Your search keyword '"Dal Cin P"' showing total 10 results

1. Clinical response to larotrectinib in adult Philadelphia chromosome–like ALL with cryptic ETV6-NTRK3 rearrangement

Author

Valentina Nardi, Nora Ku, Matthew J. Frigault, Adrian M. Dubuc, Harrison Kwei Tsai, Philip C. Amrein, Gabriela S. Hobbs, Andrew M. Brunner, Rupa Narayan, Meghan E. Burke, Julia Foster, Paola Dal Cin, Marcela V. Maus, Amir T. Fathi, and Hanno Hock

Subjects

Specialties of internal medicine, RC581-951

Abstract

Abstract: Philadelphia chromosome (Ph)–like acute lymphoblastic leukemia (ALL) is a subtype of Ph-negative ALL that molecularly resembles Ph-positive ALL. It shares the adverse prognosis of Ph-positive ALL, but lacks the BCR-ABL1 fusion oncogene. Instead, Ph-like ALL is associated with alternative mutations in signaling pathways. We describe a case of Ph-like ALL that harbored 2 genomic alterations, which activated signaling, an NRASGly12Asp mutation, and an ETV6-NTRK3 rearrangement. Initially, the NRAS mutation was detected at high frequency, whereas the gene fusion was only detectable with a targeted next-generation sequencing-based fusion assay, but not by fluorescence in situ hybridization analysis. The disease failed to respond to multiagent chemotherapy but investigational CD19-directed chimeric antigen receptor T-cell therapy resulted in a complete remission. However, the leukemia relapsed after 6 weeks. Intriguingly, the NRAS mutation was extinguished during the chimeric antigen receptor T-cell therapy and did not contribute to the relapse, which was instead associated with a rise in ETV6-NTRK3. The relapsed leukemia progressed with further chemo- and immunotherapy but was controlled for 6 weeks with substantial leukemic cytoreduction using the TRK inhibitor larotrectinib. Unfortunately, recovery of normal hematopoiesis was only marginal and the patient eventually succumbed to infections. These results demonstrate that larotrectinib has clinical activity in ETV6-NTRK3-associated Ph-like ALL.

Published

2020

2. Maternal iAMP21 acute lymphoblastic leukemia detected on prenatal cell-free DNA genetic screening

Author

Marlise R. Luskin, Marie N. Discenza, Sarah Rae Easter, Paola Dal Cin, Renius Owen, Bernard Ilagan, Meredith Masiello, and Andrew A. Lane

Subjects

Specialties of internal medicine, RC581-951

Published

2017

3. TP53 mutation defines a unique subgroup within complex karyotype de novo and therapy-related MDS/AML

Author

Weinberg, Olga K., Siddon, Alexa, Madanat, Yazan F., Gagan, Jeffrey, Arber, Daniel A., Dal Cin, Paola, Narayanan, Damodaran, Ouseph, Madhu M., Kurzer, Jason H., and Hasserjian, Robert P.

Abstract

A subset of myelodysplastic syndromes (MDS) and acute myeloid leukemia (AML) show complex karyotype (CK), and these cases include a relatively high proportion of cases of therapy-related myeloid neoplasms and TP53 mutations. We aimed to evaluate the clinicopathologic features of outcome of 299 AML and MDS patients with CK collected from multiple academic institutions. Mutations were present in 287 patients (96%), and the most common mutation detected was in TP53 gene (247, 83%). A higher frequency of TP53 mutations was present in therapy-related cases (P = .008), with a trend for worse overall survival (OS) in therapy-related patients as compared with de novo disease (P = .08) and within the therapy-related group; the presence of TP53 mutation strongly predicted for worse outcome (P = .0017). However, there was no difference in survival between CK patients based on categorization of AML vs MDS (P = .96) or presence of absence of circulating blasts ≥1% (P = .52). TP53-mutated patients presented with older age (P = .06) and lower hemoglobin levels (P = .004) and marrow blast counts (P = .02) compared with those with CK lacking TP53 mutation. Multivariable analysis identified presence of multihit TP53 mutation as strongest predictor of worse outcome, whereas neither a diagnosis of AML vs MDS nor therapy-relatedness independently influenced OS. Our findings suggest that among patients with MDS and AML, the presence of TP53 mutation (in particular multihit TP53 mutation) in the context of CK identifies a homogeneously aggressive disease, irrespective of the blast count at presentation or therapy-relatedness. The current classification of these cases into different disease categories artificially separates a single biologic disease entity.

