracht, E. van, Versteegden, L.R.M., Stolle, S., Verdurmen, W.P.R., Woestenenk, R.M., Raave, R., Hafmans, T., Oosterwijk, E., Brock, R.E., Kuppevelt, T.H. van, and Daamen, W.F.

Abstract

Contains fulltext : 135873.pdf (publisher's version ) (Open Access), Lyophilisomes are a novel class of biodegradable proteinaceous nano/micrometer capsules with potential use as drug delivery carrier. Cell-penetrating peptides (CPPs) including the TAT peptide have been successfully implemented for intracellular delivery of a broad variety of cargos including various nanoparticulate pharmaceutical carriers. In the present study, lyophilisomes were modified using CPPs in order to achieve enhanced cellular uptake. Lyophilisomes were prepared by a freezing, annealing, and lyophilization method and a cystein-elongated TAT peptide was conjugated to the lyophilisomes using a heterobifunctional linker. Fluorescent-activated cell sorting (FACS) was utilized to acquire a lyophilisome population with a particle diameter smaller than 1000 nm. Cultured HeLa, OVCAR-3, Caco-2 and SKOV-3 cells were exposed to unmodified lyophilisomes and TAT-conjugated lyophilisomes and examined with FACS. HeLa cells were investigated in more detail using a trypan blue quenching assay, confocal microscopy, and transmission electron microscopy. TAT-conjugation strongly increased binding and cellular uptake of lyophilisomes in a time-dependent manner in vitro, as assessed by FACS. These results were confirmed by confocal microscopy. Transmission electron microscopy indicated rapid cellular uptake of TAT-conjugated lyophilisomes via phagocytosis and/or macropinocytosis. In conclusion, TAT-peptides conjugated to albumin-based lyophilisomes are able to enhance cellular uptake of lyophilisomes in HeLa cells.

Published
2014

13. Foxp3+ regulatory T cells of psoriasis patients easily differentiate into IL-17A-producing cells and are found in lesional skin

Author

Bovenschen, H.J., Kerkhof, P.C. van de, Erp, P.E. van, Woestenenk, R.M., Joosten, I., Koenen, H.J.P.M., Bovenschen, H.J., Kerkhof, P.C. van de, Erp, P.E. van, Woestenenk, R.M., Joosten, I., and Koenen, H.J.P.M.

Abstract

Contains fulltext : 96935.pdf (publisher's version ) (Closed access), Psoriasis is an autoimmune-related chronic inflammatory skin disease that is strongly associated with IL-23 and T helper-17 (Th17) effector cytokines. In addition, CD4+CD25(high) regulatory T-cell (Treg) function appeared to be impaired in psoriasis. CD4+CD25(high)Foxp3+ Tregs are typically considered inhibitors of autoimmune responses. However, under proinflammatory conditions, Tregs can differentiate into inflammation-associated Th17 cells--a paradigm shift, with as yet largely unknown consequences for human disease initiation or progression. Th17 cells are highly proinflammatory T cells that are characterized by IL-17A and IL-22 production and expression of the transcription factor retinoic acid-related orphan receptor gammat (RORgammat). We here show that Tregs of patients with severe psoriasis, as compared with those of healthy controls, have an enhanced propensity to differentiate into IL-17A-producing cells on ex vivo stimulation. This enhanced Treg differentiation was linked to unexpectedly high RORgammat levels and enhanced loss of Foxp3. Notably, IL-23 boosted this Treg differentiation process particularly in patients with psoriasis but less so in controls. IL-23 further reduced Foxp3 expression while leaving the high RORgammat levels unaffected. The histone/protein deacetylase inhibitor, Trichostatin-A, prevented Th17 differentiation of Tregs in psoriasis patients. Importantly, IL-17A+/Foxp3+/CD4+ triple-positive cells were present in skin lesions of patients with severe psoriasis. These data stress the clinical relevance of Treg differentiation for the perpetuation of chronic inflammatory disease and may pave novel ways for immunotherapy.

Published
2011

14. Morphology of partial globozoospermia

Author

Dam, A.H.D.M., Ramos, L., Dijkman, H.B., Woestenenk, R.M., Robben, H., Hoven, L. van den, Kremer, J.A.M., Dam, A.H.D.M., Ramos, L., Dijkman, H.B., Woestenenk, R.M., Robben, H., Hoven, L. van den, and Kremer, J.A.M.

