CD9 Blockade Suppresses Disease Progression of High-risk Pediatric B-cell Precursor Acute Lymphoblastic Leukemia and Enhances Chemosensitivity

Overview

Journal Leukemia

Specialties Hematology
Oncology

Date 2019 Oct 19

PMID 31624373

Citations 13

Authors

Kam Tong Leung

Chi Zhang

Kathy Yuen Yee Chan

Karen Li

John Tak Kit Cheung

Margaret Heung Ling Ng

Xiao-Bing Zhang

Tony Sit

Wayne Yuk Wai Lee

Wei Kang

Ka Fai To

Jasmine Wai Sum Yu

Toni Ki Fong Man

Han Wang

Kam Sze Tsang

Frankie Wai Tsoi Cheng

Grace Kee See Lam

Tin Wai Chow

Alex Wing Kwan Leung

Ting Fan Leung

Patrick Man Pan Yuen

Pak Cheung Ng

Chi Kong Li

Affiliations

Soon will be listed here.

Abstract

CD9 has been implicated in cancer progression but its prognostic relevance and therapeutic potential in B-cell precursor acute lymphoblastic leukemia (BCP-ALL) are largely unknown. In a cohort of pediatric BCP-ALL patients, we found that CD9 cases had a significantly lower 5-year relapse-free survival rate than CD9 cases. Multivariate analysis demonstrated that CD9 positivity independently predicted inferior survival outcomes, and could be applied with established prognostic features, including prednisone response and cytogenetic status, to refine patient stratification. Administration of CD9 antibody substantially suppressed disease progression in NOD/SCID mice xenografted with CD9 cell lines and primary leukemic blasts from patients with high-risk and refractory BCP-ALL, without compromising hematopoietic stem cell engraftment. Combination of anti-CD9 with conventional chemotherapy further reduced leukemic burden and prolonged animal survival. Mechanistically, CD9 blockade inhibited leukemic cell proliferation, induced G/G cell cycle arrest, activated p38, and enhanced chemotherapeutic agent-induced apoptosis. Further, CD9 physically interacted with integrin very late antigen-4, regulated affinity to vascular cell adhesion molecule-1, and was involved in leukemia-stroma interaction. Collectively, our study established CD9 as a new prognostic marker, validated the preclinical efficacy of CD9 antibody, and laid the foundation for clinical development of CD9-targeted therapy for high-risk and refractory pediatric BCP-ALL.

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