The Classification of Myeloproliferative Neoplasms: Rationale, Historical Background and Future Perspectives with Focus on Unclassifiable Cases

Pizzi, Marco; Croci, Giorgio Alberto; Ruggeri, Marco; Tabano, Silvia; Tos, Angelo Paolo Dei; Sabattini, Elena; Gianelli, Umberto

doi:10.3390/cancers13225666

Cited by 18 publications

(14 citation statements)

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“…However, in most instances, clinical and laboratory findings coupled with the molecular search for driver mutations and/or molecular or cytogenetic markers of clonality of hematopoiesis and BM biopsy examination prompt the diagnosis. 19 From the histopathologic perspective, mimickers of MPN include immune thrombocytopenia (ITP) treated with agonists of thrombopoietin receptor that impart a striking MPN-like histologic appearance to BM biopsy, and the rare instances of autoimmune myelofibrosis, a condition in which the coexistence of lymphoid infiltrate may further trigger a diagnosis of lymphoproliferative disorder. 20,21 Spleen histology is less frequently experienced in clinical practice.…”

Section: Discussionmentioning

confidence: 99%

Splenomegaly: Dare to think rare

et al. 2022

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Section: Discussionmentioning

confidence: 99%

Splenomegaly: Dare to think rare

et al. 2022

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“…Diagnostic trephine biopsies showed age‐adjusted hypercellularity in the majority of cases (67%), increased (100%) and clustered (83%) MKC and a median (range) WHO fibrosis score of 1 (0–3). As highlighted by Pizzi et al, 6 this suggests that most new MPN‐U, diagnosed according to WHO 2016 criteria, fall within the early, non‐fibrotic and non‐advanced stage. Kim et al 12 characterised 199 MPN patients, eight of whom had MPN‐U, where CALR was the most frequent mutation, although it must be noted that this conclusion is limited by the small numbers of patients.…”

Section: Distinguishing Mpn‐u From Mds/mpn‐u: Focus Pointmentioning

confidence: 92%

“…Perhaps representing an arbitrarily defined early/prodromal phase, 21 cases could be re-classified as ET or PV whereas within the advanced phase, the vast majority could be reclassified as overt MF (25) and PV (6). The authors reported that this was most likely reflective of refined definition of prefibrotic MF and overtly fibrotic MF and updated Hb/haematocrit values within the PV category.…”

Section: Morphological and Molecular Characterisation Of Mpn-u: A Mov...mentioning

confidence: 99%

“…From a practical stance, cases of MPN-U frequently tend to fall within specific phenotypic categories. 5,6 Firstly, there are those which represent a prodromal, pre-proliferative phase MPN and therefore may share some of the classical MPN clinical features, but do not yet meet the required diagnostic criteria for accurate subclassification. For example, it may be a prepolycythaemic presentation of polycythaemia vera (PV), or a masked phenotype, e.g.…”

Section: Agnostic Cr Iter I a Of M Pn-u: A N I N Tegr Ate D A Pproach...mentioning

confidence: 99%

“…Secondly, there are those which represent a very late presentation of a classical MPN, where advanced fibrosis or disrupted BM architecture obscures the underlying diagnosis, or those where co-existing neoplastic, or indeed inf lammatory, disorders obscure the diagnostic features. 6 Finally, there are those cases which meet the diagnostic criteria for more than two MPNs at presentation, or there is clinicopathological mismatch, and hence cannot be easily classified as one of the classical MPNs. There are a number of important differential diagnoses to consider when making a diagnosis of MPN-U, and a number of diagnostic pitfalls that must be avoided.…”

Section: Agnostic Cr Iter I a Of M Pn-u: A N I N Tegr Ate D A Pproach...mentioning

confidence: 99%

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How I manage myeloproliferative neoplasm‐unclassifiable: Practical approaches for 2022 and beyond

et al. 2022

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Myeloproliferative neoplasm (MPN)‐unclassifiable (MPN‐U) or not otherwise specified represents a rare, poorly defined and heterogeneous group of MPNs. Disease incidence is difficult to define but likely represents close to 5% of all MPNs when strict World Health Organisation (WHO) criteria are applied. Dynamic review over time is required to assess if the disease can be re‐classified into another MPN entity. A diagnosis of MPN‐U leads to many challenges for both the patient and physician alike including lack of agreed monitoring and therapeutic guidelines, validated prognostic markers and licenced therapies coupled with exclusion from clinical trials. MPN‐U has an inherent risk of an aggressive clinical course and transformation in some but who, and when to treat in the chronic phase, including identifying who may require more aggressive therapy at an earlier stage, remains elusive. Moreover, despite the significant thrombotic risk, there is no agreement on systematic primary thromboprophylaxis. We hereby provide a contemporary overview of MPN‐U in addition to four illustrative cases providing our collective suggested approaches to clinical challenges.

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The personal impact of living with a myeloproliferative neoplasm

Eppingbroek,

Lechner,

Bakker

et al. 2024

Psycho-Oncology

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ObjectiveThe aim of this study is to gain insight into the physical, psychological and social impact of having a myeloproliferative neoplasm (MPN), a rare type of cancer with an often chronic course.MethodsAn online survey was conducted among 455 Dutch MPN patients (62.7% female, age M 63) to explore the impact of the disease by measuring the MPN symptom burden (MPN‐SAF TSS) and quality of life (QoL) (EORTC QLQ‐C30) and its subscales within a hierarchical QoL model. We examined differences in MPN symptom burden and QoL in relation to sociodemographic and disease‐related factors. Hierarchical regression analysis was used to explain variances in QoL.ResultsMost patients (97%) experienced MPN‐related health complaints, with a significantly higher MPN symptom burden in women (M 31.50) compared to men (M 24.10). Regarding to fatigue and cognitive functioning MPN patients suffered more compared to a reference group of other cancers. MPN subtype or type of treatment did not show significant differences in MPN symptom burden or QoL. However, experiencing side effects, complications or comorbidities significantly negatively affected MPN symptom burden and QoL. 48.8% of patients reported that MPN affected their ability to work. The explained variance in overall QoL was 58%, most importantly by disease progression, comorbidities, MPN symptom burden and role, emotional and social functioning.ConclusionThis study revealed that having an MPN has a negative impact on several domains of QoL. Symptom assessment and support should be included in the healthcare management of MPN patients.

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The Classification of Myeloproliferative Neoplasms: Rationale, Historical Background and Future Perspectives with Focus on Unclassifiable Cases

Cited by 18 publications

References 70 publications

Splenomegaly: Dare to think rare

Splenomegaly: Dare to think rare

How I manage myeloproliferative neoplasm‐unclassifiable: Practical approaches for 2022 and beyond

The personal impact of living with a myeloproliferative neoplasm

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