About

Stephen P. Hunger, MD, is a Professor of Pediatrics (Oncology) at the Perelman School of Medicine at the University of Pennsylvania. He serves as an Attending Physician and the Chief of the Division of Oncology at the Children's Hospital of Philadelphia, where he is also the Director of the Center for Childhood Cancer Research. Additionally, he holds the position of Associate Director for Pediatric Research at the Abramson Cancer Center and is a member of its Executive Committee. His professional focus is on pediatric oncology, with a particular emphasis on childhood cancer research. His contributions include leadership roles in clinical and translational research initiatives aimed at improving outcomes for children with cancer. His work involves integrating genomic analysis, personalized digital health interventions, and innovative treatment strategies to advance pediatric cancer care.

Research topics

• Computer Science
• Medicine
• Internal medicine
• Oncology
• Pediatrics
• Computational biology
• Genetics
• Biology
• Bioinformatics
• World Wide Web
• Pathology

Selected publications

• Diminished Quality of Life Despite Reduced Treatment in Children With B‐Lymphoblastic Leukemia: Children's Oncology Group AALL0932

  Pediatric Blood & Cancer · 2026-01-05

  article

  BACKGROUND: Quality of life (QOL) is impacted in children treated for leukemia. AALL0932 randomized reduction in vincristine/dexamethasone (VCR/DEX) pulses every 4 versus 12 weeks during maintenance in the average-risk subset of NCI standard risk B-ALL (NCI-SR AR B-ALL). We longitudinally assessed physical and emotional QOL, behavioral health, and school services by randomization. PROCEDURE: NCI-SR AR B-ALL English-speaking patients aged ≥4 years were evaluated at T1-T5 (∼2, 9, 18, 26 months [females treatment end], and 38 [males only] months from diagnosis) with parent-report. The Pediatric Quality of Life Inventory-4.0 and school services survey were administered longitudinally, and the Behavior Assessment Scale for Children-2 at therapy end. RESULTS: Data were obtained from 420 consented and randomized participants (mean 6.0±1.6 years, 45.7% female). Impairment among randomized participants at T2 and T4, respectively, was 11.3% and 12.5% for physical, and 12.2% and 9.8% for emotional function. In longitudinal models adjusting for race/ethnicity, time, and baseline impairment, pulse frequency was not associated with impairment (physical odds ratio [OR] = 0.9, 95% confidence interval [CI] = 0.5-1.8; emotional OR = 0.9, 95% CI = 0.5-1.7). T2 impairment was associated with increased risk of post-randomization impairment for physical (OR = 4.3, 95% CI: 1.9-9.9) and emotional (OR = 4.9, CI: 2.3-10.5) function. Approximately 73.8% reported one or more school-based service during treatment: special education/accommodations (67.6%) and physical/occupational therapy (8.8%). Depression (20%) and anxiety (19%) did not differ by pulse frequency. DISCUSSION: Children with NCI-SR AR B-ALL experience diminished QOL, despite reduced frequency of VCR/DEX maintenance pulses. Impairment begins early during ALL therapy and persists; interventions should commence early and continue throughout and after therapy.

  PublisherDOI

• Real‐World Pediatric Blinatumomab Administration: Access to Outpatient Care Delivery and Impact of a Hospital‐Dispensed Model

  Pediatric Blood & Cancer · 2026-04-10

  articleOpen access

  Blinatumomab has been shown to be highly effective for patients with pediatric B-ALL and has recently become standard of care therapy. Due to its past use in the clinical trial setting, there is limited information available about real-world administration. In this brief report, we describe our institutional experience administering blinatumomab during the first year as standard of care therapy, including initial challenges in providing access to patients without home health coverage. We describe our process for developing and implementing a process for hospital-dispensed blinatumomab, which reduced access barriers for patients.

