Platelets promote mitochondrial uncoupling and resistance to apoptosis in leukemia cells: A novel paradigm for the bone marrow microenvironment

Juliana Velez; Leonardo José Enciso; Marta Suarez; Michael Fiegl; Adriana Grismaldo; Catalina López; Alfonso Barreto; Claudia Cardozo; Pilar Palacios; Ludis Morales; Jorge Eduardo Duque; Jorge Uriel Carmona; Marina Konopleva; Michael Andreeff; Ismael Samudio

doi:10.1007/s12307-014-0149-3

Platelets promote mitochondrial uncoupling and resistance to apoptosis in leukemia cells: A novel paradigm for the bone marrow microenvironment

Juliana Velez
, Leonardo José Enciso
, Marta Suarez
, Michael Fiegl
, Adriana Grismaldo
, Catalina López
, Alfonso Barreto
, Claudia Cardozo
, Pilar Palacios
, Ludis Morales
, Jorge Eduardo Duque
, Jorge Uriel Carmona
, Marina Konopleva
, Michael Andreeff
, Ismael Samudio

Research output: Contribution to journal › Article › peer-review

32 Scopus citations

Abstract

Here we report that leukemia cell lines and primary CD34+ leukemic blasts exposed to platelet rich plasma (PRP) or platelet lysates (PL) display increased resistance to apoptosis induced by mitochondria-targeted agents ABT-737 and CDDO-Me. Intriguingly, leukemia cells exposed to platelet components demonstrate a reduction in mitochondrial membrane potential (ΔΨM) and a transient increase in oxygen consumption, suggestive of mitochondrial uncoupling. Accompanying the ranolazine-sensitive increase in oxygen consumption, a reduction in triglyceride content was also observed in leukemia cells cultured with platelet components indicating that lipolysis and fatty acid oxidation may support the molecular reduction of oxygen in these cells. Mechanistically, platelet components antagonized Bax oligomerization in accordance with previous observations supporting an antiapoptotic role for fatty acid oxidation in leukemia cells. Lastly, substantiating the notion that mitochondrial uncoupling reduces oxidative stress, platelet components induced a marked decrease in basal and rotenone-induced superoxide levels in leukemia cells. Taken together, the decrease in ΔΨM, the transient increase in ranolazine-sensitive oxygen consumption, the reduction in triglyceride levels, and the reduced generation of superoxide, all accompanying the increased resistance to mitochondrial apoptosis, substantiate the hypothesis that platelets may contribute to the chemoprotective sanctuary of the bone marrow microenvironment via promotion of mitochondrial uncoupling.

Original language	English
Pages (from-to)	79-90
Number of pages	12
Journal	Cancer Microenvironment
Volume	7
Issue number	1-2
DOIs	https://doi.org/10.1007/s12307-014-0149-3
State	Published - Aug 2014

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Keywords

ABT-737
Apoptosis
CDDO-Me
Fatty acid oxidation
Leukemia
Metabolism
Mitochondrial uncoupling
Platelets

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10.1007/s12307-014-0149-3

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Velez, J., Enciso, L. J., Suarez, M., Fiegl, M., Grismaldo, A., López, C., Barreto, A., Cardozo, C., Palacios, P., Morales, L., Duque, J. E., Carmona, J. U., Konopleva, M., Andreeff, M., & Samudio, I. (2014). Platelets promote mitochondrial uncoupling and resistance to apoptosis in leukemia cells: A novel paradigm for the bone marrow microenvironment. Cancer Microenvironment, 7(1-2), 79-90. https://doi.org/10.1007/s12307-014-0149-3

