Project EVOLVE: an international analysis of postimmunotherapy lineage switch, an emergent form of relapse in leukemia

Sara Silbert; Alexander W. Rankin; Chloe Hoang; Alexandra Semchenkova; Regina M. Myers; Elena Zerkalenkova; Hao‐Wei Wang; Alexandra E. Kovach; Constance M. Yuan; Dana Delgado Colon; Loïc Vasseur; Álex Bataller; Samuel John; Kaylyn Utley Lyons; Barbara D. Friedes; Anna Alonso‐Saladrigues; Hisham Abdel‐Azim; Estelle Balducci; Ahmed Abdulrahman; Marie Balsat; D. N. Biery; Aghiad Chamdin; Bill H. Chang; Raymund S. Cuevo; Barbara De Moerloose; David S. Dickens; Ulrich Duffner; Nicolas Duployez; Firas El Chaer; Michelle A. Elliott; Gabriele Escherich; Sneha Fernandes; Mandi R. Fitzjohn; Zhubin Gahvari; Stephan A. Grupp; Rui He; Cynthia Harrison; Christopher A. Hergott; Emily M. Hsieh; Annette S. Kim; Dennis John Kuo; Daniel P. Larson; Benjamin J. Lee; Thibaut Leguay; R. Coleman Lindsley; Abhishek A. Mangaonkar; Kerstin Mezger; Holly Pacenta; Jing Pan; Marlie R. M. Provost; Latika Puri; Sunil S. Raikar; Armando Martinez; Isabella Quijada Bristol; Kyle Murphy; Lauren T. Reiman; Michele S. Redell; Kelly Reed; Gabrielle Roth Guépin; Jeremy D. Rubinstein; Süreyya Savaşan; Kristian T. Schafernak; Alexandra M. Stevens; Aimee C. Talleur; Naomi Torres Carapia; Jacques Vargaftig; Anant Vatsayan; Matthias Wölfl; Liang Zhao; Susana Rives; Vanessa A. Fabrizio; Koji Sasaki; Ibrahim Aldoss; Nicolas Boissel; Susan R. Rheingold; Kara L. Davis; Sara Ghorashian; Elad Jacoby; А. М. Попов; Adam J. Lamble; Nirali N. Shah

doi:10.1182/blood.2024026655

Project EVOLVE: an international analysis of postimmunotherapy lineage switch, an emergent form of relapse in leukemia