Published

2022

4. TP53mutation defines a unique subgroup within complex karyotype de novo and therapy-related MDS/AML

Author

Weinberg, Olga K., Siddon, Alexa, Madanat, Yazan F., Gagan, Jeffrey, Arber, Daniel A., Dal Cin, Paola, Narayanan, Damodaran, Ouseph, Madhu M., Kurzer, Jason H., and Hasserjian, Robert P.

Abstract

A subset of myelodysplastic syndromes (MDS) and acute myeloid leukemia (AML) show complex karyotype (CK), and these cases include a relatively high proportion of cases of therapy-related myeloid neoplasms and TP53mutations. We aimed to evaluate the clinicopathologic features of outcome of 299 AML and MDS patients with CK collected from multiple academic institutions. Mutations were present in 287 patients (96%), and the most common mutation detected was in TP53gene (247, 83%). A higher frequency of TP53mutations was present in therapy-related cases (P= .008), with a trend for worse overall survival (OS) in therapy-related patients as compared with de novo disease (P= .08) and within the therapy-related group; the presence of TP53mutation strongly predicted for worse outcome (P= .0017). However, there was no difference in survival between CK patients based on categorization of AML vs MDS (P= .96) or presence of absence of circulating blasts ≥1% (P= .52). TP53-mutated patients presented with older age (P= .06) and lower hemoglobin levels (P= .004) and marrow blast counts (P= .02) compared with those with CK lacking TP53mutation. Multivariable analysis identified presence of multihit TP53mutation as strongest predictor of worse outcome, whereas neither a diagnosis of AML vs MDS nor therapy-relatedness independently influenced OS. Our findings suggest that among patients with MDS and AML, the presence of TP53mutation (in particular multihit TP53mutation) in the context of CK identifies a homogeneously aggressive disease, irrespective of the blast count at presentation or therapy-relatedness. The current classification of these cases into different disease categories artificially separates a single biologic disease entity.

Published

2022

5. t(4;12)(q12;p13) ETV6-rearranged AML without eosinophilia does not involve PDGFRA: relevance for imatinib insensitivity

Author

Mueller, Sarah B., Dal Cin, Paola, Le, Long P., Dias-Santagata, Dora, Lennerz, Jochen K., Iafrate, A. John, Marble, Hetal Desai, Brunner, Andrew M., Weinstock, Matthew J., Luskin, Marlise R., De Angelo, Daniel J., Stone, Richard M., and Nardi, Valentina

Abstract

Acute myeloid leukemia (AML) with t(4;12)(q12;p13) translocation is rare and often associated with an aggressive clinical course and poor prognosis. Previous reports based on fluorescence in situ hybridization (FISH) analysis have suggested that ETV6::PDGFRAfusions are present in these patients, despite the absence of eosinophilia, which is typically found in other hematopoietic malignancies with PDGFRA-containing fusions. We first detected an ETV6-SCFD2fusion by targeted RNA sequencing in a patient with t(4;12)(q12;p13) who had been diagnosed with an ETV6-PDGFRAfusion by FISH analysis but failed to respond to imatinib. We then retrospectively identified 4 additional patients with AML and t(4;12)(q12;p13) with apparent ETV6-PDGFRAfusions using chromosome and FISH analysis and applied targeted RNA sequencing to archival material. We again detected rearrangements between ETV6and non-PDGFRA4q12 genes, including SCFD2, CHIC2, and GSX2. None of the 3 patients who received imatinib based on the incorrect assumption of an ETV6-PDGFRAfusion responded. Our findings highlight the importance of using a sequencing-based assay to confirm the presence of targetable gene fusions, particularly in genomic regions, such as 4q12, with many clinically relevant genes that are too close to resolve by chromosome or FISH analysis. Finally, combining our data and review of the literature, we show that sequence-confirmed ETV6-PDGFRAfusions are typically found in eosinophilic disorders (3/3 cases), and patients with t(4;12)(q12;p13) without eosinophilia are found to have other 4q12 partners on sequencing (17/17 cases).

