Targetable Kinase-Activating Lesions in Ph-like Acute Lymphoblastic Leukemia

Kathryn G. Roberts; Yongjin Li; Debbie Payne-Turner; Richard C. Harvey; Yung‐Li Yang; Deqing Pei; Kelly McCastlain; Li Ding; Charles Lu; Guangchun Song; Jing Ma; Jared Becksfort; Michael Rusch; Shann-Ching Chen; John Easton; Jinjun Cheng; Kristy Boggs; Natalia Santiago-Morales; Ilaria Iacobucci; Robert S. Fulton; Ji Wen; Marcus Valentine; Cheng Cheng; Steven W. Paugh; Meenakshi Devidas; I‐Ming Chen; Shalini C. Reshmi; Amy Smith; Erin Hedlund; Pankaj Gupta; Panduka Nagahawatte; Gang Wu; Xiang Chen; Donald Yergeau; Bhavin Vadodaria; Heather L. Mulder; Naomi Winick; Eric Larsen; William L. Carroll; Nyla A. Heerema; Andrew J. Carroll; Guy H. Grayson; Sarah K. Tasian; Andrew S. Moore; Frank Keller; Melissa Frei‐Jones; James A. Whitlock; Elizabeth A. Raetz; Deborah L. White; Timothy P. Hughes; Jaime M. Guidry Auvil; Malcolm A. Smith; Guido Marcucci; Clara D. Bloomfield; Krzysztof Mrózek; Jessica Kohlschmidt; Wendy Stock; Steven M. Kornblau; Marina Konopleva; Elisabeth Paietta; Ching‐Hon Pui; Sima Jeha; Mary V. Relling; William E. Evans; Daniela S. Gerhard; Julie M. Gastier-Foster; Elaine R. Mardis; Richard K. Wilson; Mignon L. Loh; James R. Downing; Stephen P. Hunger; Cheryl L. Willman; Jinghui Zhang; Charles G. Mullighan

doi:10.1056/nejmoa1403088

Targetable Kinase-Activating Lesions in Ph-like Acute Lymphoblastic Leukemia

Kathryn G. Roberts(I.R.C.C.S. Oasi Maria SS), Yongjin Li(St. Jude Children's Research Hospital), Debbie Payne-Turner(St. Jude Children's Research Hospital), Richard C. Harvey(New Mexico Cancer Center), Yung‐Li Yang(St. Jude Children's Research Hospital), Deqing Pei(St. Jude Children's Research Hospital), Kelly McCastlain(St. Jude Children's Research Hospital), Li Ding(St. Jude Children's Research Hospital), Charles Lu(St. Jude Children's Research Hospital), Guangchun Song(St. Jude Children's Research Hospital), Jing Ma(St. Jude Children's Research Hospital), Jared Becksfort(St. Jude Children's Research Hospital), Michael Rusch(St. Jude Children's Research Hospital), Shann-Ching Chen(St. Jude Children's Research Hospital), John Easton(St. Jude Children's Research Hospital), Jinjun Cheng(St. Jude Children's Research Hospital), Kristy Boggs(St. Jude Children's Research Hospital), Natalia Santiago-Morales(St. Jude Children's Research Hospital), Ilaria Iacobucci(St. Jude Children's Research Hospital), Robert S. Fulton(St. Jude Children's Research Hospital), Ji Wen(St. Jude Children's Research Hospital), Marcus Valentine(St. Jude Children's Research Hospital), Cheng Cheng(St. Jude Children's Research Hospital), Steven W. Paugh(St. Jude Children's Research Hospital), Meenakshi Devidas(National Institutes of Health), I‐Ming Chen, Shalini C. Reshmi(Nationwide Children's Hospital), Amy Smith(Nationwide Children's Hospital), Erin Hedlund(St. Jude Children's Research Hospital), Pankaj Gupta(St. Jude Children's Research Hospital), Panduka Nagahawatte(St. Jude Children's Research Hospital), Gang Wu(St. Jude Children's Research Hospital), Xiang Chen(St. Jude Children's Research Hospital), Donald Yergeau(St. Jude Children's Research Hospital), Bhavin Vadodaria(St. Jude Children's Research Hospital), Heather L. Mulder(St. Jude Children's Research Hospital), Naomi Winick(The University of Texas Southwestern Medical Center), Eric Larsen(New England Cancer Specialists), William L. Carroll(National Institutes of Health), Nyla A. Heerema(The Ohio State University), Andrew J. Carroll(University of Alabama at Birmingham), Guy H. Grayson(Scott & White Memorial Hospital), Sarah K. Tasian(Children's Hospital of Philadelphia), Andrew S. Moore(Queensland Children’s Medical Research Institute), Frank Keller(Children's Healthcare of Atlanta), Melissa Frei‐Jones(The University of Texas Health Science Center at San Antonio), James A. Whitlock(Hospital for Sick Children), Elizabeth A. Raetz(National Cancer Institute), Deborah L. White(South Australian Health and Medical Research Institute), Timothy P. Hughes(South Australian Health and Medical Research Institute), Jaime M. Guidry Auvil(Children's Oncology Group), Malcolm A. Smith(National Institutes of Health), Guido Marcucci, Clara D. Bloomfield, Krzysztof Mrózek, Jessica Kohlschmidt(Alliance for Clinical Trials in Oncology), Wendy Stock(Comer Children's Hospital), Steven M. Kornblau(The University of Texas MD Anderson Cancer Center), Marina Konopleva(The University of Texas MD Anderson Cancer Center), Elisabeth Paietta(Albert Einstein College of Medicine), Ching‐Hon Pui(St. Jude Children's Research Hospital), Sima Jeha(St. Jude Children's Research Hospital), Mary V. Relling(Children's Oncology Group), William E. Evans(St. Jude Children's Research Hospital), Daniela S. Gerhard(Children's Oncology Group), Julie M. Gastier-Foster(Nationwide Children's Hospital), Elaine R. Mardis(Washington University Medical Center), Richard K. Wilson(St. Jude Children's Research Hospital), Mignon L. Loh(UCSF Helen Diller Family Comprehensive Cancer Center), James R. Downing(St. Jude Children's Research Hospital), Stephen P. Hunger(National Institutes of Health), Cheryl L. Willman(Children's Oncology Group), Jinghui Zhang(Children's Oncology Group), Charles G. Mullighan(National Institutes of Health)

