Literature DB >> 30117174

Genomic and clinical characterization of B/T mixed phenotype acute leukemia reveals recurrent features and T-ALL like mutations.

Xiaoli Mi1,2, Gabriel Griffin3, Winston Lee3, Sanjay Patel3, Robert Ohgami4, Chi Young Ok5, Sa Wang5, Julia T Geyer6, Wenbin Xiao7, Mikhail Roshal7, Jacqueline S Garcia3, Lewis B Silverman8,9, Stephen E Sallan8,9, Jon C Aster3, Marian H Harris2, Olga K Weinberg2.   

Abstract

The B/T subtype of mixed phenotype acute leukemia (B/T MPAL) is defined by co-expression of antigens of both B- and T-cell lineages on leukemic blasts. Although it has been suggested that multilineage antigen expression portends poor response to chemotherapy, the clinical characteristics and driver mutations that underlie the pathogenesis of this rare subtype of acute leukemia are scarcely known. We identified nine cases of B/T MPAL from multiple institutions and correlated clinical and immunophenotypic findings with next-generation sequencing data. We report that B/T MPAL commonly presents with lymphadenopathy in adolescence and young adulthood. While the tumors have diverse cytogenetic and genomic perturbations, recurrent acquired aberrations include mutations in the putative transcriptional regulator PHF6 and the JAK-STAT and Ras signaling pathways. Alterations were also identified in genes encoding hematopoietic transcription factors, cell cycle regulators/tumor suppressors, and chromatin modifying enzymes. The genomic landscape of B/T MPAL strongly resembles that of T-ALL subgroups associated with early developmental arrest, while genetic alterations that are common in B-ALL were rarely seen. Two-thirds of the patients responded to ALL-based chemotherapy with or without stem cell transplantation. Our observations lay the groundwork for further study of the unique biology and clinical trajectory of B/T MPAL.
© 2018 Wiley Periodicals, Inc.

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Year:  2018        PMID: 30117174      PMCID: PMC8193761          DOI: 10.1002/ajh.25256

Source DB:  PubMed          Journal:  Am J Hematol        ISSN: 0361-8609            Impact factor:   10.047


  32 in total

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Journal:  Blood       Date:  2007-05-07       Impact factor: 22.113

Review 2.  The genomic landscape of acute lymphoblastic leukemia in children and young adults.

Authors:  Charles G Mullighan
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4.  Mixed phenotype acute leukemia: A study of 61 cases using World Health Organization and European Group for the Immunological Classification of Leukaemias criteria.

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Journal:  Am J Clin Pathol       Date:  2014-12       Impact factor: 2.493

Review 5.  Mixed-phenotype acute leukemia: historical overview and a new definition.

Authors:  O K Weinberg; D A Arber
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7.  Combined interphase fluorescence in situ hybridization elucidates the genetic heterogeneity of T-cell acute lymphoblastic leukemia in adults.

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  11 in total

1.  PHF6 and DNMT3A mutations are enriched in distinct subgroups of mixed phenotype acute leukemia with T-lineage differentiation.

Authors:  Wenbin Xiao; Maheetha Bharadwaj; Max Levine; Noushin Farnhoud; Friederike Pastore; Bartlomiej M Getta; Anne Hultquist; Christopher Famulare; Juan S Medina; Minal A Patel; Qi Gao; Natasha Lewis; Janine Pichardo; Jeeyeon Baik; Brian Shaffer; Sergio Giralt; Raajit Rampal; Sean Devlin; Robert Cimera; Yanming Zhang; Maria E Arcila; Elli Papaemmanuil; Ross L Levine; Mikhail Roshal
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Review 4.  The Role of PHF6 in Hematopoiesis and Hematologic Malignancies.

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Review 6.  Mixed Phenotype Acute Leukemia: Current Approaches to Diagnosis and Treatment.

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7.  B/T mixed phenotype acute leukemia with high hyperdiploidy and lineage switch to B-cell acute leukemia.

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8.  MEF2C opposes Notch in lymphoid lineage decision and drives leukemia in the thymus.

Authors:  Kirsten Canté-Barrett; Mariska T Meijer; Valentina Cordo'; Rico Hagelaar; Wentao Yang; Jiyang Yu; Willem K Smits; Marloes E Nulle; Joris P Jansen; Rob Pieters; Jun J Yang; Jody J Haigh; Steven Goossens; Jules Pp Meijerink
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Review 9.  Mixed-Phenotype Acute Leukemia: Clinical Diagnosis and Therapeutic Strategies.

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10.  A transcriptomic continuum of differentiation arrest identifies myeloid interface acute leukemias with poor prognosis.

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Journal:  Leukemia       Date:  2020-07-13       Impact factor: 11.528

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