| Literature DB >> 25885405 |
Serena Rupoli1, Gaia Goteri2, Paola Picardi3, Giorgia Micucci4, Lucia Canafoglia5, Anna Rita Scortechini6, Irene Federici7, Federica Giantomassi8, Lidia Da Lio9, Antonio Zizzi10, Elisa Honorati11, Pietro Leoni12.
Abstract
BACKGROUND: Vascular events represent the most frequent complications of thrombocytemias. We aimed to evaluate their risk in the WHO histologic categories of Essential Thrombocytemia (ET) and early Primary Myelofibrosis (PMF).Entities:
Mesh:
Year: 2015 PMID: 25885405 PMCID: PMC4407780 DOI: 10.1186/s13000-015-0269-1
Source DB: PubMed Journal: Diagn Pathol ISSN: 1746-1596 Impact factor: 2.644
Figure 1H&E of bone marrow in ET (A) and in grade 0 Prefibrotic PMF (B). Original magnification x20. In cases considered ET, the cellularity appeared not increased, the megakaryocytes were mainly giant with stag-horn like nuclei and showed low tendency to aggregate. In cases considered PMF, the cellularity was increased mainly for expansion of granulopoiesis; the megakaryocytes were aggregated and showed frequently hypolobulated nuclei.
Clinico-pathological parameters for patients with ET and early/prefibrotic PMF
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| M/F | 27/34 | 26/46 | n.s. |
| Median age (years) | 58.0 (23–84) | 55.5 (20–87) | n.s. |
| Mean WBC (109/l) | 7.5 | 8.4 |
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| Mean Hb (g/dl) | 14.1 | 14.3 | n.s. |
| Mean PLT (109/l) | 751 | 798 | n.s. |
| Increased LDH (%) | 17/45 (37.7%) | 18/50 (36.0%) | n.s. |
| Splenomegaly (%) | 12 (19%) | 18 (25%) | n.s. |
| Mean semiquantitative score for granulopoiesis | 0.15 | 1.02 |
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| JAK2V617F-positive (%) | 11 (33%) | 23 (54%) | n.s. |
| History of thrombosis (%) | 5 (8%) | 16 (22%) |
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| Thrombosis at diagnosis (%) | 1 (1.6%) | 11 (15.2%) |
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| Thrombotic events during follow up (%) | 7 (11.4%) | 11 (15.2%) | n.s. |
| Progression to overt MF (%) | 1 (1.6%) | 3 (4.1%) | n.s. |
| Dead/alive | 2/59 | 8/64 | n.s. |
| Conventional Risk (Low/High) | 35/26 | 30/42 | n.s. |
| Cytoreductive therapy (%) | 51 (83%) | 64 (88%) | n.s. |
Main thrombotic events at diagnosis and during follow up in ET and PMF
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| ET | 1 | ||||||
| PMF | 2 | 1 | 1 | 3 | 3 | 1 | |
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| ET | 2 | 4 | 1 | ||||
| PMF | 2 | 2 | 2 | 1 | 1 | 3 | |
Note: AMI = acute myocardial infarction; TIA = transient ischemic attack; PAT = peripheral arterial thrombosis; DVT = deep-vein thrombosis; PE = pulmonary embolism.
Clinical characteristics in the two subgroups of prefibrotic and fibrotic PMF
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| Sex | M:F = 11/15 | M:F = 15/31 | n.s. |
| Median age at diagnosis (years) | 43 (20–87) | 61 (27–83) |
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| WBC at diagnosis (109/l) | 9100 | 8745 | n.s. |
| Hb at diagnosis (g/dl) | 14.6 | 14.3 | n.s. |
| PLT at diagnosis (109/l) | 825000 | 797500 | n.s. |
| Increased LDH | 6/19 (31.6%) | 19/31 (61.3%) | n.s. |
| Splenomegaly (%) | 6 (23%) | 12 (26%) | n.s. |
| JAK2V617-positive (%) | 9 (50%) | 14 (58%) | n.s. |
| History of thrombosis (%) | 6 (23%) | 10 (22%) | n.s. |
| Thrombosis at diagnosis (%) | 4 (15%) | 7 (15%) | n.s. |
| Thrombotic events during follow-up (%) | 6 (23%) | 5 (10%) | n.s. |
| Progression to overt MF (%) | 0 (0%) | 3 (6.5%) | n.s. |
| Dead/Alive | 2/24 | 6/40 | n.s. |
| Conventional Risk (Low/High) | 13/13 | 17/29 | n.s. |
| Cytoreductive therapy (%) | 24 (92%) | 40 (86%) | n.s. |
Figure 2Overall survival (OS) of patients with ET, prefibrotic PMF and fibrotic PMF. Significant differences were found only between ET and fibrotic PMF patients (p = 0.027).
Figure 3Risk of thrombosis during follow-up: the 15-year risk of thrombosis was 48% in prefibrotic PMF, 16% in fibrotic PMF (grade 1, 2) and 17% in ET. Differences were significant between prefibrotic PMF vs fibrotic PMF (p = 0.049) and between prefibrotic PMF vs ET (p = 0.032).
Figure 4Patients older than 60 or with prefibrotic PMF are high-risk patients, whereas those younger and with ET and fibrotic PMF should be considered at low risk. The resulting risk categories (high or low-risk) better predicted future vascular events than conventional risk factors (34% and 7% respectively for high and low risk at 15 years; p = 0.005).