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3. No non-sentinel node involvement in melanoma patients with limited Breslow thickness and low sentinel node tumour load

Author

Bogenrieder, T., Dijk, M.R. van, Blokx, W.A.M., Ramrath, K., Seldenrijk, K., Stolz, W., and Diest, P.J. van

Subjects
Translational research [ONCOL 3]
Abstract

Item does not contain fulltext AIMS: Most melanoma patients with a positive sentinel node (SN) undergo completion lymph node dissection and frequently experience associated morbidity. However, only 10-30% of SN-positive patients have further lymph node metastases. The aim of the present study was to predict the absence of non-SN metastases in a multicentre study of patients with a positive SN based on primary melanoma features and SN tumour load. METHODS AND RESULTS: Of 70 SN positive patients, 18 had non-SN metastases. Penetrative depth of metastatic cells into the SN and SN tumour load was assessed by morphometry. None of the 14 patients (20%) with a Breslow thickness

Published
2011
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5. Three members of the 6-cys protein family of plasmodium play a role in gamete fertility

Author

Dijk, M.R. van, Schaijk, B.C.L. van, Khan, S.M., Dooren, M.W. van, Ramesar, J., Kaczanowski, S., Gemert, G.J.A. van, Kroeze, H., Stunnenberg, H.G., Eling, W.M., Sauerwein, R.W., Waters, A.P., Janse, C.J., Dijk, M.R. van, Schaijk, B.C.L. van, Khan, S.M., Dooren, M.W. van, Ramesar, J., Kaczanowski, S., Gemert, G.J.A. van, Kroeze, H., Stunnenberg, H.G., Eling, W.M., Sauerwein, R.W., Waters, A.P., and Janse, C.J.

Abstract

Contains fulltext : 83802schaijk.pdf (publisher's version ) (Closed access)

Published
2010

6. Improved discrimination of melanotic schwannoma from melanocytic lesions by combined morphological and GNAQ mutational analysis.

Author

Kusters-vandevelde, H.V., Grunsven, I. van, Kusters, B., Dijk, M.R. van, Groenen, P.J.T.A., Wesseling, P., Blokx, W.A.M., Kusters-vandevelde, H.V., Grunsven, I. van, Kusters, B., Dijk, M.R. van, Groenen, P.J.T.A., Wesseling, P., and Blokx, W.A.M.

Abstract

1 december 2010, Contains fulltext : 88122.pdf (publisher's version ) (Closed access), The histological differential diagnosis between melanotic schwannoma, primary leptomeningeal melanocytic lesions and cellular blue nevus can be challenging. Correct diagnosis of melanotic schwannoma is important to select patients who need clinical evaluation for possible association with Carney complex. Recently, we described the presence of activating codon 209 mutations in the GNAQ gene in primary leptomeningeal melanocytic lesions. Identical codon 209 mutations have been described in blue nevi. The aims of the present study were to (1) perform a histological review of a series of lesions (initially) diagnosed as melanotic schwannoma and analyze them for GNAQ mutations, and (2) test the diagnostic value of GNAQ mutational analysis in the differential diagnosis with leptomeningeal melanocytic lesions. We retrieved 25 cases that were initially diagnosed as melanotic schwannoma. All cases were reviewed using established criteria and analyzed for GNAQ codon 209 mutations. After review, nine cases were classified as melanotic schwannoma. GNAQ mutations were absent in these nine cases. The remaining cases were reclassified as conventional schwannoma (n = 9), melanocytoma (n = 4), blue nevus (n = 1) and lesions that could not be classified with certainty as melanotic schwannoma or melanocytoma (n = 2). GNAQ codon 209 mutations were present in 3/4 melanocytomas and the blue nevus. Including results from our previous study in leptomeningeal melanocytic lesions, GNAQ mutations were highly specific (100%) for leptomeningeal melanocytic lesions compared to melanotic schwannoma (sensitivity 43%). We conclude that a detailed analysis of morphology combined with GNAQ mutational analysis can aid in the differential diagnosis of melanotic schwannoma with leptomeningeal melanocytic lesions.