Sara Silbert(National Institutes of Health), Alexander W. Rankin(National Institutes of Health), Chloe Hoang(National Institutes of Health), Alexandra Semchenkova(Dmitry Rogachev National Research Center of Pediatric Hematology, Oncology and Immunology), Regina M. Myers(Children's Hospital of Philadelphia), Elena Zerkalenkova(Dmitry Rogachev National Research Center of Pediatric Hematology, Oncology and Immunology), Hao‐Wei Wang(National Institutes of Health), Alexandra E. Kovach(University of Southern California), Constance M. Yuan(National Institutes of Health), Dana Delgado Colon(National Institutes of Health), Loïc Vasseur(Saint Louis University Hospital), Álex Bataller(The University of Texas MD Anderson Cancer Center), Samuel John(Southwestern Medical Center), Kaylyn Utley Lyons(University of Colorado Hospital), Barbara D. Friedes(Children's Hospital of Philadelphia), Anna Alonso‐Saladrigues(Hospital Sant Joan de Déu Barcelona), Hisham Abdel‐Azim(Loma Linda University Medical Center), Estelle Balducci(Hôpital Necker-Enfants Malades), Ahmed Abdulrahman(Children's Healthcare of Atlanta), Marie Balsat(Hôpital Lyon Sud), D. N. Biery(National Institutes of Health), Aghiad Chamdin(Central Michigan University), Bill H. Chang(Oregon Health and Science University Hospital), Raymund S. Cuevo(Virginia Cancer Institute), Barbara De Moerloose(Ghent University Hospital), David S. Dickens(University of Iowa Hospitals and Clinics), Ulrich Duffner(Michigan United), Nicolas Duployez(Centre Hospitalier Universitaire de Lille), Firas El Chaer(University of Virginia), Michelle A. Elliott(Mayo Clinic), Gabriele Escherich(Universität Hamburg), Sneha Fernandes(Great Ormond Street Hospital), Mandi R. Fitzjohn(University of Colorado Hospital), Zhubin Gahvari(University of Wisconsin–Madison), Stephan A. Grupp(Children's Hospital of Philadelphia), Rui He(Inova Health System), Cynthia Harrison(National Institutes of Health), Christopher A. Hergott(Brigham and Women's Hospital), Emily M. Hsieh(Children's Hospital of Los Angeles), Annette S. Kim(University of Michigan), Dennis John Kuo(University of California San Diego), Daniel P. Larson(Mayo Clinic), Benjamin J. Lee(Chapman University), Thibaut Leguay(Centre Hospitalier Universitaire de Bordeaux), R. Coleman Lindsley(Dana-Farber Cancer Institute), Abhishek A. Mangaonkar(Mayo Clinic), Kerstin Mezger(Universität Hamburg), Holly Pacenta(Cook Children's Medical Center), Jing Pan(Beijing Hospital), Marlie R. M. Provost(HealthONE), Latika Puri(Loma Linda University Children's Hospital), Sunil S. Raikar(Emory University), Armando Martinez(National Institutes of Health), Isabella Quijada Bristol(National Institutes of Health), Kyle Murphy(National Institutes of Health), Lauren T. Reiman(University of Southern California), Michele S. Redell(Baylor College of Medicine), Kelly Reed(University of Virginia), Gabrielle Roth Guépin(Centre Hospitalier Régional et Universitaire de Nancy), Jeremy D. Rubinstein(Cincinnati Children's Hospital Medical Center), Süreyya Savaşan(Central Michigan University), Kristian T. Schafernak(Phoenix Children's Hospital), Alexandra M. Stevens(Baylor College of Medicine), Aimee C. Talleur(St. Jude Children's Research Hospital), Naomi Torres Carapia(Children's Hospital of Los Angeles), Jacques Vargaftig(Institut Curie), Anant Vatsayan(Children's National), Matthias Wölfl(Universitätsklinikum Würzburg), Liang Zhao(Chinese Academy of Medical Sciences & Peking Union Medical College), Susana Rives(Hospital Sant Joan de Déu Barcelona), Vanessa A. Fabrizio(Children's Hospital Colorado), Koji Sasaki(The University of Texas MD Anderson Cancer Center), Ibrahim Aldoss(City Of Hope National Medical Center), Nicolas Boissel(Université Paris Cité), Susan R. Rheingold(Children's Hospital of Philadelphia), Kara L. Davis(Institute for Stem Cell Biology and Regenerative Medicine), Sara Ghorashian(Great Ormond Street Hospital), Elad Jacoby(Tel Aviv University), А. М. Попов(National Medical Research Center for Hematology), Adam J. Lamble(Seattle Children's Hospital), Nirali N. Shah(National Institutes of Health)

Blood

April 7, 2025

10.1182/blood.2024026655

Cited by 23Open Access

Full Text

Abstract

ABSTRACT: Lineage switch (LS), defined as the immunophenotypic transformation of acute leukemia, has emerged as a mechanism of relapse after antigen-targeted immunotherapy, which is associated with dismal outcomes. Through an international collaborative effort, we identified cases of LS after a host of antigen-targeted therapies (eg, CD19, CD22, CD38, and CD7), described how LS was diagnosed, reviewed treatment approaches, and analyzed overall outcomes for this form of postimmunotherapy relapse. Collectively, 75 cases of LS were evaluated, including 53 (70.7%) cases of B-cell acute lymphoblastic leukemia (B-ALL) transforming to acute myeloid leukemia (AML), 17 (22.7%) cases of B-ALL transforming to mixed phenotypic acute leukemia (MPAL)/acute leukemias of ambiguous lineage (ALAL), and 5 (6.7%) cases of rare LS presentation (ie, T-cell ALL to AML). An additional 10 cases with incomplete changes in immunophenotype, referred to as "lineage drift" were also described. With a primary focus on the 70 cases of LS from B-ALL to AML or MPAL/ALAL, LS emerged at a median of 1.5 months (range, 0-36.5) after immunotherapy, with 81.4% presenting with LS within the first 6 months from the most proximal immunotherapy. Although most involved KMT2A rearrangements (n = 45, 64.3%), other rare cytogenetic and/or molecular alterations were uniquely observed. Treatment outcomes were generally poor, with remission rates of <40%. The median overall survival after LS diagnosis was 4.8 months. Outcomes were similarly poor for those with rare immunophenotypes of LS or lineage drift. This global initiative robustly categorizes lineage changes after immunotherapy and, through enhanced understanding, establishes a foundation for improving outcomes of LS.

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