Targeting the 5T4 Oncofetal Glycoprotein with an Antibody Drug Conjugate (A1mcMMAF) Improves Survival in Patient-derived Xenograft Models of Acute Lymphoblastic Leukemia

Overview

Journal Haematologica

Specialty Hematology

Date 2017 Mar 26

PMID 28341731

Citations 6

Authors

Owen J McGinn

Shekhar Krishnan

Jean-Pierre Bourquin

Puja Sapra

Clare Dempsey

Vaskar Saha

Peter L Stern

Affiliations

Soon will be listed here.

Abstract

Outcome in childhood acute lymphoblastic leukemia is prognosticated from levels of minimal residual disease after remission induction therapy. Higher levels of minimal residual disease are associated with inferior results even with intensification of therapy, thus suggesting that identification and targeting of minimal residual disease cells could be a therapeutic strategy. Here we identify high expression of 5T4 in subclonal populations of patient-derived xenografts from patients with high, post-induction levels of minimal residual disease. 5T4-positive cells showed preferential ability to overcome the NOD-IL2Rγ mouse xenograft barrier, migrated on a CXCL12 gradient, preferentially localized to bone marrow and displayed the ability to reconstitute the original clonal composition on limited dilution engraftment. Treatment with A1mcMMAF (a 5T4-antibody drug conjugate) significantly improved survival without overt toxicity in mice engrafted with a 5T4-positive acute lymphoblastic leukemia cell line. Mice engrafted with 5T4-positive patient-derived xenograft cells were treated with combination chemotherapy or dexamethasone alone and then given A1mcMMAF in the minimal residual disease setting. Combination chemotherapy was toxic to NOD-IL2Rγ mice. While dexamethasone or A1mcMMAF alone improved outcomes, the sequential administration of dexamethasone and A1mcMMAF significantly improved survival (=0.0006) over either monotherapy. These data show that specifically targeting minimal residual disease cells improved outcomes and support further investigation of A1mcMMAF in patients with high-risk B-cell precursor acute lymphoblastic leukemia identified by 5T4 expression at diagnosis.

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