Published

2022

6. Targeted FGFR inhibition results in a durable remission in an FGFR1-driven myeloid neoplasm with eosinophilia

Author

Kasbekar, Monica, Nardi, Valentina, Dal Cin, Paola, Brunner, Andrew M., Burke, Meghan, Chen, Yi-Bin, Connolly, Christine, Fathi, Amir T., Foster, Julia, Macrae, Molly, McAfee, Steven L., McGregor, Kristin, Narayan, Rupa, Ramos, Aura Y., Som, Tina T., Vartanian, Meghan, Friedman, Robb S., Benhadji, Karim A., and Hobbs, Gabriela S.

Published

2020

7. A cryptic imatinib-sensitive G3BP1-PDGFRB rearrangement in a myeloid neoplasm with eosinophilia

Author

Jan, Max, Grinshpun, Daniel E., Villalba, Julian A., Dal Cin, Paola, Sykes, David B., Iafrate, A. John, Ebert, Benjamin L., Hobbs, Gabriela S., and Nardi, Valentina

Published

2020

8. A cryptic imatinib-sensitive G3BP1-PDGFRBrearrangement in a myeloid neoplasm with eosinophilia

Author

Jan, Max, Grinshpun, Daniel E., Villalba, Julian A., Dal Cin, Paola, Sykes, David B., Iafrate, A. John, Ebert, Benjamin L., Hobbs, Gabriela S., and Nardi, Valentina

Abstract

•Targeted RNA sequencing detected a cryptic G3BP1-PDGFRBrearrangement in a myeloid neoplasm with eosinophilia and normal FISH studies.•Consistent with the patient's response to imatinib, we demonstrate this rearrangement is oncogenic and sensitive to TKI in cell culture.

Published

2020

9. Clinical response to larotrectinib in adult Philadelphia chromosome–like ALL with cryptic ETV6-NTRK3 rearrangement

Author

Nardi, Valentina, Ku, Nora, Frigault, Matthew J., Dubuc, Adrian M., Tsai, Harrison Kwei, Amrein, Philip C., Hobbs, Gabriela S., Brunner, Andrew M., Narayan, Rupa, Burke, Meghan E., Foster, Julia, Dal Cin, Paola, Maus, Marcela V., Fathi, Amir T., and Hock, Hanno

Abstract

Philadelphia chromosome (Ph)–like acute lymphoblastic leukemia (ALL) is a subtype of Ph-negative ALL that molecularly resembles Ph-positive ALL. It shares the adverse prognosis of Ph-positive ALL, but lacks the BCR-ABL1 fusion oncogene. Instead, Ph-like ALL is associated with alternative mutations in signaling pathways. We describe a case of Ph-like ALL that harbored 2 genomic alterations, which activated signaling, an NRASGly12Asp mutation, and an ETV6-NTRK3 rearrangement. Initially, the NRAS mutation was detected at high frequency, whereas the gene fusion was only detectable with a targeted next-generation sequencing-based fusion assay, but not by fluorescence in situ hybridization analysis. The disease failed to respond to multiagent chemotherapy but investigational CD19-directed chimeric antigen receptor T-cell therapy resulted in a complete remission. However, the leukemia relapsed after 6 weeks. Intriguingly, the NRAS mutation was extinguished during the chimeric antigen receptor T-cell therapy and did not contribute to the relapse, which was instead associated with a rise in ETV6-NTRK3. The relapsed leukemia progressed with further chemo- and immunotherapy but was controlled for 6 weeks with substantial leukemic cytoreduction using the TRK inhibitor larotrectinib. Unfortunately, recovery of normal hematopoiesis was only marginal and the patient eventually succumbed to infections. These results demonstrate that larotrectinib has clinical activity in ETV6-NTRK3-associated Ph-like ALL.

Published

2020

10. Maternal iAMP21 acute lymphoblastic leukemia detected on prenatal cell-free DNA genetic screening

Author

Luskin, Marlise R., Discenza, Marie N., Easter, Sarah Rae, Dal Cin, Paola, Owen, Renius, Ilagan, Bernard, Masiello, Meredith, and Lane, Andrew A.

Published

2017