Published
2010

7. Gene disruption of Plasmodium falciparum p52 results in attenuation of malaria liver stage development in cultured primary human hepatocytes

Author

Schaijk, B.C.L. van, Janse, C.J., Gemert, G.J.A. van, Dijk, M.R. van, Gego, A., Franetich, J.F., Vegte-Bolmer, M.G. van de, Yalaoui, S., Silvie, O., Hoffman, S.L., Waters, A.P., Mazier, D., Sauerwein, R.W., Khan, S.M., Schaijk, B.C.L. van, Janse, C.J., Gemert, G.J.A. van, Dijk, M.R. van, Gego, A., Franetich, J.F., Vegte-Bolmer, M.G. van de, Yalaoui, S., Silvie, O., Hoffman, S.L., Waters, A.P., Mazier, D., Sauerwein, R.W., and Khan, S.M.

Abstract

Contains fulltext : 70169.pdf (publisher's version ) (Open Access), Difficulties with inducing sterile and long lasting protective immunity against malaria with subunit vaccines has renewed interest in vaccinations with attenuated Plasmodium parasites. Immunizations with sporozoites that are attenuated by radiation (RAS) can induce strong protective immunity both in humans and rodent models of malaria. Recently, in rodent parasites it has been shown that through the deletion of a single gene, sporozoites can also become attenuated in liver stage development and, importantly, immunization with these sporozoites results in immune responses identical to RAS. The promise of vaccination using these genetically attenuated sporozoites (GAS) depends on translating the results in rodent malaria models to human malaria. In this study, we perform the first essential step in this transition by disrupting, p52, in P. falciparum an ortholog of the rodent parasite gene, p36p, which we had previously shown can confer long lasting protective immunity in mice. These P. falciparum P52 deficient sporozoites demonstrate gliding motility, cell traversal and an invasion rate into primary human hepatocytes in vitro that is comparable to wild type sporozoites. However, inside the host hepatocyte development is arrested very soon after invasion. This study reveals, for the first time, that disrupting the equivalent gene in both P. falciparum and rodent malaria Plasmodium species generates parasites that become similarly arrested during liver stage development and these results pave the way for further development of GAS for human use.

Published
2008

8. Reclassification of 300 primary cutaneous B-Cell lymphomas according to the new WHO-EORTC classification for cutaneous lymphomas: comparison with previous classifications and identification of prognostic markers.

Author

Senff, N.J., Hoefnagel, J.J., Jansen, P.A.M., Vermeer, M.H., Baarlen, J. van, Blokx, W.A.M., Dijk, M.R. van, Geerts, M.L., Hebeda, K.M., Kluin, P.M., Lam, K.H., Meijer, C.J., Willemze, R., Senff, N.J., Hoefnagel, J.J., Jansen, P.A.M., Vermeer, M.H., Baarlen, J. van, Blokx, W.A.M., Dijk, M.R. van, Geerts, M.L., Hebeda, K.M., Kluin, P.M., Lam, K.H., Meijer, C.J., and Willemze, R.

Abstract

Contains fulltext : 52490.pdf (publisher's version ) (Closed access), PURPOSE: In the new WHO-European Organisation for Research and Treatment of Cancer (WHO-EORTC) classification for cutaneous lymphomas three major groups of primary cutaneous B-cell lymphoma (CBCL) are distinguished: primary cutaneous marginal zone B-cell lymphoma (PCMZL) and primary cutaneous follicle center lymphoma (PCFCL) with a good prognosis, and primary cutaneous large B-cell lymphoma, leg type (PCLBCL-LT), with an intermediate-level prognosis. This study aimed to assess the clinical significance of the new classification compared with previous classification schemes (EORTC 1997; WHO 2001) and to define prognostic factors within the newly defined categories. PATIENTS AND METHODS: In the present study clinical data and histologic sections of 300 patients with CBCL, formerly classified according to the EORTC classification, were reviewed and reclassified according to the WHO and the new WHO-EORTC classification schemes. RESULTS: After reclassification, the study comprised 71 patients with PCMZL, 171 patients with PCFCL, and 58 patients with PCLBCL-LT, showing 5-year disease-specific survivals of 98%, 95%, and 50%, respectively. When compared with the EORTC and WHO schemes, 5.3% and 36.3% of patients with CBCL were reclassified into another prognostic category. Multivariate analysis of PCFCL revealed localization on the leg and expression of FOXP1 as independent parameters associated with a poor prognosis. Expression of Bcl-2 or MUM-1 had no significant effect on survival in this group. In PCLBCL-LT, no independent prognostic parameters were found. CONCLUSION: These results emphasize the clinical significance of the WHO-EORTC classification, but suggest that within the group of PCFCL, distinction should be made between lymphomas presenting on the legs and lymphomas presenting at other sites.

