Bak compensated for Bax in p53-null cells to release cytochrome c for the initiation of mitochondrial signaling during Withanolide D-induced apoptosis

Bak compensated for Bax in p53-null cells to release cytochrome c for the initiation of mitochondrial signaling during Withanolide D-induced apoptosis

The goal of cancer chemotherapy to induce multi-directional apoptosis as targeting a single pathway is unable to decrease all the downstream effect arises from crosstalk. Present study reports that Withanolide D (WithaD), a steroidal lactone isolated from Withania somnifera, induced cellular apoptos...

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Veröffentlicht in:PloS one 2012-03, Vol.7 (3), p.e34277-e34277
Hauptverfasser: Mondal, Susmita, Bhattacharya, Kaushik, Mallick, Asish, Sangwan, Rajender, Mandal, Chitra
Format: Artikel
Sprache:eng
Schlagworte:
Activation
Animals
Antineoplastic Agents - pharmacology
Apoptosis
Bax protein
bcl-2 Homologous Antagonist-Killer Protein - genetics
bcl-2 Homologous Antagonist-Killer Protein - physiology
bcl-2-Associated X Protein - genetics
bcl-2-Associated X Protein - physiology
Bids
Biology
Cancer
Cancer therapies
Caprolactone
Cell Line, Tumor
Chemotherapy
Councils
Crosstalk
Cytochrome
Cytochrome c
Cytochromes c - metabolism
Disruption
Gene Expression Regulation, Neoplastic
Humans
K562 Cells
Kinases
Leukemia
Membrane potential
Mice
Mice, Nude
Mitochondria
Mitochondria - metabolism
Molting
Neoplasm Transplantation
Null cells
Oligomerization
p53 Protein
Proteins
Signal Transduction
Signaling
Translocation
Tumor proteins
Tumor Suppressor Protein p53 - genetics
Tumorigenesis
Withania somnifera
Withanolides - pharmacology
Xenografts
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Zusammenfassung:The goal of cancer chemotherapy to induce multi-directional apoptosis as targeting a single pathway is unable to decrease all the downstream effect arises from crosstalk. Present study reports that Withanolide D (WithaD), a steroidal lactone isolated from Withania somnifera, induced cellular apoptosis in which mitochondria and p53 were intricately involved. In MOLT-3 and HCT116p53+/+ cells, WithaD induced crosstalk between intrinsic and extrinsic signaling through Bid, whereas in K562 and HCT116p53-/- cells, only intrinsic pathway was activated where Bid remain unaltered. WithaD showed pronounced activation of p53 in cancer cells. Moreover, lowered apoptogenic effect of HCT116p53-/- over HCT116p53+/+ established a strong correlation between WithaD-mediated apoptosis and p53. WithaD induced Bax and Bak upregulation in HCT116p53+/+, whereas increase only Bak expression in HCT116p53-/- cells, which was coordinated with augmented p53 expression. p53 inhibition substantially reduced Bax level and failed to inhibit Bak upregulation in HCT116p53+/+ cells confirming p53-dependent Bax and p53-independent Bak activation. Additionally, in HCT116p53+/+ cells, combined loss of Bax and Bak (HCT116Bax-Bak-) reduced WithaD-induced apoptosis and completely blocked cytochrome c release whereas single loss of Bax or Bak (HCT116Bax-Bak+/HCT116Bax+Bak-) was only marginally effective after WithaD treatment. In HCT116p53-/- cells, though Bax translocation to mitochondria was abrogated, Bak oligomerization helped the cells to release cytochrome c even before the disruption of mitochondrial membrane potential. WithaD also showed in vitro growth-inhibitory activity against an array of p53 wild type and null cancer cells and K562 xenograft in vivo. Taken together, WithaD elicited apoptosis in malignant cells through Bax/Bak dependent pathway in p53-wild type cells, whereas Bak compensated against loss of Bax in p53-null cells.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0034277