Abstract
Abstract 2800
Many patients with MDS require regular transfusions. Several reviews have documented poorer clinical outcomes and overall survival (OS) in transfusion-dependent MDS patients. A US registry of 600 lower-risk MDS patients prospectively collected data on clinical outcomes in chelated and non-chelated transfused patients. This 24-month interim analysis reports on cardiac events, leukemic transformation and OS.
This is a 5-year, non-interventional registry in MDS patients (aged ≥18 years) with lower-risk MDS (based on WHO, FAB and/or IPSS criteria) from 107 US centers. Patients had to have transfusional iron overload (serum ferritin ≥1000 μg/L and/or ≥20 packed red blood cell units and/or ongoing transfusion requirement of ≥6 units every 12 weeks). Follow-up was every 6 months for up to 60 months or death. Use of chelation therapy was not required. Chelated patients were those who had ever used iron chelation; a sub-analysis was done on patients with ≥6 months chelation. Assessments included demographics, disease status, MDS therapy, comorbidities, and causes of death. Differences between non-chelated and chelated patients are reported.
600 patients enrolled; as of May 26, 2011, 249 continued in the registry. 351 patients discontinued due to: lost to follow-up (n=51, 8.5%); death (n=278, 46.3%); other (n=22, 3.7%). 263/600 patients received chelation therapy, of whom 191 received ≥6 months.
Demographics, IPSS risk status and transfusion burden
| . | Non-chelated n(%)* . | Chelated n(%)* . | Chelated ≥6 months n(%)* . |
|---|---|---|---|
| Age, yrs Median (range) | 77 (47–99) | 75 (21–94) | 74 (21–94) |
| Male:Female ratio | 1.42:1 | 1.31:1 | 1.20:1 |
| IPSS risk status–low | 56 (33.7) | 56 (44.1) | 38 (40.0) |
| IPSS risk status - INT-1 | 110 (66.3) | 71 (55.9) | 57 (60.0) |
| Baseline ferritin, ng/mL Median (range) | 1353 (3–7379) | 1512 (81–16422) | 1500 (81–16422) |
| Median number of Lifetime units transfused | 20.0 | 39.0 | 44.0 |
| Units transfused/4 weeks while on registry | 1.51 | 2.11 | 2.19 |
| . | Non-chelated n(%)* . | Chelated n(%)* . | Chelated ≥6 months n(%)* . |
|---|---|---|---|
| Age, yrs Median (range) | 77 (47–99) | 75 (21–94) | 74 (21–94) |
| Male:Female ratio | 1.42:1 | 1.31:1 | 1.20:1 |
| IPSS risk status–low | 56 (33.7) | 56 (44.1) | 38 (40.0) |
| IPSS risk status - INT-1 | 110 (66.3) | 71 (55.9) | 57 (60.0) |
| Baseline ferritin, ng/mL Median (range) | 1353 (3–7379) | 1512 (81–16422) | 1500 (81–16422) |
| Median number of Lifetime units transfused | 20.0 | 39.0 | 44.0 |
| Units transfused/4 weeks while on registry | 1.51 | 2.11 | 2.19 |
n (%) unless otherwise indicated
Leukemic transformation and cardiac events were more common in non-chelated patients (Table 2). Time to leukemic transformation was significantly shorter in non-chelated versus chelated patients. A greater percentage of deaths occurred in non-chelated patients; time to death was significantly shorter in non-chelated versus chelated patients. The most frequent reasons for death were MDS/AML, cardiac, and infection.