Published
2007

9. Genetically attenuated P36p-deficient Plasmodium berghei sporozoites confer long-lasting and partial cross-species protection.

Author

Douradinha, B.G., Dijk, M.R. van, Ataide, R., Gemert, G.J.A. van, Thompson, J., Franetich, J.F., Mazier, D., Luty, A.J.F., Sauerwein, R.W., Janse, C.J., Waters, A.P., Mota, M.M., Douradinha, B.G., Dijk, M.R. van, Ataide, R., Gemert, G.J.A. van, Thompson, J., Franetich, J.F., Mazier, D., Luty, A.J.F., Sauerwein, R.W., Janse, C.J., Waters, A.P., and Mota, M.M.

Abstract

Contains fulltext : 51720.pdf (publisher's version ) (Closed access), Immunisation with live, radiation-attenuated sporozoites (RAS) or genetically attenuated sporozoites (GAS) of rodent plasmodial parasites protects against subsequent challenge infections. We recently showed that immunisation with Plasmodium berghei GAS that lack the microneme protein P36p protects mice for a period of up to 4 months. Here, we show that the period of full protection induced by p36p(-)-sporozoites lasts 12 and 18 months in C57Bl6 and BALB/c mice, respectively. Full protection is also achieved with three doses of only 1000 p36p(-) (but not RAS) sporozoites. Subcutaneous, intradermal or intramuscular routes of administration also lead to partial protection. In addition, immunisation with either P. berghei RAS- or, to a lesser extent, p36p(-)-sporozoites inhibits parasite intrahepatic development in mice challenged with Plasmodium yoelii sporozoites. Since naturally acquired malaria infections or subunit-based vaccines only induce short-term immune responses, the protection conferred by immunisation with p36p(-)-sporozoites described here further emphasises the potential of GAS as a vaccination strategy for malaria.

Published
2007

10. Pfs47, paralog of the male fertility factor Pfs48/45, is a female specific surface protein in Plasmodium falciparum.

Author

Schaijk, B.C.L. van, Dijk, M.R. van, Vegte-Bolmer, M.G. van de, Gemert, G.J.A. van, Dooren, M.W. van, Eksi, S., Roeffen, W.F.G., Janse, C.J., Waters, A.P., Sauerwein, R.W., Schaijk, B.C.L. van, Dijk, M.R. van, Vegte-Bolmer, M.G. van de, Gemert, G.J.A. van, Dooren, M.W. van, Eksi, S., Roeffen, W.F.G., Janse, C.J., Waters, A.P., and Sauerwein, R.W.

Abstract

Contains fulltext : 49758schaijk.pdf (publisher's version ) (Closed access), The genome of Plasmodium falciparum contains a small gene family that expresses proteins characterized by the presence of 6-cysteine domains. Most of these proteins are expressed on the surface of the parasite and some are known to play a role in cell-cell interactions. Two members of this family, Pfs48/45 and Pfs230, form a complex localized on the surface of gametes and are recognized as important targets for transmission-blocking vaccines. In this study we report the analysis of an additional member of this family, Pfs47 the closest paralog of Pfs48/45. We demonstrate that Pfs47 is expressed only in female gametocytes and is located on the surface of female gametes following emergence from red blood cells. In contrast to the critical function of P48/45 for male fertility, Pfs47 does not appear crucial for female fertility. Parasites lacking Pfs47 through targeted gene disruption, produce normal numbers of oocysts when included in the blood meal of the mosquito vector. In addition, three monoclonal antibodies against Pfs47 were unable to inhibit oocyst development when present in a blood meal containing wild type parasites. These results show redundancy in protein function for Pfs47 and reduce the support for candidacy of Pfs47 as a transmission-blocking vaccine target.

Published
2006

11. Genetically attenuated, P36p-deficient malarial sporozoites induce protective immunity and apoptosis of infected liver cells.

