The genetic basis and cell of origin of mixed phenotype acute leukaemia

Alexander, TB; Gu, Z; Iacobucci, I; Dickerson, K; Choi, JK; Xu, B; Payne-Turner, D; Yoshihara, H; Loh, ML; Horan, J; Buldini, B; Basso, G; Elitzur, S; de, Haas, V; Zwaan, CM; Yeoh, A; Reinhardt, D; Tomizawa, D; Kiyokawa, N; Lammens, T; De, Moerloose, B; Catchpoole, D; Hori, H; Moorman, A; Moore, AS; Hrusak, O; Meshinchi, S; Orgel, E; Devidas, M; Borowitz, M; Wood, B; Heerema, NA; Carrol, A; Yang, Y-L; Smith, MA; Davidsen, TM; Hermida, LC; Gesuwan, P; Marra, MA; Ma, Y; Mungall, AJ; Moore, RA; Jones, SJM; Valentine, M; Janke, LJ; Rubnitz, JE; Pui, C-H; Ding, L; Liu, Y; Zhang, J; Nichols, KE; Downing, JR; Cao, X; Shi, L; Pounds, S; Newman, S; Pei, D; Guidry, Auvil, JM; Gerhard, DS; Hunger, SP; Inaba, H; Mullighan, CG

doi:10.1038/s41586-018-0436-0

The genetic basis and cell of origin of mixed phenotype acute leukaemia

Lookup NU author(s): Professor Anthony Moorman ORCiD

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Abstract

Mixed phenotype acute leukaemia (MPAL) is a high-risk subtype of leukaemia with myeloid and lymphoid features, limited genetic characterization, and a lack of consensus regarding appropriate therapy. Here we show that the two principal subtypes of MPAL, T/myeloid (T/M) and B/myeloid (B/M), are genetically distinct. Rearrangement of ZNF384 is common in B/M MPAL, and biallelic WT1 alterations are common in T/M MPAL, which shares genomic features with early T-cell precursor acute lymphoblastic leukaemia. We show that the intratumoral immunophenotypic heterogeneity characteristic of MPAL is independent of somatic genetic variation, that founding lesions arise in primitive haematopoietic progenitors, and that individual phenotypic subpopulations can reconstitute the immunophenotypic diversity in vivo. These findings indicate that the cell of origin and founding lesions, rather than an accumulation of distinct genomic alterations, prime tumour cells for lineage promiscuity. Moreover, these findings position MPAL in the spectrum of immature leukaemias and provide a genetically informed framework for future clinical trials of potential treatments for MPAL.

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Author(s): Alexander TB, Gu Z, Iacobucci I, Dickerson K, Choi JK, Xu B, Payne-Turner D, Yoshihara H, Loh ML, Horan J, Buldini B, Basso G, Elitzur S, de Haas V, Zwaan CM, Yeoh A, Reinhardt D, Tomizawa D, Kiyokawa N, Lammens T, De Moerloose B, Catchpoole D, Hori H, Moorman A, Moore AS, Hrusak O, Meshinchi S, Orgel E, Devidas M, Borowitz M, Wood B, Heerema NA, Carrol A, Yang Y-L, Smith MA, Davidsen TM, Hermida LC, Gesuwan P, Marra MA, Ma Y, Mungall AJ, Moore RA, Jones SJM, Valentine M, Janke LJ, Rubnitz JE, Pui C-H, Ding L, Liu Y, Zhang J, Nichols KE, Downing JR, Cao X, Shi L, Pounds S, Newman S, Pei D, Guidry Auvil JM, Gerhard DS, Hunger SP, Inaba H, Mullighan CG

Publication type: Article

Publication status: Published

Journal: Nature

Year: 2018

Volume: 562

Issue: 7727

Pages: 373-379

Online publication date: 12/09/2018

Acceptance date: 03/07/2018

ISSN (print): 0028-0836

ISSN (electronic): 1476-4687

Publisher: Nature Publishing Group

URL: https://doi.org/10.1038/s41586-018-0436-0

DOI: 10.1038/s41586-018-0436-0

PubMed id: 30209392

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The genetic basis and cell of origin of mixed phenotype acute leukaemia

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