BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Autoimmunity, Doxorubicin, rs2476601, ERBB2, Coagulation, Hepatitis, Endothelial cell)
Bookmark Forward

Depletion of SAM50 Specifically Targets BCR-ABL-Expressing Leukemic Stem and Progenitor Cells by Interfering with Mitochondrial Functions.

Marta E Capala, Maurien Pruis, Edo Vellenga, Jan Jacob Schuringa

Stem cells and development 2016 Mar 1


filter terms:
  • aid (1)
  • BCR ABL (3)
  • CD34 (1)
  • cells (5)
  • growth (1)
  • hematopoietic stem and progenitor cells (5)
  • human cells (1)
  • leukemia (1)
  • mitochondria (2)
  • oxygen (2)
  • SAM50 (6)
  • species (2)
  • stem cells (2)
    • Sizes of these terms reflect their relevance to your search.

    A high proliferation rate of malignant cells requires an increased energy production, both by anaerobic glucose metabolism and mitochondrial respiration. Moreover, increased levels of mitochondria-produced reactive oxygen species (ROS) promote survival of transformed cells and contribute to the disease progression both in solid tumors and leukemia. Consequently, interfering with mitochondrial metabolism has been used as a strategy to specifically target leukemic cells. SAM50 is a mitochondrial outer membrane protein involved in the formation of mitochondrial intermembrane space bridging (MIB) complex. Although the importance of SAM50 in maintaining MIB integrity and in the assembly of mitochondrial respiratory chain complexes has been described, its specific role in the normal and leukemic hematopoietic cells remains unknown. We observed that human leukemic cells display a specific dependency on SAM50 expression, as downregulation of SAM50 in BCR-ABL-expressing, but not normal CD34(+) human hematopoietic stem and progenitor cells (HSPCs) caused a significant decrease in growth, colony formation, and replating capacity. Mitochondrial functions of BCR-ABL-expressing HSPCs were compromised, as seen by a decreased mitochondrial membrane potential and respiration. This effect of SAM50 downregulation was recapitulated in normal HSPCs exposed to cytokine-rich culture conditions that stimulate proliferation. Both oncogene-transduced and cytokine-stimulated HSPCs showed increased mitochondrial membrane potential and increased ROS levels compared to their normal counterparts. Therefore, we postulate that human leukemic HSPCs are highly dependent on the proper functioning of mitochondria and that disruption of mitochondrial integrity may aid in targeting leukemic cells.

    Citation

    Marta E Capala, Maurien Pruis, Edo Vellenga, Jan Jacob Schuringa. Depletion of SAM50 Specifically Targets BCR-ABL-Expressing Leukemic Stem and Progenitor Cells by Interfering with Mitochondrial Functions. Stem cells and development. 2016 Mar 1;25(5):427-37


    PMID: 26855047

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.