Summary of AML transformation, cardiac events and deaths
| . | Patient categories . | ||
|---|---|---|---|
| Non-chelated n (%) . | Chelated . | ||
| All n (%) . | ≥6 months n (%) . | ||
| AML transformation | 30 (8.9) | 12 (4.6) | 10 (5.2) |
| Mean±SD time to transformation (mos) | 27.3±20.3 | 40.6±25.3 | 40.8±27.0 |
| Cardiac events | 155 (46.0) | 113 (43.0) | 76 (39.8) |
| Deaths | |||
| Number (%) | 171 (50.7) | 107 (40.7) | 70 (36.6) |
| Median (25th, 75th percentiles) time to death (mos)* | 52.2† (24.0, 136.2) | 99.3†‡ (54.1, NA) | 104.4‡ (63.4, NA) |
| Causes of Death | |||
| MDS/AML | 75 (22.3) | 47 (17.9) | 32 (16.8) |
| Cardiac | 28 (8.3) | 15 (5.7) | 10 (5.2) |
| Infection | 22 (6.5) | 8 (3.0) | 8 (4.2) |
| Unknown | 16 (4.7) | 10 (3.8) | 6 (3.1) |
| Other | 10 (3.0) | 9 (3.4) | 4 (2.1) |
| Malignancy | 9 (2.7) | 3 (1.1) | 0 |
| Respiratory | 7 (2.1) | 7 (2.7) | 4 (2.1) |
| Multiorgan failure | 2 (0.6) | 2 (0.8) | 2 (1.0) |
| CVA | 1 (0.3) | 4 (1.5) | 3 (1.6) |
| GvHD/transplant | 1 (0.3) | 2 (0.8) | 1 (0.5) |
| . | Patient categories . | ||
|---|---|---|---|
| Non-chelated n (%) . | Chelated . | ||
| All n (%) . | ≥6 months n (%) . | ||
| AML transformation | 30 (8.9) | 12 (4.6) | 10 (5.2) |
| Mean±SD time to transformation (mos) | 27.3±20.3 | 40.6±25.3 | 40.8±27.0 |
| Cardiac events | 155 (46.0) | 113 (43.0) | 76 (39.8) |
| Deaths | |||
| Number (%) | 171 (50.7) | 107 (40.7) | 70 (36.6) |
| Median (25th, 75th percentiles) time to death (mos)* | 52.2† (24.0, 136.2) | 99.3†‡ (54.1, NA) | 104.4‡ (63.4, NA) |
| Causes of Death | |||
| MDS/AML | 75 (22.3) | 47 (17.9) | 32 (16.8) |
| Cardiac | 28 (8.3) | 15 (5.7) | 10 (5.2) |
| Infection | 22 (6.5) | 8 (3.0) | 8 (4.2) |
| Unknown | 16 (4.7) | 10 (3.8) | 6 (3.1) |
| Other | 10 (3.0) | 9 (3.4) | 4 (2.1) |
| Malignancy | 9 (2.7) | 3 (1.1) | 0 |
| Respiratory | 7 (2.1) | 7 (2.7) | 4 (2.1) |
| Multiorgan failure | 2 (0.6) | 2 (0.8) | 2 (1.0) |
| CVA | 1 (0.3) | 4 (1.5) | 3 (1.6) |
| GvHD/transplant | 1 (0.3) | 2 (0.8) | 1 (0.5) |
NA, not attained; CVA, cerebrovascular accident; GvHD, graft versus host disease.
Time to death from diagnosis.
P<0.0001, non-chelated vs chelated
P<0.0001, non-chelated vs chelated≥6 months.
At baseline, non-chelated patients had a higher incidence of cardiac disorders than chelated patients (51.3% vs 35%). While on the registry, non-chelated patients had a higher incidence of comorbidities than did chelated patients, predominantly vascular, cardiac and endocrine. Lifetime use of MDS therapies (pre- and on-registry) was lower among non-chelated versus chelated patients (88.4% vs 94.3%).
At the 24-month analysis, use of chelation was associated with lower AML transformation, fewer cardiac events, and better OS. The two patients groups had similar age, gender, and risk status breakdown (IPSS); however the non-chelated group had a higher prevalence of cardiac comorbidities. Ongoing follow-up for the 5-year duration of this registry will provide further data on differences in outcomes between chelated and non-chelated patients.
Lyons:Amgen: Consultancy, Honoraria, Research Funding; Celgene: Consultancy, Honoraria, Research Funding; Incyte: Research Funding; Telik: Research Funding; Alexion: Consultancy, Honoraria; Novartis: Research Funding. Sharma:Novartis: Employment. Paley:Novartis: Employment. Esposito:Novartis: Employment.
Author notes
Asterisk with author names denotes non-ASH members.
