Your search keyword '"Marc Geirnaert"' showing total 2 results

1. A Descriptive Analysis of Obinutuzumab Usage in a Single Canadian Centre

Author

Spencer B. Gibson, James B. Johnston, Oliver Bucher, Nicole Bourrier, Mandy Squires, Versha Banerji, David E. Dawe, Ivan Landego, Zeb Aurangzeb, Marc Geirnaert, Irena Hibbert, Theresa L. Whiteside, and Erin Streu

Subjects

education.field_of_study, medicine.medical_specialty, Chlorambucil, business.industry, Incidence (epidemiology), Immunology, Population, Cell Biology, Hematology, Gene mutation, Biochemistry, chemistry.chemical_compound, Tolerability, chemistry, Obinutuzumab, Internal medicine, Cohort, Medicine, Progression-free survival, education, business, medicine.drug

Abstract

Background:Chronic lymphocytic leukemia (CLL) is the most prevalent leukemia in North America with the majority of patients being over the age of 70 (Goede et al, 2014). CLL is a heterogeneous disease with some patients undergoing treatment at time of diagnosis, while others follow along a more indolent, asymptomatic course. When indicated, the choice of treatment is based on the patient's functional status, renal function and other comorbidities (Shanafelt, 2013). Previous studies have shown that unfit patients treated with Obinutuzumab plus Chlorambucil have shown prolongation of progression free survival and higher rates of complete response compared to other monoclonal based regimens (Goede et al, 2014). The aim of this study is to investigate the clinical use and uptake of Obinutuzumab in combination with Chlorambucil in a Canadian based population. Methods:All patients receiving Obinutuzumab were identified using the CLL CAISIS database. Then a retrospective chart review was conducted for patients approved for first-line antibody treatment with Obinutuzumab from January 1, 2014 to December 31, 2017. Data including patient characteristics, patterns of treatment, reported toxicities, response rates and survival data were collected and analyzed. This data was used to determine the overall safety and efficacy of this treatment regimen. Results: There were a total of 66 patients that met the inclusion criteria for this study. This cohort consisted of 54.5% males and 45.5% females, with a median age at diagnosis of 68 years (range: 46-94). Within this population 47 patients underwent florescence in situ hybridization testing, which identified 32 patients with chromosomal abnormalities. The immunoglobulin heavy chain variable region gene mutation was also tested in 41 patients, and identified 22 patients that were unmutated. At the time of treatment the median age was 73 (range: 55-98) with a median Cumulative Illness Rating Scale (CIRS) score of 8 (range: 3-15). Of the 66 patients who started treatment with Obinutuzumab, 50 patients (76%) achieved a partial response and 5 patients (8%) had no response. Of note, 21 patients (31.8%) discontinued treatment prior to completion of all six cycles due to cytopenias (4), other comorbidities (4), progression of CLL (2), decline in functional/mental status (2), patient request (2) and other (7). In regards to their treatment there was a high incidence of infusion related reactions (IRRs) on the first day of treatment, with 30 patients (45.5%) requiring intervention. There was a subset of 15 patients that had received low dose Chlorambucil prior to treatment with Obinutuzumab which resulted in a lower average lymphocyte count (38.1) and lower rate of IRRs (33%) compared to those with no prior Chlorambucil (average lymphocyte count: 66.5, rate of IRR: 42%). Due to toxicity and tolerability of Chlorambucil, dose reduction was observed in 37 patients (56%) throughout all six cycles of treatment. In the end, only 18 patients (27.3%) received all doses of Obinutuzumab and Chlorambucil while 37 patients (56%) received all doses of Obinutuzumab. Within the entire cohort, 12 patients have relapsed and 9 of these patients have required additional therapy. This relapse rate can be attributed to lack of response to Obinutuzumab (3), a 17p del (1), poor prognostic markers (5), and inadequate Obinutuzumab (1). Conclusion:In this current study, our results demonstrate that the majority of patients in this cohort were able to complete treatment with Obinutuzumab. Although our demographics were similar to previous studies, we found higher partial response rates (76%) likely due to differences in standards of practice, such as imaging studies after treatment. Disclosures Whiteside: Roche: Membership on an entity's Board of Directors or advisory committees, Other: teaching sessions. Dawe:AstraZeneca: Membership on an entity's Board of Directors or advisory committees; Merck: Membership on an entity's Board of Directors or advisory committees. Johnston:Roche: Other: unrestricted grant received in the past; Abbvie: Other: unrestricted grant received in the past; Teva: Other: unrestricted grant received in the past; Gilead: Other: unrestricted grant received in the past; Janssen: Other: unrestricted grant received in the past. Banerji:Roche: Other: Unrestricted grant received in the past; Janssen: Other: Unrestricted grant received in the past; Abbvie: Other: Unrestricted grant received in the past; Gilead: Other: Unrestricted grant received in the past; Teva: Other: Unrestricted grant received in the past.

