An Unexpected Protein Interaction Promotes Drug Resistance in Leukemia

Overview

Journal Nat Commun

Specialty Biology

Date 2017 Nov 18

PMID 29146910

Citations 14

Authors

Aaron Pitre

Yubin Ge

Wenwei Lin

Yao Wang

Yu Fukuda

Jamshid Temirov

Aaron H Phillips

Jennifer L Peters

Yiping Fan

Jing Ma

Amanda Nourse

Chandrima Sinha

Hai Lin

Richard Kriwacki

James R Downing

Tanja A Gruber

Victoria E Centonze

Anjaparavanda P Naren

Taosheng Chen

John D Schuetz

Affiliations

Soon will be listed here.

Abstract

The overall survival of patients with acute myeloid leukemia (AML) is poor and identification of new disease-related therapeutic targets remains a major goal for this disease. Here we show that expression of MPP1, a PDZ-domain-containing protein, highly correlated with ABCC4 in AML, is associated with worse overall survival in AML. Murine hematopoietic progenitor cells overexpressing MPP1 acquired the ability to serially replate in methylcellulose culture, a property crucially dependent upon ABCC4. The highly conserved PDZ-binding motif of ABCC4 is required for ABCC4 and MPP1 to form a protein complex, which increased ABCC4 membrane localization and retention, to enhance drug resistance. Specific disruption of this protein complex, either genetically or chemically, removed ABCC4 from the plasma membrane, increased drug sensitivity, and abrogated MPP1-dependent hematopoietic progenitor cell replating in methylcellulose. High-throughput screening identified Antimycin A as a small molecule that disrupted the ABCC4-MPP1 protein complex and reversed drug resistance in AML cell lines and in primary patient AML cells. In all, targeting the ABCC4-MPP1 protein complex can lead to new therapies to improve treatment outcome of AML, a disease where the long-term prognosis is poor.

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