Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UNIPROT:P02794 (
ferritin
)
17,525
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Artesunate
(
ART
) is an anti-malaria drug that has been shown to exhibit anti-tumor activity, and functional lysosomes are reported to be required for
ART
-induced cancer cell death, whereas the underlying molecular mechanisms remain largely elusive. In this study, we aimed to elucidate the molecular mechanisms underlying
ART
-induced cell death. We first confirmed that
ART
induces apoptotic cell death in cancer cells. Interestingly, we found that
ART
preferably accumulates in the lysosomes and is able to activate lysosomal function via promotion of lysosomal V-ATPase assembly. Furthermore, we found that lysosomes function upstream of mitochondria in reactive oxygen species production. Importantly, we provided evidence showing that lysosomal iron is required for the lysosomal activation and mitochondrial reactive oxygen species production induced by
ART
. Finally, we showed that
ART
-induced cell death is mediated by the release of iron in the lysosomes, which results from the lysosomal degradation of
ferritin
, an iron storage protein. Meanwhile, overexpression of ferritin heavy chain significantly protected cells from
ART
-induced cell death. In addition, knockdown of nuclear receptor coactivator 4, the adaptor protein for
ferritin
degradation, was able to block
ART
-mediated
ferritin
degradation and rescue the
ART
-induced cell death. In summary, our study demonstrates that
ART
treatment activates lysosomal function and then promotes
ferritin
degradation, subsequently leading to the increase of lysosomal iron that is utilized by
ART
for its cytotoxic effect on cancer cells. Thus, our data reveal a new mechanistic action underlying
ART
-induced cell death in cancer cells.
...
PMID:Artesunate induces cell death in human cancer cells via enhancing lysosomal function and lysosomal degradation of ferritin. 2530 13
Artesunate
(
ART
) is a prominent anti-malarial with significant anti-cancer properties. Our previous studies showed that
ART
enhances lysosomal function and
ferritin
degradation, which was necessary for its anti-cancer properties.
ART
targeting to mitochondria also significantly improved its efficacy, but the effect of
ART
on mitophagy, an important cellular pathway that facilitates the removal of damaged mitochondria, remains unknown. Here, we first observed that
ART
mainly localizes in the mitochondria and its probe labeling revealed that it binds to a large number of mitochondrial proteins and causes mitochondrial fission. Second, we found that
ART
treatment leads to autophagy induction and the decrease of mitochondrial proteins. When autophagy is inhibited, the decrease of mitochondrial proteins could be reversed, indicating that the degradation of mitochondrial proteins is through mitophagy. Third, our results showed that
ART
treatment stabilizes the full-length form of PTEN induced putative kinase 1 (PINK1) on the mitochondria and activates the PINK1-dependent pathway. This in turn leads to the recruitment of Parkin, sequestosome 1 (SQSTM1), ubiquitin and microtubule-associated proteins 1A/1B light chain 3 (LC3) to the mitochondria and culminates in mitophagy. When PINK1 is knocked down,
ART
-induced mitophagy is markedly suppressed. Finally, we investigated the effect of mitophagy by
ART
on mitochondrial functions and found that knockdown of PINK1 alters the cellular redox status in
ART
-treated cells, which is accompanied with a significant decrease in glutathione (GSH) and increase in mitochondrial reactive oxidative species (mROS) and cellular lactate levels. Additionally, knockdown of PINK1 leads to a significant increase of mitochondrial depolarization and more cell apoptosis by
ART
, suggesting that mitophagy protects from
ART
-induced cell death. Taken together, our findings reveal the molecular mechanism that
ART
induces cytoprotective mitophagy through the PINK1-dependent pathway, suggesting that mitophagy inhibition could enhance the anti-cancer activity of
ART
.
...
PMID:Artesunate-induced mitophagy alters cellular redox status. 3019 90
Sorafenib is the first-line medication for advanced hepatocellular carcinoma (HCC), but it can only extend limited survival. It is imperative to find a combination strategy to increase sorafenib efficacy.
Artesunate
is such a preferred candidate, because artesunate is clinically well-tolerated and more importantly both drugs can induce ferroptosis through different mechanisms. In this study we investigated the combined effect of sorafenib and artesunate in inducing ferroptosis of HCC and elucidated the involved molecular mechanisms. We showed that artesunate greatly enhanced the anticancer effects of low dose of sorafenib against Huh7, SNU-449, and SNU-182 HCC cell lines in vitro and against Huh7 cell xenograft model in Balb/c nude mice. The combination index method confirmed that the combined effect of sorafenib and artesunate was synergistic. Compared with the treatment with artesunate or sorafenib alone, combined treatment induced significantly exacerbated lipid peroxidation and ferroptosis, which was blocked by N-acetyl cysteine and ferroptosis inhibitors liproxstatin-1 and deferoxamine mesylate, but not by inhibitors of other types of cell death (z-VAD, necrostatin-1 and belnacasan). In Huh7 cells, we demonstrated that the combined treatment induced oxidative stress and lysosome-mediated ferritinophagy, two essential aspects of ferroptosis. Sorafenib at low dose mainly caused oxidative stress through mitochondrial impairments and SLC7A11-invovled glutathione depletion.
Artesunate
-induced lysosome activation synergized with sorafenib-mediated pro-oxidative effects by promoting sequential reactions including lysosomal cathepsin B/L activation,
ferritin
degradation, lipid peroxidation, and consequent ferroptosis. Taken together, artesunate could be repurposed to sensitize sorafenib in HCC treatment. The combined treatment can be easily translated into clinical applications.
...
PMID:Artesunate synergizes with sorafenib to induce ferroptosis in hepatocellular carcinoma. 3269 65