Author

Dijk, M.R. van, Douradinha, B.G., Franke-Fayard, B., Heussler, V., Dooren, M.W. van, Schaijk, B.C.L. van, Gemert, G.J.A. van, Sauerwein, R.W., Mota, M.M., Waters, A.P., Janse, C.J., Dijk, M.R. van, Douradinha, B.G., Franke-Fayard, B., Heussler, V., Dooren, M.W. van, Schaijk, B.C.L. van, Gemert, G.J.A. van, Sauerwein, R.W., Mota, M.M., Waters, A.P., and Janse, C.J.

Abstract

Contains fulltext : 47790schaijk.pdf (publisher's version ) (Closed access), Immunization with Plasmodium sporozoites that have been attenuated by gamma-irradiation or specific genetic modification can induce protective immunity against subsequent malaria infection. The mechanism of protection is only known for radiation-attenuated sporozoites, involving cell-mediated and humoral immune responses invoked by infected hepatocytes cells that contain long-lived, partially developed parasites. Here we analyzed sporozoites of Plasmodium berghei that are deficient in P36p (p36p(-)), a member of the P48/45 family of surface proteins. P36p plays no role in the ability of sporozoites to infect and traverse hepatocytes, but p36p(-) sporozoites abort during development within the hepatocyte. Immunization with p36p(-) sporozoites results in a protective immunity against subsequent challenge with infectious wild-type sporozoites, another example of a specifically genetically attenuated sporozoite (GAS) conferring protective immunity. Comparison of biological characteristics of p36p(-) sporozoites with radiation-attenuated sporozoites demonstrates that liver cells infected with p36p(-) sporozoites disappear rapidly as a result of apoptosis of host cells that may potentiate the immune response. Such knowledge of the biological characteristics of GAS and their evoked immune responses are essential for further investigation of the utility of an optimized GAS-based malaria vaccine.

Published
2005

12. A central role for P48/45 in malaria parasite male gamete fertility.

Author

Dijk, M.R. van, Janse, C.J., Thompson, J., Waters, A.P., Braks, J.A.M., Dodemont, H.J., Stunnenberg, H.G., Gemert, G.J.A. van, Sauerwein, R.W., Eling, W.M.C., Dijk, M.R. van, Janse, C.J., Thompson, J., Waters, A.P., Braks, J.A.M., Dodemont, H.J., Stunnenberg, H.G., Gemert, G.J.A. van, Sauerwein, R.W., and Eling, W.M.C.

Abstract

Contains fulltext : 185544.pdf (publisher's version ) (Closed access), Fertilization and zygote development are obligate features of the malaria parasite life cycle and occur during parasite transmission to mosquitoes. The surface protein PFS48/45 is expressed by male and female gametes of Plasmodium falciparum and PFS48/45 antibodies prevent zygote development and transmission. Here, gene disruption was used to show that Pfs48/45 and the ortholog Pbs48/45 from a rodent malaria parasite P. berghei play a conserved and important role in fertilization. p48/45- parasites had a reduced capacity to produce oocysts in mosquitoes due to greatly reduced zygote formation. Unexpectedly, only male gamete fertility of p48/45- parasites was affected, failing to penetrate otherwise fertile female gametes. P48/45 is shown to be a surface protein of malaria parasites with a demonstrable role in fertilization.

Published
2001

13. Imaging the (un)imaginable of the Barrier Immune system

Author

Guo, N., Koning, F., Pascutti, M.F., Quint, K.D., Ossendorp, F.A., Yazdanbakhsh, M., Mebius, R.E., Dijk, M.R. van, and Leiden University

Subjects
Imaging mass cytometry, Mycosis Fungoides, Human intestine, Psoriasis, Mass cytometry, Proliferating cells
Abstract

This thesis focused on investigate immune compartmentalization in the developing human intestine, and lesional⁠/healthy skin tissue from patients with mycosis fungoides and psoriasis by single-cell spectral flow cytometry, suspension mass cytometry, single-cell RNA-sequencing, functional assays, RNAscope and imaging mass cytometry⁠.

