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: EC:3.6.3.44 (
P-glycoprotein
)
13,344
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The anticancer drug doxorubicin induces the synthesis of nitric oxide, a small molecule that enhances the drug cytotoxicity and reduces the drug efflux through the membrane pump
P-glycoprotein
(Pgp). Doxorubicin also induces the translocation on the plasma membrane of the protein
calreticulin
(
CRT
), which allows tumour cells to be phagocytized by dendritic cells. We have shown that doxorubicin elicits nitric oxide synthesis and
CRT
exposure only in drug-sensitive cells, not in drug-resistant ones, which are indeed chemo-immunoresistant. In this work, we investigate the mechanisms by which nitric oxide induces the translocation of
CRT
and the molecular basis of this chemo-immunoresistance. In the drug-sensitive colon cancer HT29 cells doxorubicin increased nitric oxide synthesis,
CRT
exposure and cells phagocytosis. Nitric oxide promoted the translocation of
CRT
in a guanosine monophosphate (cGMP) and actin cytoskeleton-dependent way.
CRT
translocation did not occur in drug-resistant HT29-dx cells, where the doxorubicin-induced nitric oxide synthesis was absent. By increasing nitric oxide with stimuli other than doxorubicin, the
CRT
exposure was obtained also in HT29-dx cells. Although in sensitive cells the
CRT
translocation was followed by the phagocytosis, in drug-resistant cells the phagocytosis did not occur despite the
CRT
exposure. In HT29-dx cells
CRT
was bound to Pgp and only by silencing the latter the
CRT
-operated phagocytosis was restored, suggesting that Pgp impairs the functional activity of
CRT
and the tumour cells phagocytosis. Our work suggests that the levels of nitric oxide and Pgp critically modulate the recognition of the tumour cells by dendritic cells, and proposes a new potential therapeutic approach against chemo-immunoresistant tumours.
...
PMID:Nitric oxide and P-glycoprotein modulate the phagocytosis of colon cancer cells. 2071 30
Cardiac glycosides induce a strong immunological cancer cell cytotoxicity, in which the released intracellular components of dying tumor cells (e.g.
calreticulin
, HMGB1 and ATP) stimulate immunity and help in eradicating cancer. Among the cardiac glycosides, oleandrin is an inhibitor of
P-glycoprotein
expression and exerts excellent penetration through the blood-brain barrier which also harbors neuroprotective and anti-glioma efficacies. Cardiac glycosides also exert neuroprotective activities, one explanation for such an action is the metabolic arrest as a defense strategy against hypoxia. Recently, it was also shown that oleandrin increases survival of glioma-implanted mice alone and in synergy with temozolomide, which also associated with the release of brain derived neurotrophic factor and activation of its receptor TrkB. In conclusion, oleandrin strongly deserves to be studied as a candidate molecule in treatment of neurodegenerative and neurooncological diseases.
...
PMID:Neuroprotective and tumoricidal activities of cardiac glycosides. Could oleandrin be a new weapon against stroke and glioblastoma? 2938 86
Doxorubicin is a strong inducer of immunogenic cell death (ICD), but it is ineffective in
P-glycoprotein
(Pgp)-expressing cells. Indeed, Pgp effluxes doxorubicin and impairs the immunesensitizing functions of
calreticulin
(
CRT
), an "eat-me" signal mediating ICD. It is unknown if classical Pgp inhibitors, designed to reverse chemoresistance, may restore ICD. We addressed this question by using Pgp-expressing cancer cells, treated with Tariquidar, a clinically approved Pgp inhibitor, and
R
-3 compound, a
N
,
N
-bis(alkanol)amine aryl ester derivative with the same potency of Tariquidar as Pgp inhibitor. In Pgp-expressing/doxorubicin-resistant cells, Tariquidar and
R
-3 increased doxorubicin accumulation and toxicity, reduced Pgp activity, and increased
CRT
translocation and ATP and HMGB1 release. Unexpectedly, only
R
-3 promoted phagocytosis by dendritic cells and activation of antitumor CD8
+
T-lymphocytes. Although Tariquidar did not alter the amount of Pgp present on cell surface,
R
-3 promoted Pgp internalization and ubiquitination, disrupting its interaction with
CRT
. Pgp knock-out restores doxorubicin-induced ICD in MDA-MB-231/DX cells that recapitulated the phenotype of
R
-3-treated cells. Our work demonstrates that plasma membrane-associated Pgp prevents a complete ICD notwithstanding the release of ATP and HMGB1, and the exposure of
CRT
. Pharmacological compounds reducing Pgp activity and amount may act as promising chemo- and immunesensitizing agents.
...
PMID:Insights into P-Glycoprotein Inhibitors: New Inducers of Immunogenic Cell Death. 3233 68
