Identification and Targeting of Treatment Resistant Progenitor Populations in T-cell Acute Lymphoblastic Leukemia

Overview

Journal Res Sq

Date 2023 Nov 14

PMID 37961674

Authors

Kai Tan

Jason Xu

Changya Chen

Tiffaney Vincent

Petri Polonen

Jianzhong Hu

Satoshi Yoshimura

Wenbao Yu

Jonathan Sussman

Chia-Hui Chen

Elizabeth Li

Caroline Diorio

Rawan Shraim

Haley Newman

Lahari Uppuluri

Alexander Li

Gregory Chen

Shovik Bandyopadhyay

David Wu

Yang-Yang Ding

Jessica Xu

Tristan Lim

Miles Hsu

Anusha Thadi

Kyung Jin Ahn

Chi-Yun Wu

Jacqueline Peng

Yusha Sun

Alice Wang

Rushabh Mehta

David Frank

Lauren Meyer

Mignon Loh

Elizabeth Raetz

Zhiguo Chen

Brent Wood

Meenakshi Devidas

Kimberly Dunsmore

Stuart Winter

Ti-Cheng Chang

Gang Wu

Stanley Pounds

Nancy Zhang

William Carroll

Stephen Hunger

Kathrin Bernt

Jun Yang

Charles Mullighan

David Teachey

Affiliations

Soon will be listed here.

Abstract

Refractoriness to initial chemotherapy and relapse after remission are the main obstacles to cure in T-cell Acute Lymphoblastic Leukemia (T-ALL). Biomarker guided risk stratification and targeted therapy have the potential to improve outcomes in high-risk T-ALL; however, cellular and genetic factors contributing to treatment resistance remain unknown. Previous bulk genomic studies in T-ALL have implicated tumor heterogeneity as an unexplored mechanism for treatment failure. To link tumor subpopulations with clinical outcome, we created an atlas of healthy pediatric hematopoiesis and applied single-cell multiomic (CITE-seq/snATAC-seq) analysis to a cohort of 40 cases of T-ALL treated on the Children's Oncology Group AALL0434 clinical trial. The cohort was carefully selected to capture the immunophenotypic diversity of T-ALL, with early T-cell precursor (ETP) and Near/Non-ETP subtypes represented, as well as enriched with both relapsed and treatment refractory cases. Integrated analyses of T-ALL blasts and normal T-cell precursors identified a bone-marrow progenitor-like (BMP-like) leukemia sub-population associated with treatment failure and poor overall survival. The single-cell-derived molecular signature of BMP-like blasts predicted poor outcome across multiple subtypes of T-ALL within two independent patient cohorts using bulk RNA-sequencing data from over 1300 patients. We defined the mutational landscape of BMP-like T-ALL, finding that mutations additively drive T-ALL blasts away from the BMP-like state. We transcriptionally matched BMP-like blasts to early thymic seeding progenitors that have low expression and high stem cell gene expression, corresponding to a corticosteroid and conventional cytotoxic resistant phenotype we observed in drug screening. To identify novel targets for BMP-like blasts, we performed and drug screening against the BMP-like signature and prioritized BMP-like overexpressed cell-surface (CD44, ITGA4, LGALS1) and intracellular proteins (BCL-2, MCL-1, BTK, NF-κB) as candidates for precision targeted therapy. We established patient derived xenograft models of BMP-high and BMP-low leukemias, which revealed vulnerability of BMP-like blasts to apoptosis-inducing agents, TEC-kinase inhibitors, and proteasome inhibitors. Our study establishes the first multi-omic signatures for rapid risk-stratification and targeted treatment of high-risk T-ALL.

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