Published
2023

14. Cutaneous CD30-positive lymphoproliferations

Author

Melchers, R.C., Vermeer, M.H., Willemze, R., Quint, K.D., Dijk, M.R. van, Bekkenk, M.W., Doorn, R. van, Veelken, J.H., Neelis, K.J., Jansen, P.M., and Leiden University

Subjects
Cutaneous lymphoma, Whole genome sequencing, Lymphomatoid papulosis, Second hematological malignancy, Brentuximab vedotin, ALK translocation, Primary anaplastic large cell lymphoma
Abstract

Cutaneous lymphomas originate from cancer of the lymphocytes in the skin without lymph node/organ involvement at time of diagnosis. There are many types of cutaneous lymphomas, with this thesis focusing on CD30-positive cutaneous lymphomas, consisting of a spectrum with lymphomatoid papulosis (LyP) on one side, and primary cutaneous anaplastic large cell lymphoma (C-ALCL) on the other. LyP is characterized by multiple skin lesion that resolve spontaneously, and C-ALCL by a solitary or grouped tumor that persists. This thesis shows that approximately 15% of LyP patients develop a second skin lymphoma/blood cancer, but also have an increased risk of developing other cancers (squamous cell carcinoma/melanoma/colon/lung/bladder cancer). At molecular level, a subcategory of patients was found in C-ALCL with ALK translocations, suggestive of a systemic lymphoma. It appears that these patients also have a favorable prognosis and can be treated with radiotherapy. The optimal dose of radiotherapy was also demonstrated (8 Gray). In addition, different types of mutations (PI-3-K/MAPK/G pathways) seem to occur in C-ALCL compared to more aggressive lymphomas (JAK-STAT). C-ALCL patients with ≤5 tumors are best treated with radiotherapy, and patients with >5 lesions with methotrexate. Targeted therapies remain for patients not responding to methotrexate or with systemic involvement.

Published
2023

15. Clinical staging and prognostic factors in folliculotropic mycosis fungoides

Author

Santen, S. van, Willemze, R., Vermeer, M.H., Jansen, P.M., Smit, V.T.H.B.M., Veelken, J.H., Bekkenk, M.W., Dijk, M.R. van, and Leiden University

Subjects
Mycosis fungoides, Cutaneous T cell lymphomas, Folliculotropic mycosis fungoides
Abstract

Folliculotropic mycosis fungoides (FMF) is a distinct variant of mycosis fungoides (MF), the most prevalent type of cutaneous T cell lymphoma. FMF accounts for approximately 10% of all MF cases and is generally characterized by distinct clinical , histopathologic and prognostic features. The studies in this thesis were aimed to address questions regarding clinical staging, disease course, suitable treatment and prognosis of subgroups of patients with FMF.

Published
2021

16. Diagnostic and prognostic markers of cutaneous lymphomas

Author

Schrader, A.M.R., Willemze, R., Vermeer, M.H., Jansen, P.M., Smit, V.T.H.B.M., Dijk, M.R. van, Koens, L., and Leiden University

Subjects
TOX, Cutaneous B-cell lymphoma, immune system diseases, Cutaneous T-cell lymphoma, hemic and lymphatic diseases, Diagnosis, Pathology, Molecular diagnostics, MYC, TP63, Prognosis, NF-kB pathway
Abstract

This thesis comprises immunophenotypic and molecular studies in several types of cutaneous lymphomas. These studies provide a better definition of the clinicopathologic entities and provide adjunctive diagnostic markers that may aid in diagnosis of these patients in routine diagnostics, including TOX expression in cutaneous T-cell lymphomas and MYC expression and MYC rearrangements in cutaneous B-cell lymphomas (CBCLs). Also, the results demonstrate that adverse prognostic factors in systemic lymphomas are not directly transferrable to cutaneous lymphoma patients, including TP63 rearrangements in primary cutaneous CD30+ lymphoproliferative disorders and double hit status in CBCL, underlining the importance of a separate classification system for cutaneous lymphomas. Finally, these studies may have consequences for the management and treatment of patients with cutaneous lymphomas, because of the identification of recurrent molecular alterations that could provide attractive targets for novel therapeutics, including MYD88 and CD79B mutations in patients with intravascular large B-cell lymphomas.

