Hepatic IGFBP1 is a prosurvival factor that binds to BAK, protects the liver from apoptosis, and antagonizes the proapoptotic actions of p53 at mitochondria

Leu, Julia I-Ju; George, Donna L.

doi:10.1101/gad.1567107

Cited by 96 publications

(79 citation statements)

References 75 publications

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“…PFT-α is a small-molecule inhibitor shown to specifically inhibit the direct proapoptotic actions of p53 at mitochondria, by reducing the affinity of p53 toward its mitochondrial interaction partners Bcl-2, Bcl-XL, and Bak. 106,107 Pretreatment with PFT-α was shown to rescue primary thymocytes in vitro and mice in vivo, from lethal doses of γ-irradiation or DNA-damaging agents.…”

Section: Pft-α Inhibits B-agnp-and F-agnpinduced P53-dependent Ros Prmentioning

confidence: 99%

Comparative assessment of the apoptotic potential of silver nanoparticles synthesized by Bacillus tequilensis and Calocybe indica in MDA-MB-231 human breast cancer cells: targeting p53 for anticancer therapy

Gurunathan¹,

Park²,

Han³

et al. 2015

IJN

275

151

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Background Recently, the use of nanotechnology has been expanding very rapidly in diverse areas of research, such as consumer products, energy, materials, and medicine. This is especially true in the area of nanomedicine, due to physicochemical properties, such as mechanical, chemical, magnetic, optical, and electrical properties, compared with bulk materials. The first goal of this study was to produce silver nanoparticles (AgNPs) using two different biological resources as reducing agents, Bacillus tequilensis and Calocybe indica. The second goal was to investigate the apoptotic potential of the as-prepared AgNPs in breast cancer cells. The final goal was to investigate the role of p53 in the cellular response elicited by AgNPs. Methods The synthesis and characterization of AgNPs were assessed by various analytical techniques, including ultraviolet-visible (UV-vis) spectroscopy, X-ray diffraction (XRD), Fourier transform infrared (FTIR) spectroscopy, dynamic light scattering (DLS), and transmission electron microscopy (TEM). The apoptotic efficiency of AgNPs was confirmed using a series of assays, including cell viability, leakage of lactate dehydrogenase (LDH), production of reactive oxygen species (ROS), DNA fragmentation, mitochondrial membrane potential, and Western blot. Results The absorption spectrum of the yellow AgNPs showed the presence of nanoparticles. XRD and FTIR spectroscopy results confirmed the crystal structure and biomolecules involved in the synthesis of AgNPs. The AgNPs derived from bacteria and fungi showed distinguishable shapes, with an average size of 20 nm. Cell viability assays suggested a dose-dependent toxic effect of AgNPs, which was confirmed by leakage of LDH, activation of ROS, and terminal deoxynucleotidyl transferase dUTP nick end labeling (TUNEL)-positive cells in MDA-MB-231 breast cancer cells. Western blot analyses revealed that AgNPs induce cellular apoptosis via activation of p53, p-Erk1/2, and caspase-3 signaling, and downregulation of Bcl-2. Cells pretreated with pifithrin-alpha were protected from p53-mediated AgNPs-induced toxicity. Conclusion We have demonstrated a simple approach for the synthesis of AgNPs using the novel strains B. tequilensis and C. indica , as well as their mechanism of cell death in a p53-dependent manner in MDA-MB-231 human breast cancer cells. The present findings could provide insight for the future development of a suitable anticancer drug, which may lead to the development of novel nanotherapeutic molecules for the treatment of cancers.

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Section: Pft-α Inhibits B-agnp-and F-agnpinduced P53-dependent Ros Prmentioning

confidence: 99%

Comparative assessment of the apoptotic potential of silver nanoparticles synthesized by Bacillus tequilensis and Calocybe indica in MDA-MB-231 human breast cancer cells: targeting p53 for anticancer therapy

Gurunathan¹,

Park²,

Han³

et al. 2015

IJN

275

151

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“…In contrast to the thymus-and spleen-derived cells that undergo p53-mediated apoptosis in response to genotoxic stress, liver cancer cells tend to be resistant [25][26][27] suggesting that the HCC may have mechanism(s) leading to inactivation of p53-mediated apoptosis. In our earlier proteomic studies, 11,28,29 we identified members of the heat shock family proteins that are often upregulated in HCC and associated prognostic outcomes, and mortalin as a marker for predicting HCC metastasis and recurrence.…”

Section: Discussionmentioning

confidence: 99%

Induction of mutant p53‐dependent apoptosis in human hepatocellular carcinoma by targeting stress protein mortalin