Abstract

Contains fulltext : 97124.pdf (publisher's version ) (Closed access), Total globozoospermia is a rare sperm morphology disorder that consists of 100% round-headed, acrosomeless spermatozoa. There is also a larger group of patients whose sperm cells are partially acrosomeless. The aim of this investigation was to describe partial globozoospermia compared to total globozoospermia and normozoospermia. Ejaculates from 10 patients with more than 50% acrosomeless spermatozoa (partial globozoospermia), 3 patients with total globozoospermia, and 9 normozoospermic controls were analyzed with light microscopy, transmission electron microscopy, and flow cytometry. Qualitative and quantitative examination of spermatozoa from the 3 groups shows differences in the percentage of round-headed sperm cells and acrosome malformation. Total globozoospermia presents as a homogenous kind of teratozoospermia. Partial globozoospermia is a distinctive sperm malformation with an increased proportion of round-headed sperm cells and acrosome malformations compared to normozoospermia, which exists separately from total globozoospermia. It thereby contains oval sperm cells that may have distinctive malformations of the sperm head matrix, but also morphologically normal sperm cells that may be used in a clinical setting.

Published
2011

15. Concurrent detection of circulating minor histocompatibility antigen-specific CD8+ T cells in SCT recipients by combinatorial encoding MHC multimers

Author

Broen, K.C.J., Greupink-Draaisma, A.L., Woestenenk, R.M., Schaap, N.P.M., Brickner, A.G., Dolstra, H., Broen, K.C.J., Greupink-Draaisma, A.L., Woestenenk, R.M., Schaap, N.P.M., Brickner, A.G., and Dolstra, H.

Abstract

Contains fulltext : 95751.pdf (publisher's version ) (Open Access), Allogeneic stem cell transplantation (SCT) is a potentially curative treatment for patients with hematologic malignancies. Its therapeutic effect is largely dependent on recognition of minor histocompatibility antigens (MiHA) by donor-derived CD8 T cells. Therefore, monitoring of multiple MiHA-specific CD8 T cell responses may prove to be valuable for evaluating the efficacy of allogeneic SCT. In this study, we investigated the use of the combinatorial encoding MHC multimer technique to simultaneously detect MiHA-specific CD8 T cells in peripheral blood of SCT recipients. Feasibility of this approach was demonstrated by applying dual-color encoding MHC multimers for a set of 10 known MiHA. Interestingly, single staining using a fluorochrome- and Qdot-based five-color combination showed comparable results to dual-color staining for most MiHA-specific CD8 T cell responses. In addition, we determined the potential value of combinatorial encoding MHC multimers in MiHA identification. Therefore, a set of 75 candidate MiHA peptides was predicted from polymorphic genes with a hematopoietic expression profile and further selected for high and intermediate binding affinity for HLA-A2. Screening of a large cohort of SCT recipients resulted in the detection of dual-color encoded CD8 T cells following MHC multimer-based T cell enrichment and short ex vivo expansion. Interestingly, candidate MiHA-specific CD8 T cell responses for LAG3 and TLR10 derived polymorphic peptides could be confirmed by genotyping of the respective SNPs. These findings demonstrate the potency of the combinatorial MHC multimer approach in the monitoring of CD8 T cell responses to known and potential MiHA in limited amounts of peripheral blood from allogeneic SCT recipients.

Published
2011

16. Deficiency of either P-glycoprotein or breast cancer resistance protein protect against acute kidney injury.

Author

Huls, M., Schoeber, J.P.H., Verfaillie, C.M., Luttun, A., Ulloa-Montoya, F., Menke, A.L., Bolderen, L.R. van, Woestenenk, R.M., Merkx, G.F.M., Wetzels, J.F.M., Russel, F.G.M., Masereeuw, R., Huls, M., Schoeber, J.P.H., Verfaillie, C.M., Luttun, A., Ulloa-Montoya, F., Menke, A.L., Bolderen, L.R. van, Woestenenk, R.M., Merkx, G.F.M., Wetzels, J.F.M., Russel, F.G.M., and Masereeuw, R.

