Sezary Syndrome and Combination Immunomodulatory Therapy: Improving Clinical Outcomes

Blood ◽  
2008 ◽  
Vol 112 (11) ◽  
pp. 4957-4957 ◽  
Author(s):  
Eugenia Piliotis ◽  
Panayiota Govas ◽  
Kevin R Imrie ◽  
Matthew C Cheung ◽  
Neil Shear ◽  
...  
Keyword(s):  
Median Survival ◽  
Peripheral Blood ◽  
Progressive Disease ◽  
Age At Diagnosis ◽  
Immunomodulatory Therapy ◽  
Sézary Syndrome ◽  
Base Line ◽  
Sezary Syndrome ◽  
Historical Series ◽  
Peripheral Blood Involvement

Abstract Introduction: Sezary syndrome is a rare, aggressive and advanced stage of cutaneous T cell lymphoma where patients exhibit total body erythroderma and peripheral blood involvement. Patients can progress from preexisting mycoses fungoides or present de-novo. Historically median survival has been less than two years however with current combinations of skin directed and immunomodulatory therapy median survival has been documented up to 3–4 years, however randomized trials are lacking given the rarity of this disorder. We describe the outcomes 23 patients followed in our centre diagnosed with sezary syndrome based on peripheral blood involvement and erythroderma who have been treated primarily with combination skin and immunomodulatory therapy. Methods: A review of all patients diagnosed with sezary syndrome in our centre was conducted. Base line characteristics, survival, number and type of therapies as well as responses to treatments were recorded Results: 23 patients were identified. 11 male, 12 female, average age at diagnosis 64.7 yrs (range 47–85). Therapies included total skin electron beam (TSEB), PUVA, Interferon, oral retinoids, and extracorporeal photophoresis (ECP). 5 patients had received prior traditional chemotherapy including CHOP, chlorambucil and purine analogues with either no or transient responses. 19 patients received a combination of all 5 therapies. 19 patients received IFN, 13 TSEB, 21 PUVA, 18 ECP and 16 oral retinoids. 7 patients received 3 or fewer therapies (3 in process of escalating therapy, 1 CR to TSEB, 3 pts refused multiagent therapy as elderly and stable on PUVA +/− retinoids). 6 patients achieved a durable complete remission while on therapy (4 received IFN/TSEB/PUVA/ECP, 1 IFN/PUVA/ECP, 1 TSEB alone), 3 patients had progressive disease, and the remainder either had partial responses or stable disease. Median follow-up was 44 months (range 9–127). Median survival of the entire cohort was 37 months (mean 52 months, range 6–108 months, 5 patients have been diagnosed in the last 12 months). There have been 5 deaths to date, median 43 months (range 33–101) from the time of diagnosis. Cause of death included 2 cardiac, 1 renal, 1 infection, and 1 progressive disease. There was no correlation between survival and LDH at presentation, sezary cell count or number of therapies. There was a modest correlation between survival and age at diagnosis (R2=0.1263). Patients who received TSEB had an average of 57 months survival vs. 33.5 months than those who did not, however this was not statistically significant. Reasons not to receive TSEB included 5 patient refusal, 3 still escalating therapy, 2 had adequate response to other therapies. Patients who achieved a CR to therapy had a median survival of 63 months (average 65 months) vs. those who did not achieve a CR had a median survival of 22 months (average 65 months). Conclusions: Patients receiving combination immunotherapy and skin based treatments for sezary syndrome appear to be living longer than historical series. Given the small number of this cohort it was not possible to statistically determine variables predictive of prolonged survival, however patients who received TSEB and or achieved a CR to treatment had median survival of approximately 5 years. The majority of patients received maintenance immunotherapy to sustain disease control.

scholarly journals The Role of Tumor Microenvironment in the Pathogenesis of Sézary Syndrome

2022 ◽  
Vol 23 (2) ◽  
pp. 936
Author(s):  
Denis Miyashiro ◽  
Bruno de Castro e Souza ◽  
Marina Passos Torrealba ◽  
Kelly Cristina Gomes Manfrere ◽  
Maria Notomi Sato ◽  
...  
Keyword(s):  
Tumor Microenvironment ◽  
Immune Dysregulation ◽  
Sézary Syndrome ◽  
Sezary Syndrome ◽  
Immunologic Response ◽  
T Cell Lymphomas ◽  
Sézary Cells ◽  
Peripheral Blood Involvement ◽  
Malignant T Cells

Sézary syndrome is an aggressive leukemic variant of cutaneous T-cell lymphomas, characterized by erythroderma, lymphadenopathy, and peripheral blood involvement by CD4+ malignant T-cells. The pathogenesis of Sézary syndrome is not fully understood. However, the course of the disease is strongly influenced by the tumor microenvironment, which is altered by a combination of cytokines, chemokines, and growth factors. The crosstalk between malignant and reactive cells affects the immunologic response against tumor cells causing immune dysregulation. This review focuses on the interaction of malignant Sézary cells and the tumor microenvironment.

