Your search keyword '"Scott Walsh"' showing total 2 results

1. Sezary Syndrome and Combination Immunomodulatory Therapy: Improving Clinical Outcomes

Author

Eugenia Piliotis, Neil H. Shear, Kevin Imrie, David Barth, Panayiota Govas, Cathy Fairlie, Scott Walsh, and Matthew C. Cheung

Subjects

medicine.medical_specialty, Chemotherapy, Mycosis fungoides, Chlorambucil, business.industry, medicine.medical_treatment, Immunology, Cutaneous T-cell lymphoma, Erythroderma, Cell Biology, Hematology, medicine.disease, Biochemistry, Chemotherapy regimen, Surgery, Internal medicine, Medicine, business, Progressive disease, Sezary Cell, medicine.drug

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.

Published

2008

2. Baseline Demographics and Disease Characteristics of Patients with Hypereosinophilic Syndrome in a Placebo-Controlled Trial Evaluating the Steroid-Sparing Effects of the Anti-IL-5 Monoclonal Antibody, Mepolizumab

Author

Scott Walsh, Lawrence B. Schwartz, Johannes Huss-Marp, Gerald J. Gleich, and William W. Busse

Subjects

medicine.medical_specialty, Hypereosinophilic syndrome, business.industry, Immunology, Placebo-controlled study, Cell Biology, Hematology, Gene rearrangement, medicine.disease, Biochemistry, Gastroenterology, Imatinib mesylate, Prednisone, Internal medicine, medicine, Eosinophilia, medicine.symptom, business, Mepolizumab, Interleukin 5, medicine.drug

Abstract

Mepolizumab is a humanized anti-IL-5 monoclonal antibody that blocks the actions of IL-5, the hematopoietin most responsible for eosinophil production, differentiation, and survival. Clinical experience in small numbers of patients with hypereosinophilic syndrome (HES), asthma, and atopic dermatitis indicated that intravenous (IV) mepolizumab therapy was associated with a reduction in blood eosinophils and was well-tolerated. A multicenter (26 sites worldwide), randomized, double-blind, placebo-controlled, and parallel-group trial has been conducted to evaluate the steroid-sparing effects of mepolizumab in patients with HES, and its efficacy and safety in controlling the signs and symptoms of this disease. The trial recruited patients 18–85 years of age with HES (blood eosinophil count >1500/μl for ≥6 months with evidence of eosinophilia-related organ involvement or dysfunction, without any known cause of eosinophilia), who tested negative for the FIP1L1-PDGFRα gene rearrangement and required 20–60 mg/day prednisone (monotherapy) to maintain blood eosinophils at Patient demographics Placebo (n=42) Mepolizumab (n=43) Total (n=85) Age, y (mean±SD) 49.1±14.4 47.0±16.2 48.1±15.3 Men, % 17 (40%) 26 (60%) 43 (51%) Caucasian, % 34 (81%) 38 (88%) 72 (85%) Weight, kg (mean±SD) 79.7±18.3 80.9±22.2 80.3±20.3 BMI, kg/m2 (mean±SD) 27.8±5.8 27.0±6.4 27.4±6.1 Baseline prednisone≤30 mg, n (%) 30 (71%) 30 (70%) 60 (71%) Baseline prednisone >30 mg, n (%) 12 (29%) 13 (30%) 25 (29%) Previously treated for HES, n (%) 40 (95%) 41 (95%) 81 (95%) HES duration, y (mean±SD) 6.5±9.5 4.3±5.6 5.4±7.8 Age at HES onset, y (mean±SD) 42.7±16.2 42.7±17.7 42.7±16.9

Published

2006