Literature DB >> 35487785

Harnessing the power of sphingolipids: Prospects for acute myeloid leukemia.

Johnson Ung1, Su-Fern Tan2, Todd E Fox3, Jeremy J P Shaw4, Luke R Vass4, Pedro Costa-Pinheiro5, Francine E Garrett-Bakelman6, Michael K Keng2, Arati Sharma7, David F Claxton7, Ross L Levine8, Martin S Tallman9, Myles C Cabot10, Mark Kester3, David J Feith2, Thomas P Loughran11.   

Abstract

Acute myeloid leukemia (AML) is an aggressive, heterogenous malignancy characterized by clonal expansion of bone marrow-derived myeloid progenitor cells. While our current understanding of the molecular and genomic landscape of AML has evolved dramatically and opened avenues for molecularly targeted therapeutics to improve upon standard intensive induction chemotherapy, curative treatments are elusive, particularly in older patients. Responses to current AML treatments are transient and incomplete, necessitating the development of novel treatment strategies to improve outcomes. To this end, harnessing the power of bioactive sphingolipids to treat cancer shows great promise. Sphingolipids are involved in many hallmarks of cancer of paramount importance in AML. Leukemic blast survival is influenced by cellular levels of ceramide, a bona fide pro-death molecule, and its conversion to signaling molecules such as sphingosine-1-phosphate and glycosphingolipids. Preclinical studies demonstrate the efficacy of therapeutics that target dysregulated sphingolipid metabolism as well as their combinatorial synergy with clinically-relevant therapeutics. Thus, increased understanding of sphingolipid dysregulation may be exploited to improve AML patient care and outcomes. This review summarizes the current knowledge of dysregulated sphingolipid metabolism in AML, evaluates how pro-survival sphingolipids promote AML pathogenesis, and discusses the therapeutic potential of targeting these dysregulated sphingolipid pathways.
Copyright © 2022 Elsevier Ltd. All rights reserved.

Entities:  

Keywords:  Bcl-2; Ceramide; Mcl-1; Sphingolipid dysregulation; Sphingosine-1-phosphate; Therapeutics

Mesh:

Substances:

Year:  2022        PMID: 35487785      PMCID: PMC9475810          DOI: 10.1016/j.blre.2022.100950

Source DB:  PubMed          Journal:  Blood Rev        ISSN: 0268-960X            Impact factor:   10.626


  223 in total

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Authors:  Samy A F Morad; Myles C Cabot
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Review 3.  Therapeutic potential of targeting sphingosine kinases and sphingosine 1-phosphate in hematological malignancies.

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Journal:  Leukemia       Date:  2016-07-27       Impact factor: 11.528

4.  Targeting FLT3-ITD signaling mediates ceramide-dependent mitophagy and attenuates drug resistance in AML.

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Journal:  Blood       Date:  2016-08-18       Impact factor: 22.113

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7.  Small-molecule targeting of MUSASHI RNA-binding activity in acute myeloid leukemia.

Authors:  Gerard Minuesa; Steven K Albanese; Wei Xie; Yaniv Kazansky; Daniel Worroll; Arthur Chow; Alexandra Schurer; Sun-Mi Park; Christina Z Rotsides; James Taggart; Andrea Rizzi; Levi N Naden; Timothy Chou; Saroj Gourkanti; Daniel Cappel; Maria C Passarelli; Lauren Fairchild; Carolina Adura; J Fraser Glickman; Jessica Schulman; Christopher Famulare; Minal Patel; Joseph K Eibl; Gregory M Ross; Shibani Bhattacharya; Derek S Tan; Christina S Leslie; Thijs Beuming; Dinshaw J Patel; Yehuda Goldgur; John D Chodera; Michael G Kharas
Journal:  Nat Commun       Date:  2019-06-19       Impact factor: 14.919

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Authors:  Tapan Mahendra Kadia; Hagop M Kantarjian; Marina Konopleva
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Review 9.  Targeting FLT3 mutations in AML: review of current knowledge and evidence.

Authors:  Naval Daver; Richard F Schlenk; Nigel H Russell; Mark J Levis
Journal:  Leukemia       Date:  2019-01-16       Impact factor: 11.528

10.  A Comparison of High-Dose Cytarabine During Induction Versus Consolidation Therapy in Newly Diagnosed AML.

Authors:  Anthony P Schwarer; Jason Butler; Kathryn Jackson; Ashanka Beligaswatte; Louisa Martin; Glen Kennedy; Zantomio Daniela; Ian Lewis; Devendra Hiwase; Joel Wight; Simon He; Andrew Grigg; Kirk Morris; Peter Mollee; Paula Marlton
Journal:  Hemasphere       Date:  2018-11-28
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