@article{2a855a6f808f4b82954f9445a99816b8,

title = "Platelets promote mitochondrial uncoupling and resistance to apoptosis in leukemia cells: A novel paradigm for the bone marrow microenvironment",

abstract = "Here we report that leukemia cell lines and primary CD34+ leukemic blasts exposed to platelet rich plasma (PRP) or platelet lysates (PL) display increased resistance to apoptosis induced by mitochondria-targeted agents ABT-737 and CDDO-Me. Intriguingly, leukemia cells exposed to platelet components demonstrate a reduction in mitochondrial membrane potential (ΔΨM) and a transient increase in oxygen consumption, suggestive of mitochondrial uncoupling. Accompanying the ranolazine-sensitive increase in oxygen consumption, a reduction in triglyceride content was also observed in leukemia cells cultured with platelet components indicating that lipolysis and fatty acid oxidation may support the molecular reduction of oxygen in these cells. Mechanistically, platelet components antagonized Bax oligomerization in accordance with previous observations supporting an antiapoptotic role for fatty acid oxidation in leukemia cells. Lastly, substantiating the notion that mitochondrial uncoupling reduces oxidative stress, platelet components induced a marked decrease in basal and rotenone-induced superoxide levels in leukemia cells. Taken together, the decrease in ΔΨM, the transient increase in ranolazine-sensitive oxygen consumption, the reduction in triglyceride levels, and the reduced generation of superoxide, all accompanying the increased resistance to mitochondrial apoptosis, substantiate the hypothesis that platelets may contribute to the chemoprotective sanctuary of the bone marrow microenvironment via promotion of mitochondrial uncoupling.",

keywords = "ABT-737, Apoptosis, CDDO-Me, Fatty acid oxidation, Leukemia, Metabolism, Mitochondrial uncoupling, Platelets",

author = "Juliana Velez and Enciso, \{Leonardo Jos{\'e}\} and Marta Suarez and Michael Fiegl and Adriana Grismaldo and Catalina L{\'o}pez and Alfonso Barreto and Claudia Cardozo and Pilar Palacios and Ludis Morales and Duque, \{Jorge Eduardo\} and Carmona, \{Jorge Uriel\} and Marina Konopleva and Michael Andreeff and Ismael Samudio",

note = "Funding Information: Acknowledgments This work was supported by funds from the Oficina para el Fomento de la Investigaci{\'o}n, Pontificia Universidad Javeriana (OFI; Project ID 4049) to I.S., a grant from the Departamento Administrativo de Ciencia y Tecnologia COLCIENCIAS (Project ID 120351929072) to I.S., NIH CA51164, CA16672 and CA100632 to M.A., and the Paul and Mary Haas chair in Genetics to M.A. The authors wish to acknowledge Alba Myriam Campos and Antonia Infante for technical and administrative support and Angelica Pinz{\'o}n for technical support. The authors are particularly grateful to Dr. Dario Londo{\~n}o for his scientific and clinical contributions to this project.",

year = "2014",

month = aug,

doi = "10.1007/s12307-014-0149-3",

language = "English",

volume = "7",

pages = "79--90",

journal = "Cancer Microenvironment",

issn = "1875-2292",

publisher = "Springer Netherlands",

number = "1-2",

}

Velez, J, Enciso, LJ, Suarez, M, Fiegl, M, Grismaldo, A, López, C, Barreto, A, Cardozo, C, Palacios, P, Morales, L, Duque, JE, Carmona, JU, Konopleva, M, Andreeff, M & Samudio, I 2014, 'Platelets promote mitochondrial uncoupling and resistance to apoptosis in leukemia cells: A novel paradigm for the bone marrow microenvironment', Cancer Microenvironment, vol. 7, no. 1-2, pp. 79-90. https://doi.org/10.1007/s12307-014-0149-3

TY - JOUR

T1 - Platelets promote mitochondrial uncoupling and resistance to apoptosis in leukemia cells

T2 - A novel paradigm for the bone marrow microenvironment

AU - Velez, Juliana

AU - Enciso, Leonardo José

AU - Suarez, Marta

AU - Fiegl, Michael

AU - Grismaldo, Adriana

AU - López, Catalina

AU - Barreto, Alfonso

AU - Cardozo, Claudia

AU - Palacios, Pilar

AU - Morales, Ludis

AU - Duque, Jorge Eduardo

AU - Carmona, Jorge Uriel

AU - Konopleva, Marina

AU - Andreeff, Michael

AU - Samudio, Ismael

N1 - Funding Information: Acknowledgments This work was supported by funds from the Oficina para el Fomento de la Investigación, Pontificia Universidad Javeriana (OFI; Project ID 4049) to I.S., a grant from the Departamento Administrativo de Ciencia y Tecnologia COLCIENCIAS (Project ID 120351929072) to I.S., NIH CA51164, CA16672 and CA100632 to M.A., and the Paul and Mary Haas chair in Genetics to M.A. The authors wish to acknowledge Alba Myriam Campos and Antonia Infante for technical and administrative support and Angelica Pinzón for technical support. The authors are particularly grateful to Dr. Dario Londoño for his scientific and clinical contributions to this project.