Published

2018

2. Population Based Study on the Utilization and Cost of Azacitidine In a Canadian Province

Author

Kristjan Paulson, Matthew D. Seftel, Sri Navaratnam, Venetia Bourrier, Bernie Lozar, Marc Geirnaert, Rajat Kumar, Pat Burns, Donald S. Houston, and Pamela Skrabek

Subjects

Cytopenia, Pediatrics, medicine.medical_specialty, education.field_of_study, business.industry, medicine.medical_treatment, Immunology, Population, Cell Biology, Hematology, Hematopoietic stem cell transplantation, medicine.disease, Biochemistry, law.invention, Clinical trial, Randomized controlled trial, law, Cohort, medicine, Adverse effect, business, education, Febrile neutropenia

Abstract

Abstract 1508 Background: Azacitidine (AZA) is an efficacious therapy for high risk Myelodysplastic Syndrome (MDS). In a randomized trial by Fenaux et al. patients were treated with a median of 9 cycles of AZA at 75mg/m2/day × 7 days every 28 days. Based on the published treatment regimen (Lancet Oncol 2009; 10: 223-32), the average cost of AZA is estimated to be $10,000 Canadian dollars per month. With a median of nine full dose cycles of AZA cost per patient is anticipated to be $90,000. In many health care systems, AZA has not been approved, due to financial constraints. Population based studies may provide a more realistic estimate of AZA drug utilization and cost. The province of Manitoba (population 1.2 million) offers a unique opportunity to perform population based studies, as provincial health and pharmacy services capture information regarding administration of parenteral drugs like AZA. Although AZA is not funded by the province, it was provided by the manufacturer on compassionate basis for any patient who met the approved criteria from April 2009 to 31 March 2010. Enrolled patients continued to receive the drug even after March 2010. The drug was administered at a single site. Methods: All patients enrolled during the period of compassionate use (April 2009-31 March 2010) who received one or more doses of AZA were prospectively followed for drug administration, response, toxicity and outcome. For this analysis, the last follow up was 31 July 2010. Results: Eleven eligible patients received at least one cycle of AZA. The diagnosis was MDS in 8, AML in remission with underlying MDS in 2 and CMML in 1. Four of eleven patients had therapy-related MDS and two patients were ECOG >2 at onset of therapy. A total of 42 cycles were given with a median of 3.0 (range 1–9) cycles per patient. There was a 25–50% dose reduction in 9 of 42 cycles (21%) due to cytopenias. Eleven of 42 cycles (26%) were complicated by febrile neutropenia, with 7 of these episodes requiring hospital admission. Reasons for discontinuing AZA were: (a) progressive cytopenia or transformation to AML in four (b) acceptance for allogeneic hematopoietic stem cell transplantation (HSCT) in three (c) severe sepsis during therapy in two (d) lack of objective response in one. Only one patient continues on AZA. Hematologic improvement and transfusion independence was seen in 5/11 and 3/11 patients respectively. There were two patients with bone marrow complete response (CR) in addition to hematologic improvement, one of whom underwent HSCT. The approximate cost of AZA in this cohort is $34,090 per patient. Conclusion: In this population based study, we demonstrate that many MDS patients are withdrawn from further treatment due to adverse effects or lack of early response, in contrast to patients participating in clinical trials. Despite receiving dose reductions and fewer total cycles of AZA, a comparable number of patients (45.5%) had objective responses. Our study suggests that the actual drug acquisition cost would be just over one third (38%) of the projected cost based on clinical trial data. Decisions to fund or deny expensive drugs should include data from population based studies. Disclosures: Kumar: Celgene: Membership on an entity's Board of Directors or advisory committees.

Published

2010