New England Journal of Medicine

September 11, 2014

10.1056/nejmoa1403088

Cited by 1,373Open Access

Full Text

Abstract

BACKGROUND: Philadelphia chromosome-like acute lymphoblastic leukemia (Ph-like ALL) is characterized by a gene-expression profile similar to that of BCR-ABL1-positive ALL, alterations of lymphoid transcription factor genes, and a poor outcome. The frequency and spectrum of genetic alterations in Ph-like ALL and its responsiveness to tyrosine kinase inhibition are undefined, especially in adolescents and adults. METHODS: We performed genomic profiling of 1725 patients with precursor B-cell ALL and detailed genomic analysis of 154 patients with Ph-like ALL. We examined the functional effects of fusion proteins and the efficacy of tyrosine kinase inhibitors in mouse pre-B cells and xenografts of human Ph-like ALL. RESULTS: Ph-like ALL increased in frequency from 10% among children with standard-risk ALL to 27% among young adults with ALL and was associated with a poor outcome. Kinase-activating alterations were identified in 91% of patients with Ph-like ALL; rearrangements involving ABL1, ABL2, CRLF2, CSF1R, EPOR, JAK2, NTRK3, PDGFRB, PTK2B, TSLP, or TYK2 and sequence mutations involving FLT3, IL7R, or SH2B3 were most common. Expression of ABL1, ABL2, CSF1R, JAK2, and PDGFRB fusions resulted in cytokine-independent proliferation and activation of phosphorylated STAT5. Cell lines and human leukemic cells expressing ABL1, ABL2, CSF1R, and PDGFRB fusions were sensitive in vitro to dasatinib, EPOR and JAK2 rearrangements were sensitive to ruxolitinib, and the ETV6-NTRK3 fusion was sensitive to crizotinib. CONCLUSIONS: Ph-like ALL was found to be characterized by a range of genomic alterations that activate a limited number of signaling pathways, all of which may be amenable to inhibition with approved tyrosine kinase inhibitors. Trials identifying Ph-like ALL are needed to assess whether adding tyrosine kinase inhibitors to current therapy will improve the survival of patients with this type of leukemia. (Funded by the American Lebanese Syrian Associated Charities and others.).

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