Abstract

Contains fulltext : 88153.pdf (publisher's version ) (Open Access), The kidney has a high capacity to regenerate after ischemic injury via several mechanisms, one of which involves bone marrow-derived (stem) cells. The ATP binding cassette transporters, P-glycoprotein and breast cancer resistance protein, are determinants for the enriched stem and progenitor cell fraction in bone marrow. Because they are upregulated after acute kidney injury, we hypothesized that both efflux pumps may play a role in protecting against renal injury. Surprisingly, transporter-deficient mice were protected against ischemia-induced renal injury. To further study this, bone marrow from irradiated wild-type mice was reconstituted by bone marrow from wild-type, P-glycoprotein- or breast cancer resistance protein-deficient mice. Four weeks later, kidney injury was induced and its function evaluated. Significantly more bone marrow-derived cells were detected in kidneys grafted with transporter-deficient bone marrow. A gender mismatch study suggested that cell fusion of resident tubular cells with bone marrow cells was unlikely. Renal function analyses indicated an absence of renal damage following ischemia-reperfusion in animals transplanted with transporter-deficient bone marrow. When wild-type bone marrow was transplanted in breast cancer resistance protein-deficient mice this protection is lost. Furthermore, we demonstrate that transporter-deficient bone marrow contained significantly more monocytes, granulocytes, and early outgrowth endothelial progenitor cells.

Published
2010

17. Lyophilisomes: Potential carriers for tumor targeting.

Author

Bracht, E. van, Geutjes, P.J., Woestenenk, R.M., Wismans, P.G.P., Oosterwijk, E., Kuppevelt, T. van, Daamen, W.F., Bracht, E. van, Geutjes, P.J., Woestenenk, R.M., Wismans, P.G.P., Oosterwijk, E., Kuppevelt, T. van, and Daamen, W.F.

Abstract

Item does not contain fulltext

Published
2010

18. Sorting Catalytically Active Polymersome Nanoreactors by Flow Cytometry

Author

Nallani, M., Woestenenk, R.M., Hoog, H.P.M. de, Dongen, S.F.M. van, Boezeman, J.B.M., Cornelissen, J.J.L.M., Nolte, R.J.M., Hest, J.C.M. van, Nallani, M., Woestenenk, R.M., Hoog, H.P.M. de, Dongen, S.F.M. van, Boezeman, J.B.M., Cornelissen, J.J.L.M., Nolte, R.J.M., and Hest, J.C.M. van

Abstract

Contains fulltext : 75851.pdf (publisher's version ) (Closed access)

Published
2009

19. Clinical grade Treg: GMP isolation, improvement of purity by CD127 Depletion, Treg expansion, and Treg cryopreservation

Author

Peters, J.H., Preijers, F.W.M.B., Woestenenk, R.M., Hilbrands, L.B., Koenen, H.J.P.M., Joosten, I., Peters, J.H., Preijers, F.W.M.B., Woestenenk, R.M., Hilbrands, L.B., Koenen, H.J.P.M., and Joosten, I.

Abstract

Contains fulltext : 69507.pdf ( ) (Open Access), BACKGROUND: Treg based immunotherapy is of great interest to facilitate tolerance in autoimmunity and transplantation. For clinical trials, it is essential to have a clinical grade Treg isolation protocol in accordance with Good Manufacturing Practice (GMP) guidelines. To obtain sufficient Treg for immunotherapy, subsequent ex vivo expansion might be needed. METHODOLOGY/PRINCIPAL FINDINGS: Treg were isolated from leukapheresis products by CliniMACS based GMP isolation strategies, using anti-CD25, anti-CD8 and anti-CD19 coated microbeads. CliniMACS isolation procedures led to 40-60% pure CD4(pos)CD25(high)FoxP3(pos) Treg populations that were anergic and had moderate suppressive activity. Such CliniMACS isolated Treg populations could be expanded with maintenance of suppressive function. Alloantigen stimulated expansion caused an enrichment of alloantigen-specific Treg. Depletion of unwanted CD19(pos) cells during CliniMACS Treg isolation proved necessary to prevent B-cell outgrowth during expansion. CD4(pos)CD127(pos) conventional T cells were the major contaminating cell type in CliniMACS isolated Treg populations. Depletion of CD127(pos) cells improved the purity of CD4(pos)CD25(high)FoxP3(pos) Treg in CliniMACS isolated cell populations to approximately 90%. Expanded CD127(neg) CliniMACS isolated Treg populations showed very potent suppressive capacity and high FoxP3 expression. Furthermore, our data show that cryopreservation of CliniMACS isolated Treg is feasible, but that activation after thawing is necessary to restore suppressive potential. CONCLUSIONS/SIGNIFICANCE: The feasibility of Treg based therapy is widely accepted, provided that tailor-made clinical grade procedures for isolation and ex vivo cell handling are available. We here provide further support for this approach by showing that a high Treg purity can be reached, and that isolated cells can be cryopreserved and expanded successfully.