Transformation of Mycosis Fungoides/Sezary Syndrome: Clinical Characteristics and Prognosis

Blood ◽  
1998 ◽  
Vol 92 (4) ◽  
pp. 1150-1159 ◽  
Author(s):  
Eleni Diamandidou ◽  
Maria Colome-Grimmer ◽  
Luis Fayad ◽  
Madeleine Duvic ◽  
Razelle Kurzrock
Keyword(s):  
Mycosis Fungoides ◽  
Median Survival ◽  
Cell Transformation ◽  
Large Cell ◽  
Lactic Dehydrogenase ◽  
Cumulative Probability ◽  
Sézary Syndrome ◽  
Sezary Syndrome ◽  
Large Cell Transformation ◽  
American Society

Abstract The occurrence of large cell transformation has been well documented in a subgroup of patients with mycosis fungoides/Sezary syndrome (MF/SS). However, because of the rarity of MF/SS, little is known about the influence of clinicopathologic features in predicting large cell transformation and about outcome in the transformed cases. We evaluated all patients with MF/SS who were registered in our clinic during the study period and for whom pathologic slides for review were available or could be obtained. Disease was classified as transformed if biopsy showed large cells (≥4 times the size of a small lymphocyte) in more than 25% of the infiltrate or if they formed microscopic nodules. Twenty-six patients with transformation were identified from a total of 115 evaluable cases with a diagnosis of MF/SS. The actuarial cumulative probability of transformation reached 39% in 12 years. The median time from diagnosis of MF/SS to transformation was 12 months (range, 0 to 128 months). Thirty-one percent of all patients with stage IIB-IV disease at presentation eventually transformed versus 14% of those with stage I-IIA (P= .03), with transformation being especially common in patients with tumors (T3), 46% of whom transformed. Combining elevated β2 microglobulin and lactic dehydrogenase (neither elevated v one or both elevated) was also predictive for transformation (P = .009). The median survival from initial diagnosis of MF/SS for the transformed patients was 37 months versus 163 months for the untransformed group (P = .0029). The median survival from transformation was 19.4 months (range, 2+ to 138 months). The following characteristics were associated with an inferior survival in transformed patients: (1) early transformation (<2 years from the diagnosis v ≥2 years; P = .011) and (2) advanced stage (IIB-IV v I-IIA; 2-year survival, 23% v 86%;P = .0035). We conclude that MF/SS patients with stages IIB-IV disease and, in particular, those with tumors have a high incidence of large-cell transformation. Patients with transformation have a relatively poor survival, especially if transformation occurs early (within 2 years) in the course of disease or if they are staged as IIB or higher. © 1998 by The American Society of Hematology.

Phase I/II Study of Oral FodosineTM, a PNP Inhibitor in Refractory Cutaneous T-Cell Lymphoma Patients.

Blood ◽  
2005 ◽  
Vol 106 (11) ◽  
pp. 2683-2683 ◽  
Author(s):  
Madeleine Duvic ◽  
Debra Breneman ◽  
Maureen Cooper ◽  
Gustavo Fonseca ◽  
J. Claude Bennett ◽  
...  
Keyword(s):  
T Cell ◽  
Mycosis Fungoides ◽  
Progressive Disease ◽  
Treatment Cycle ◽  
Cell Lymphoma ◽  
Preliminary Evidence ◽  
Sézary Syndrome ◽  
Sezary Syndrome ◽  
Minor Response