PY - 2014/8

Y1 - 2014/8

N2 - Here we report that leukemia cell lines and primary CD34+ leukemic blasts exposed to platelet rich plasma (PRP) or platelet lysates (PL) display increased resistance to apoptosis induced by mitochondria-targeted agents ABT-737 and CDDO-Me. Intriguingly, leukemia cells exposed to platelet components demonstrate a reduction in mitochondrial membrane potential (ΔΨM) and a transient increase in oxygen consumption, suggestive of mitochondrial uncoupling. Accompanying the ranolazine-sensitive increase in oxygen consumption, a reduction in triglyceride content was also observed in leukemia cells cultured with platelet components indicating that lipolysis and fatty acid oxidation may support the molecular reduction of oxygen in these cells. Mechanistically, platelet components antagonized Bax oligomerization in accordance with previous observations supporting an antiapoptotic role for fatty acid oxidation in leukemia cells. Lastly, substantiating the notion that mitochondrial uncoupling reduces oxidative stress, platelet components induced a marked decrease in basal and rotenone-induced superoxide levels in leukemia cells. Taken together, the decrease in ΔΨM, the transient increase in ranolazine-sensitive oxygen consumption, the reduction in triglyceride levels, and the reduced generation of superoxide, all accompanying the increased resistance to mitochondrial apoptosis, substantiate the hypothesis that platelets may contribute to the chemoprotective sanctuary of the bone marrow microenvironment via promotion of mitochondrial uncoupling.

AB - Here we report that leukemia cell lines and primary CD34+ leukemic blasts exposed to platelet rich plasma (PRP) or platelet lysates (PL) display increased resistance to apoptosis induced by mitochondria-targeted agents ABT-737 and CDDO-Me. Intriguingly, leukemia cells exposed to platelet components demonstrate a reduction in mitochondrial membrane potential (ΔΨM) and a transient increase in oxygen consumption, suggestive of mitochondrial uncoupling. Accompanying the ranolazine-sensitive increase in oxygen consumption, a reduction in triglyceride content was also observed in leukemia cells cultured with platelet components indicating that lipolysis and fatty acid oxidation may support the molecular reduction of oxygen in these cells. Mechanistically, platelet components antagonized Bax oligomerization in accordance with previous observations supporting an antiapoptotic role for fatty acid oxidation in leukemia cells. Lastly, substantiating the notion that mitochondrial uncoupling reduces oxidative stress, platelet components induced a marked decrease in basal and rotenone-induced superoxide levels in leukemia cells. Taken together, the decrease in ΔΨM, the transient increase in ranolazine-sensitive oxygen consumption, the reduction in triglyceride levels, and the reduced generation of superoxide, all accompanying the increased resistance to mitochondrial apoptosis, substantiate the hypothesis that platelets may contribute to the chemoprotective sanctuary of the bone marrow microenvironment via promotion of mitochondrial uncoupling.

KW - ABT-737

KW - Apoptosis

KW - CDDO-Me

KW - Fatty acid oxidation

KW - Leukemia

KW - Metabolism

KW - Mitochondrial uncoupling

KW - Platelets

UR - https://www.scopus.com/pages/publications/84907018289

U2 - 10.1007/s12307-014-0149-3

DO - 10.1007/s12307-014-0149-3

M3 - Article

AN - SCOPUS:84907018289

SN - 1875-2292

VL - 7

SP - 79

EP - 90

JO - Cancer Microenvironment

JF - Cancer Microenvironment

IS - 1-2

ER -

Platelets promote mitochondrial uncoupling and resistance to apoptosis in leukemia cells: A novel paradigm for the bone marrow microenvironment

Abstract

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Keywords

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