Genomic subtyping and therapeutic targeting of acute erythroleukemia.

Ilaria Iacobucci ,Hamish S Scott ,Edgar Sioson ,Andrew H Wei ,Ji Wen ,Cheng Cheng ,Franco Locatelli ,Christopher N Hahn ,R Coleman Lindsley ,Sarah M Morris ,John K Choi ,Chunxu Qu ,Guangchun Song ,Laura J Janke ,Elliot Stieglitz ,Torsten Haferlach ,Lei Shi ,Deqing Pei ,Giuseppe Basso ,Manja Meggendorfer ,Stanley Pounds ,Katherine E Masih ,Benjamin L Ebert ,Allen Eng Juh Yeoh ,Marcus B Valentine ,Xin Zhou ,Nobutaka Kiyokawa ,Eric J Enemark ,Benjamin T Kile ,Mignon L Loh ,Michael Rusch ,Ian D Lewis ,Rhonda E Ries ,Soheil Meshinchi ,Debbie Payne-Turner ,Catherine Carmichael ,Anna L Brown ,L Bik To ,Shirley Kow Yin Kham ,Stephen P Hunger ,Xiaotu Ma ,Yongjin Li ,Virginia Valentine ,Richard J D’andrea ,Paula Marlton ,Thomas Alexander ,Daisuke Tomizawa ,Charles G Mullighan

doi:10.1038/s41588-019-0375-1

Abstract

Acute erythroid leukemia (AEL) is a high-risk leukemia of poorly understood genetic basis, with controversy regarding diagnosis in the spectrum of myelodysplasia and myeloid leukemia. We compared genomic features of 159 childhood and adult AEL cases with non-AEL myeloid disorders and defined five age-related subgroups with distinct transcriptional profiles: adult, TP53 mutated; NPM1 mutated; KMT2A mutated/rearranged; adult, DDX41 mutated; and pediatric, NUP98 rearranged. Genomic features influenced outcome, with NPM1 mutations and HOXB9 overexpression being associated with a favorable prognosis and TP53, FLT3 or RB1 alterations associated with poor survival. Targetable signaling mutations were present in 45% of cases and included recurrent mutations of ALK and NTRK1, the latter of which drives erythroid leukemogenesis sensitive to TRK inhibition. This genomic landscape of AEL provides the framework for accurate diagnosis and risk stratification of this disease, and the rationale for testing targeted therapies in this high-risk leukemia.

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