Literature DB >> 33665638

Abnormal dopamine receptor signaling allows selective therapeutic targeting of neoplastic progenitors in AML patients.

Lili Aslostovar1, Allison L Boyd1, Yannick D Benoit2, Justin Di Lu3, Juan Luis Garcia Rodriguez1, Mio Nakanishi1, Deanna P Porras1,3, Jennifer C Reid1,3, Ryan R Mitchell1, Brian Leber4, Anargyros Xenocostas5, Ronan Foley6, Mickie Bhatia1,3.   

Abstract

The aberrant expression of dopamine receptors (DRDs) in acute myeloid leukemia (AML) cells has encouraged the repurposing of DRD antagonists such as thioridazine (TDZ) as anti-leukemic agents. Here, we access patient cells from a Phase I dose escalation trial to resolve the cellular and molecular bases of response to TDZ, and we extend these findings to an additional independent cohort of AML patient samples tested preclinically. We reveal that in DRD2+ AML patients, DRD signaling in leukemic progenitors provides leukemia-exclusive networks of sensitivity that spare healthy hematopoiesis. AML progenitor cell suppression can be increased by the isolation of the positive enantiomer from the racemic TDZ mixture (TDZ+), and this is accompanied by reduced cardiac liability. Our study indicates that the development of DRD-directed therapies provides a targeting strategy for a subset of AML patients and potentially other cancers that acquire DRD expression upon transformation from healthy tissue. Crown
Copyright © 2021.

Entities:  

Keywords:  Phase I trial; QTc interval; acute myeloid leukemia; cyclic AMP; dopamine receptor; leukemic progenitor; targeted therapy; thioridazine; xenograft

Mesh:

Substances:

Year:  2021        PMID: 33665638      PMCID: PMC7897800          DOI: 10.1016/j.xcrm.2021.100202

Source DB:  PubMed          Journal:  Cell Rep Med        ISSN: 2666-3791


  65 in total

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