Published
2020

17. The interplay of curriculum structure and professional identity formation of medical students : Birds of a feather flock together

Author

Broek, Willemina Elisabeth Sjoukje van den, Dijk, M.R. van, Cate, T.J. ten, Wijnen-Meijer, M., and University Utrecht

Subjects
professional identity formation, medical education, curriculum structure
Abstract

Professional identity formation (PIF) of medical trainees is defined as “a representation of self, achieved in stages over time during which the characteristics, values, and norms of the medical profession are internalized, resulting in an individual thinking, acting, and feeling like a physician”. Although important, medical education takes place within curricular structures that are often not deliberately created with PIF in mind. The thesis explores the interaction between curriculum structures and PIF in two recently introduced curricular structures: 1) The Bachelor-Master structure, providing an option to interrupt or terminate medical studies; 2) The final year of medical school designed as a transitional year to graduation, during which students work in authentic settings with the clinical responsibilities approaching the level of a starting resident, in elective rotations. We found that the Bachelor-Master structure does not stimulate students in any way to permanently stop their medical training, but there seems to be a tendency to insert a break in the program at the bachelor-master transition. This can also be seen as an interruption of PIF. For the transitional year, findings in the thesis suggest that transitional-year electives lead to early specialty preference streaming. We also found a relation between transitional-year characteristics and students identifying with members of the professional group, a process called ‘social identification’. Finally, we found relatively small differences between strength of identification with professional and interprofessional groups, suggesting that at this stage of training PIF does not seem to hamper interprofessional group processes.

Published
2020

18. Diagnostic and prognostic markers in tumor stage mycosis fungoides and Sézary syndrome

Author

Boonk, S.E., Vermeer, M.H., Willemze, R., Tensen, C.P., Dijk, M.R. van, Sigurdsson, V., Veelken, J.H., and Leiden University

Subjects
Mycosis fungoides, Diagnostic biomarkers, Erythrodermic inflammatory dermatoses, Sézary syndrome, Prognosis
Abstract

The studies described in this thesis focused on identifying diagnostic and prognostic markers in tumor stage mycosis fungoides (stage IIB) and Sézary syndrome. Sézary syndrome is a type of cutaneous T-cell lymphoma, characterized by an erythroderma, lymphadenopathy and malignant T cells in skin, lymph nodes and blood. Especially in the early stages of disease, it can be difficult to differentiate Sézary syndrome from erythrodermic inflammatory dermatoses. The studies identified immunohistochemical (TOX), immunophenotypic (CD7, CD26), molecular (STAT4, TWIST1, DNM3/ PLS3) and epigenetic (CMTM2) markers that are useful as additional diagnostic markers to discriminate Sézary syndrome from erythrodermic inflammatory dermatoses. Of the molecular markers, PLS3 expression was an important prognostic factor in Sézary syndrome. In addition, it was shown that the number of tumors and time interval between tumor formation differs greatly among patients with mycosis fungoides stage IIB and these differences correlate with survival. Patients that developed four or more tumors during the first 6 months after diagnosis of stage IIB have a poor prognosis.

Published
2017

19. PD-1 Expression in primary cutaneous lymphoma

Author

Cetinozman, F., Willemze, R., Jansen, P.M., Dijk, M.R. van, Krieken, J.H.J.M van, Smit, V.T.H.B.M., Vermeer, M.H., and Leiden University

Subjects
Mycosis fungoides, Programmed death-1, Cutaneous lymphoma, Sézary syndrome, hemic and lymphatic diseases, Programmed death-1, Cutaneous lymphoma, Sézary syndrome, Mycosis fungoides, Erythroderma, Immunohistochemistry, Immunohistochemistry, Erythroderma
Abstract

The molecule programmed death-1 (PD-1) is a critical element in the negative regulation of cellular immune responses. Blockage of the interaction between PD-1 and its ligand PD-L1 has emerged as a promising therapeutic approach for several cancers underlining the importance of this molecule. Expression of PD-1 has been used as valuable marker in the differentiation between different types of T-cell non-Hodgkin lymphoma. The studies presented in this thesis are focused on the expression of PD-1 in primary cutaneous T-cell lymphomas and cutaneous B-cell lymphomas in order to determine whether expression of PD-1 might also be a useful marker in the diagnosis of different types of cutaneous lymphoma. Differentiation between the different types of cutaneous lymphoma is extremely important, as they have a completely different prognosis and require different types of treatment. The investigations in this thesis provide a detailed description of the differential expression of PD-1 in distinct types of cutaneous lymphomas, revealing that PD-1 has the potential of a diagnostic biomarker, especially for Sézary syndrome and primary cutaneous small/medium-sized pleomorphic T cell lymphoma. The overall conclusion is that PD-1 may serve as a suitable adjunct to improve diagnosis, and may enable better classification of provisionally classified cutaneous lymphoma entities.

Published
2016

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