Published
2008

20. Dynamics in chimerism of T cells and dendritic cells in relapsed CML patients and the influence on the induction of alloreactivity following donor lymphocyte infusion.

Author

Levenga, H., Woestenenk, R.M., Schattenberg, A.V.M.B., Maas, F.M.H.M., Jansen, J.H., Raymakers, R.A.P., Mulder, P.H.M. de, Wiel-van Kemenade, E. van de, Schaap, N.P.M., Witte, T.J.M. de, Dolstra, H., Levenga, H., Woestenenk, R.M., Schattenberg, A.V.M.B., Maas, F.M.H.M., Jansen, J.H., Raymakers, R.A.P., Mulder, P.H.M. de, Wiel-van Kemenade, E. van de, Schaap, N.P.M., Witte, T.J.M. de, and Dolstra, H.

Abstract

Contains fulltext : 52204.pdf (publisher's version ) (Closed access), Donor lymphocyte infusion (DLI) after allogeneic SCT induces complete remissions in approximately 80% of patients with relapsed CML in chronic phase, but some patients do not respond to DLI. We studied absolute numbers of dendritic cell (DC) subsets and chimerism in T cells and two subsets of blood DCs (myeloid DCs (MDCs) and plasmacytoid DCs (PDCs)) in relation to DLI-induced alloreactivity. Based on T cell and DC chimerism, we identified three groups. Four patients were completely donor chimeric in T cells and DC subsets. These patients had an early stage of relapse, and three of the four patients attained complete molecular remission (CMolR) without significant GVHD. Six patients were completely donor in T cells and mixed chimeric in DC subsets. All patients entered CMolR, but this was associated with GVHD in four and cytopenia in three patients. Five patients had mixed chimerism in T cells and complete recipient chimerism in MDC; only two patients entered CMolR. Our data suggest that the combination of donor T cells and mixed chimerism in DC subsets induces a potent graft-versus-leukemia (GVL) effect in association with GVHD. DLI in patients with an early relapse and donor chimerism in both T cells and DC subsets results in GVL reactivity without GVHD.

Published
2007

21. A frameshift polymorphism in P2X5 elicits an allogeneic cytotoxic T lymphocyte response associated with remission of chronic myeloid leukemia.

Author

Rijke, B. de, Zoetbrood, A., Beekman, J.M., Otterud, B.E., Maas, F.M.H.M., Woestenenk, R.M., Kester, M., Leppert, M., Schattenberg, A.V.M.B., Witte, T.J.M. de, Wiel-van Kemenade, E. van de, Dolstra, H., Rijke, B. de, Zoetbrood, A., Beekman, J.M., Otterud, B.E., Maas, F.M.H.M., Woestenenk, R.M., Kester, M., Leppert, M., Schattenberg, A.V.M.B., Witte, T.J.M. de, Wiel-van Kemenade, E. van de, and Dolstra, H.

Abstract

Contains fulltext : 48913.pdf (publisher's version ) (Open Access), Minor histocompatibility antigens (mHAgs) constitute the targets of the graft-versus-leukemia response after HLA-identical allogeneic stem cell transplantation. Here, we have used genetic linkage analysis to identify a novel mHAg, designated lymphoid-restricted histocompatibility antigen-1 (LRH-1), which is encoded by the P2X5 gene and elicited an allogeneic CTL response in a patient with chronic myeloid leukemia after donor lymphocyte infusion. We demonstrate that immunogenicity for LRH-1 is due to differential protein expression in recipient and donor cells as a consequence of a homozygous frameshift polymorphism in the donor. Tetramer analysis showed that emergence of LRH-1-specific CD8+ cytotoxic T cells in peripheral blood and bone marrow correlated with complete remission of chronic myeloid leukemia. Furthermore, the restricted expression of LRH-1 in hematopoietic cells including leukemic CD34+ progenitor cells provides evidence of a role for LRH-1-specific CD8+ cytotoxic T cells in selective graft-versus-leukemia reactivity in the absence of severe graft-versus-host disease. These findings illustrate that the P2X5-encoded mHAg LRH-1 could be an attractive target for specific immunotherapy to treat hematological malignancies recurring after allogeneic stem cell transplantation.

Published
2005

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