Genetic factors rather than blast reduction determine outcomes of allogeneic HCT in BCR-ABL–negative MPN in blast phase

Gupta, Vikas; Kennedy, James A.; Capo‐Chichi, José‐Mario; Kim, Soyoung; Hu, Zhen-Huan; Alyea, Edwin P.; Popat, Uday; Sobecks, Ronald; Scott, Bart L.; Gerds, Aaron T.; Salit, Rachel B.; Deeg, H. Joachim; Nakamura, R.; Saber, Wael

doi:10.1182/bloodadvances.2020002727

Cited by 31 publications

(31 citation statements)

References 38 publications

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“…Conflicting results have been published regarding the impact of molecular abnormalities on transplantation outcomes (Table 3). In some European series, CALR-mutated patients had better survival than those with other genotypes [13,64,89], and ASXL1-mutated patients had higher relapse incidence [64,89], but these findings have not been confirmed in other studies [90][91][92] In a series of 95 patients with post-MPN AML, detection of TP53 gene mutations by NGS at the time of allo-HCT was associated with a higher risk of relapse and worse survival, suggesting that the adverse impact of these mutations could not be overcome by transplantation [93].…”

Section: Impact Of Molecular Profiling On Transplantationmentioning

confidence: 82%

Impact of molecular profiling on the management of patients with myelofibrosis

Pastor‐Galán¹,

Martín²,

Ferrer³

et al. 2022

Cancer Treatment Reviews

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Section: Impact Of Molecular Profiling On Transplantationmentioning

confidence: 82%

Impact of molecular profiling on the management of patients with myelofibrosis

Pastor‐Galán¹,

Martín²,

Ferrer³

et al. 2022

Cancer Treatment Reviews

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“…That prompts one to rethink the timing of HSCT in this clinical context. A recent report by CIBMTR highlighted how the disease genotype can overcome the prognostic impact of disease status at transplant, in particular, a TP53 -mutated status was correlated with dismal outcome regardless of the achievement of a response before HSCT [ 36 ]. Indeed, the immunologic effect by HSCT appears to be largely ineffective in this subgroup, possibly, also due to an immunosuppressive phenotype conferred by the TP53 mutant [ 37 ].…”

Section: Treatmentmentioning

confidence: 99%

Acute Myeloid Leukemia Evolving from Myeloproliferative Neoplasms: Many Sides of a Challenging Disease

Mannelli¹

2021

JCM

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The evolution to blast phase is a frequently unpredictable and almost invariably fatal event in the course of myeloproliferative neoplasms. The molecular mechanisms underlying blast transformation have not been elucidated and the specific genetic and epigenetic events governing leukemogenesis remain unclear. The result of the long-lasting dynamics, passing through progressive genetic steps, is the emergence of one or more clones often characterized by complex genetics, either at conventional karyotyping or at modern high-throughput sequencing analyses, with all clinical and prognostic correlates. The current therapeutic approaches are largely inadequate and incapable of modifying the inherent unfavorable outcome. In this perspective, the application of targeted strategies should aim to prevent the occurrence of leukemic evolution. At transformation, the crucial target of treatment should be the allocation to allogeneic transplant for eligible patients. With this in mind, novel combination treatments may provide useful bridging strategies, beyond potentially improving outcomes for patients who are not candidates for intensive approaches.

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“…There is no one-size-fits-all approach in patients with MF; how ever, we strongly rec om mend against waiting for dis ease to prog ress to AP/BP as out comes after the HCT are poor and many patients never make it to the trans plant stage. [11][12][13] Our goal in the begin ning is to under stand the nat u ral history of the dis ease based on best avail able infor ma tion on clin i cal and genetic risk fac tors. This infor ma tion helps in understand ing the expected sur vival and the like li hood of response and the dura bil ity of nontransplant ther apy.…”

Section: Optimal Tim Ing Of Hct In Mf?mentioning

confidence: 99%

Novel therapies vs hematopoietic cell transplantation in myelofibrosis: who, when, how?

England

Gupta

2021

Hematology

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Myelofibrosis is one of the classical Philadelphia chromosome–negative myeloproliferative neoplasms characterized by progressive marrow failure and chronic inflammation. Discovery of the JAK2 mutation paved the way for development of small molecular inhibitors and further facilitated the research in understanding of molecular biology of the disease. Development of novel medications and synergistic combinations with standard JAK inhibitor (JAKi) therapy may have the potential to improve depth and duration of disease control and symptomatic benefit, whereas advancements in allogeneic hematopoietic stem cell transplantation (HCT) have improved tolerability and donor availability, allowing for more patients to pursue this potentially curative therapy. The increase in options for medical therapy and changing risk profile of HCT is leading to increased complexity in counseling patients on choice of management strategy. In this case-based review, we summarize our approach to symptom-directed medical therapy, including the use of novel drugs and combination therapies currently under study in advanced clinical trials. We outline our recommendations for optimal timing of HCT, including risk-adapted selection for early HCT as opposed to delayed HCT after upfront JAKi therapy, as well as the use of pretransplant JAKi and alternative donor sources.

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Genetic factors rather than blast reduction determine outcomes of allogeneic HCT in BCR-ABL–negative MPN in blast phase

Cited by 31 publications

References 38 publications

Impact of molecular profiling on the management of patients with myelofibrosis

Impact of molecular profiling on the management of patients with myelofibrosis

Acute Myeloid Leukemia Evolving from Myeloproliferative Neoplasms: Many Sides of a Challenging Disease

Novel therapies vs hematopoietic cell transplantation in myelofibrosis: who, when, how?

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