Abstract Suppression of T-cell immunity seen in children with inherited purine nucleoside phosphorylase (PNP) deficiency supports the potential application of PNP inhibitors for the therapy of T-cell malignancies. Forodesine (FodosineTM) is a specific PNP inhibitor that raises plasma 2′-deoxyguanosine (dGuo) and intracellular dGTP levels, leading to T-cell apoptosis. IV administration of forodesine has shown activity in cutaneous T-cell lymphoma (CTCL) patients. To determine the safety, pharmacokinetics and pharmacodynamics of oral forodesine in patients with refractory CTCL, as well as preliminary evidence of efficacy, five cohorts of patients (≥ 3patients per cohort) were evaluated sequentially, receiving forodesine at 40, 80, 160, 320, and 480 mg/m2 once per day for 28 days. At the end of the treatment cycle (Day 28), all patients with stable or improved disease could enter a long-term, follow-up period. To date, 12 patients have been treated, 11 completing the 28-day cycle. Forodesine is orally absorbed (40%–50%), mean terminal half-life of 12 to 20 h. dGuo levels were elevated in all patients (0.8–2.8 μM, predose levels ≤ 0.004 μM). Forodesine was generally safe and well tolerated in this population. Safety data is available for first 7 patients. No serious adverse events possibly related to the drug occurred. The most common adverse event possibly drug related was nausea (2 patients). Of the 11 patients completing the treatment cycle, 9 began long-term treatment. Of these 9 patients, 4 have received >3 months of treatment, while 1 patient continues to receive for >8 months. Efficacy data are available for 8 patients: 2 with partial response, 3 with minor response, 2 with progressive disease, and 1 with stable disease (Table). Forodesine showed preliminary evidence of clinical activity in refractory CTCL patients. Additional clinical and pharmacodynamic data will be presented. Clinical and Pharmacodynamic Activity of Oral Forodesine In CTCL Patients Patient Diagnosis Dose (mg/m2) Treatment Plasma dGuo (Cmax, M) μ Clinical Response PR = partial response; MR = minor response; SD = stable disease; PD = progressive disease; N/A = not available 2001 Sezary syndrome (IVA) 40 Completed 0.6 PR 3001 Mycosis fungoides (IVB) 40 Completed 1.7 PD 3002 Mycosis fungoides (IIB) 40 Completed 1.2 MR 3003 Mycosis fungoides (IB) 80 Completed 1.2 MR 3004 Sezary syndrome (IVA) 80 Completed 1.0 MR 3005 Sezary syndrome 80 Completed 1.6 PD 2002 IIA 80 Completed 1.1 PR 2003 III 80 Completed 1.7 N/A 3006 Mycosis fungoides/Sezary syndrome (IVB) 160 Completed 2.8 SD 4001 III 320 Completed 1.8 N/A 1001 Mycosis fungoides (IB) 320 Completed 1.3 N/A 3012 Mycosis fungoides/Sezary syndrome (IVA vs B) 320 Not Completed N/A Not evaluable

Sezary Syndrome: Clinicopathological and Immunophenotypical Characteristics and Their Impact On Survival

Blood ◽  
2012 ◽  
Vol 120 (21) ◽  
pp. 5085-5085
Author(s):  
Darcie Deaver ◽  
Pedro Horna ◽  
Lubomir Sokol
Keyword(s):  
T Cell ◽  
Cell Count ◽  
Peripheral Blood ◽  
Nk Cell ◽  
Stage Iv ◽  
Absolute Lymphocyte Count ◽  
Sézary Syndrome ◽  
Sezary Syndrome ◽  
Stage Of Disease ◽  
Stage Iv Disease

Abstract Abstract 5085 Background: Sezary syndrome is a rare leukemic subtype of cutaneous T cell lymphoma with aggressive clinical behavior and poor prognosis compare to the most common type of CTCL, mycosis fungoides. Hematologic criteria for the diagnosis of Sezary syndrome include an absolute Sezary cell count of >1000cells/mm3 in peripheral blood the presence of a clonal T cell population, increased CD4/CD8 ratio, and aberrant expression of T cell markers. Objectives: To evaluate clinical, pathological and immunophenotypical characteristic in patients with Sezary syndrome and determine the impact of these factors on disease survival. Research Design and Methods: Retrospective chart review of 17 consecutive patients diagnosed with Sezary syndrome at Moffitt Cancer Center from January 1998-June 2012. Data points collected were age, gender, stage of disease, date of diagnosis, date of death, and analysis of peripheral blood by flow cytometry. Statistical analyses were performed by SPSS statistical software (IBM, Somers, NY). All causes of death were included in the survival analysis. Survival curves were estimated by the Kaplan-Meier method. Results: Of the 17 patients evaluated 10 (58. 8%) were female, and 7 (41. 2%) were male, median age was 71 years (range 50–89). Patients were staged according to 2007 ISCL/EORTC staging system 8 (47. 1%) stage III and 9 (52. 9%) stage IV. Median survival was 20. 9 months (range 0–107. 6) for all stages; 27 months and 9. 36 months for stage III and IV, respectively. As expected, stage IV disease was associated with a higher CD4:CD8 ratio (median 62. 5/uL versus 8. 6/uL), absolute lymphocyte count (median 9, 860/ul versus 2800), and absolute Sezary cell count (median of 8, 700/uL versus 1, 700/uL). Interestingly, stage IV disease was also associated with a higher absolute NK cell count (median 280/uL versus 60/uL) and a lower absolute CD8 T cell count (median 165/uL versus 290/uL). Of all parameters studied the only ones showing statistical correlation with the stage of disease were the NK cell count (p = 0. 018) and the CD4:CD8 ratio (p = 0. 039). The immunophenotype of the Sezary cells did not correlate with stage of disease. Survival analysis did not show any significant differences by grouping patients according to high or low levels of variables described above, although the series is small. Conclusion: We concluded that increased burden of disease in the peripheral blood did not affect overall survival in our patient population. However, Higher CD4:CD8 ratio, higher absolute lymphocyte count, and lower absolute CD8+ T cell count was associated with more advanced stage of disease suggesting that a lack of cytotoxic T cells can be responsible for profound immunosuppression and disease progression found in patients with advanced stage of CTCL. Disclosures: No relevant conflicts of interest to declare.

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