  PublisherDOI

• Adding Induction Intrathecal Cytarabine in Newly Diagnosed CNS2 B-Acute Lymphoblastic Leukemia Does Not Improve Outcomes

  Blood Advances · 2026-04-15

  articleOpen access

  Patients with central nervous system (CNS) disease at diagnosis on Children's Oncology Group (COG) B-acute lymphoblastic leukemia (B-ALL) trials AALL0331 and AALL0232 had inferior outcomes, largely secondary to CNS relapse. In response, for patients with newly diagnosed B-ALL enrolled on COG studies AALL0932 and AALL1131, therapy was adjusted to incorporate additional intrathecal cytarabine during induction for patients with low level CNS involvement (CNS2). We evaluated the impact of this intervention. Event-free survival (EFS), overall survival (OS), and cumulative incidence of relapse (CIR) were compared among CNS2 patients pre- versus post-amendment, stratified by receipt of a 3-drug (SR) or 4-drug (HR) induction. Multivariable models were constructed to adjust for demographic and disease variables. When stratified by trial, pre- and post-amendment patients with CNS2 status did not differ significantly by demographic or disease factors. Additional intrathecal cytarabine doses during induction did not improve outcomes for patients with B-ALL. Multivariable analyses adjusting for disease prognosticators, race/ethnicity, and leukemia cytogenetics did not identify any subpopulation that significantly benefited from additional intrathecal cytarabine. Additional intrathecal cytarabine during induction for CNS2 patients did not improve outcomes or mitigate the adverse prognostic impact of CNS2 status in B-ALL. Future COG B-ALL studies will not include additional intrathecal cytarabine in induction for patients with CNS2 disease. Alternative treatment strategies are needed for patients with CNS2 disease.

  PublisherOA PDFDOI

• Reduced-intensity reinduction for children and young persons with relapsed acute lymphoblastic leukemia

  Leukemia · 2026-04-29

  articleOpen access
  PublisherOA PDFDOI

• Correction: Impact of Genetic Ancestry on Genomics and Survival Outcomes in T-cell Acute Lymphoblastic Leukemia

  Blood Cancer Discovery · 2026-02-12

  articleOpen access

  In the original version of this article (1), in Fig. 3B, patients with high-risk NGS but low-risk MRD and WBC were inadvertently misclassified as "adverse" rather than in the correct "intermediate" risk category.

  PublisherOA PDFDOI

• Next Generation Sequencing Minimal Residual Disease in Pediatric B-ALL after CD19 and/or CD22 CAR T-cell Therapy: Depth and Kinetics of Response Predict Relapse Risk.

  Transplantation and Cellular Therapy · 2026-02-01

  article
  PublisherDOI

• High Rates of Clinically Significant Late Infections and Recurrent Sinopulmonary Disease in Long-Term Survivors after CD19 CAR T-cell Therapy for Pediatric B-ALL

  Transplantation and Cellular Therapy · 2026-02-01

  article
  PublisherDOI

• Chromosome 15q deletions confer inferior outcomes among children with ETV6::RUNX1 B-Cell Acute Lymphoblastic Leukemia

  Blood Advances · 2026-04-15

  articleOpen access
  PublisherDOI

• Erratum: Successful Outcomes of Newly Diagnosed T Lymphoblastic Lymphoma: Results From Children's Oncology Group AALL0434

  Journal of Clinical Oncology · 2026-01-05

  article
  PublisherDOI

• Figure S1 from Integrative Genomic Analyses Identify LncRNA Regulatory Networks across Pediatric Leukemias and Solid Tumors

  2025-11-24

  articleOpen access

  <p>Figure S1: Workflow for RNA-seq gene mapping and quantification</p>

  PublisherOA PDFDOI

Recent grants

• NIH Grant F32CA009184

  NIH · $69k

• NIH Grant U01CA157937

  NIH · $2.9M · 2017

• NIH Grant RC2CA148529

  NIH · $1.7M · 2012

• Center for Pediatric Tumor Cell Atlas - Admin Supplement

  NIH · $16.2M · 2023–2025

• NIH Grant M01RR000082

  NIH · $30.1M · 2011

Frequent coauthors

• Meenakshi Devidas

  St. Jude Children's Research Hospital

  1351 shared

• Mignon L. Loh

  St. Jude Children's Research Hospital

  1097 shared

• William L. Carroll

  St. Jude Children's Research Hospital

  1047 shared

• Elizabeth A. Raetz

  NYU Langone Health

  905 shared

• Naomi J. Winick

  The University of Texas Southwestern Medical Center

  840 shared

• Cheryl L. Willman

  St. Jude Children's Research Hospital

  693 shared

• Michael J. Borowitz

  St. Jude Children's Research Hospital

  641 shared

• Bruce M. Camitta

  Medical College of Wisconsin

  492 shared

Education

• B.S., Applied Biology

  Massachusetts Institute of Technology

  1981

• M.D.

  University of Connecticut School of Medicine

  1985

Awards & honors

• The ASPHO 2025 Distinguished Career Award