Lü

Lee

Kaul

et al. 2011

Intl Journal of Cancer

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Stress protein mortalin (mtHSP70) is highly expressed in cancer cells. It was shown to contribute to carcinogenesis by sequestrating the wild type p53, a key tumor suppressor protein, in the cytoplasm resulting in an abrogation of its transcriptional activation function. We have found that the level of mortalin expression has significant correlation with human hepatocellular carcinoma (HCC) malignancy and therefore investigated whether it interacts with and influences the activities of mutant p53, frequently associated with HCC development. We have detected mortalin-p53 interactions in liver tumor and five HCC cell lines that harbored mutant p53. The data was in contrast to the normal liver and immortalized normal hepatocytes that lacked mortalin-p53 interaction. Furthermore, we have found that the shRNA-mediated mortalin silencing could induce mutant p53-mediated tumor-specific apoptosis in HCC. Such allotment of apoptotic function to mutant p53 by targeting mortalin-p53 interaction in cancer cells is a promising strategy for HCC therapy.Hepatocellular carcinoma (HCC) is a lethal malignancy associated with poor prognosis and the fifth most common cancer worldwide. Effective HCC therapeutics still await molecular understanding of the mechanisms and development of effective reagents that could selectively kill cancer cells. Like any other tumors, HCC has high rate of mutations in tumor suppressor protein p53, and is afflicted in p53-mediated functions including cell cycle arrest and apoptosis.1 Recently, several studies have identified that the mutant p53 executes transcription and nontranscription activities.2,3 Several p53 mutants with a low level of transcriptional activation function were also shown to induce apoptosis in cancer cells demonstrating nontranscriptional apoptotic ability of mutant p53. 4,5 However, in cancer cells such apoptotic function of p53 is often deregulated by multiple pathways including its binding with other proteins.6,7 Restoration of p53-mediated apoptosis is an attractive strategy for cancer therapy.Mortalin/mthsp70/GRP75/PBP74 is a member of the heat shock protein 70 family and has been shown to have multiple functions including chaperoning, mitochondrial import, energy generation and intracellular trafficking. 8,9 It exists in multiple subcellular sites and possesses multiple binding partners. 8,9 Several studies have shown that mortalin is frequently upregulated in cancers and contributes to carcinogenesis. [10][11][12][13][14] It was shown to cause cytoplasmic sequestration of wild type p53 resulting in inhibition of its transcriptional activation and control of centrosome duplication functions, both commonly associated with cancers.15-17 Furthermore, mortalin binding p53 peptides and cationic inhibitor of mortalin (MKT-077) were shown to (i) release p53 from mortalin-p53 complexes, (ii) cause nuclear translocation of p53 and (iii) cause growth arrest of cancer cells that contained wild type p53. 16,18 Mortalin was identified as a marker for HCC metastasis and recurrence by prot...

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“…Activated Bax and Bak adopt a new conformation that allows them to homo-oligomerize and form the OMM pore. Somewhat controversially, in addition to BH3-only proteins, other proteins including transcription factors such as p53 and IGFBP1 have been reported to directly bind and activate Bax/ Bak (15,16).…”

Section: Bcl-2 Family Members: Components Of the Omm Pore And Regulatmentioning

confidence: 99%

The mitochondrial gateway to cell death

Smith

Kluck

et al. 2008

IUBMB Life

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Mitochondria play a key role in death signaling. The intermembrane space of these organelles contains a number of proteins which promote cell death once they are redistributed to the cytosol. The formation of pores in the outer membrane of mitochondria defines a gateway through which the apoptogenic proteins pass during death signaling. Interactions between pro‐apoptotic and pro‐survival members of the Bcl‐2 family of proteins are decisive in the initiation of pore opening. While the specific composition of the pore in molecular terms is still subject to debate and continuing investigation, it is recognized functionally as a passive channel which not only allows egress of proteins to cytosol but also entry in the reverse direction. A variety of constraints may restrict the release of proteins from the intermembrane space to the cytosol. These include trapping in the intercristal spaces formed by the convoluted invaginations of the inner membrane, binding of proteins to the inner membrane or to other soluble proteins of the intermembrane space, or insertion of proteins into the inner membrane. There is a corresponding variety of mechanisms that facilitate release of apoptogenic proteins from such entrapment. Morphological changes that expand the inner membrane enable proteins to be released from enclosure in intercristal spaces, allowing these proteins access to the mitochondrial gateway. Specific cases include cytochrome c molecules bound to inner membrane cardiolipin and released upon oxidation of that lipid component. Further, AIF that is embedded in the inner membrane is released by proteases (caspases or calpains), which enter from the cytosol once the outer membrane pore has opened. The facilitation (or restriction) of apoptogenic protein release through the mitochondrial gateway may provide new opportunities for regulating cell death. © 2008 IUBMB IUBMB Life, 60(6): 383–389, 2008.

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Hepatic IGFBP1 is a prosurvival factor that binds to BAK, protects the liver from apoptosis, and antagonizes the proapoptotic actions of p53 at mitochondria

Cited by 96 publications

References 75 publications

Comparative assessment of the apoptotic potential of silver nanoparticles synthesized by Bacillus tequilensis and Calocybe indica in MDA-MB-231 human breast cancer cells: targeting p53 for anticancer therapy

Comparative assessment of the apoptotic potential of silver nanoparticles synthesized by Bacillus tequilensis and Calocybe indica in MDA-MB-231 human breast cancer cells: targeting p53 for anticancer therapy

Induction of mutant p53‐dependent apoptosis in human hepatocellular carcinoma by targeting stress protein mortalin

The mitochondrial gateway to cell death

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Hepatic IGFBP1 is a prosurvival factor that binds to BAK, protects the liver from apoptosis, and antagonizes the proapoptotic actions of p53 at mitochondria

Cited by 96 publications

References 75 publications

Comparative assessment of the apoptotic potential of silver nanoparticles synthesized by Bacillus tequilensis and Calocybe indica in&nbsp;MDA-MB-231 human breast cancer cells: targeting p53 for anticancer therapy

Comparative assessment of the apoptotic potential of silver nanoparticles synthesized by Bacillus tequilensis and Calocybe indica in&nbsp;MDA-MB-231 human breast cancer cells: targeting p53 for anticancer therapy

Induction of mutant p53‐dependent apoptosis in human hepatocellular carcinoma by targeting stress protein mortalin

The mitochondrial gateway to cell death

Contact Info

Product

Resources

About

Comparative assessment of the apoptotic potential of silver nanoparticles synthesized by Bacillus tequilensis and Calocybe indica in MDA-MB-231 human breast cancer cells: targeting p53 for anticancer therapy

Comparative assessment of the apoptotic potential of silver nanoparticles synthesized by Bacillus tequilensis and Calocybe indica in MDA-MB-231 human breast cancer cells: targeting p53 for anticancer therapy