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: UMLS:C0017636 (
glioblastoma
)
18,345
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Glioblastoma
is a fatal disease in which most targeted therapies have clinically failed. However, pharmacological reactivation of tumour suppressors has not been thoroughly studied as yet as a
glioblastoma
therapeutic strategy. Tumour suppressor protein phosphatase 2A is inhibited by non-genetic mechanisms in
glioblastoma
, and thus, it would be potentially amendable for therapeutic reactivation. Here, we demonstrate that
s
mall
m
olecule
a
ctivators of
p
rotein phosphatase 2A, NZ-8-061 and
DBK
-1154, effectively cross the
in vitro
model of blood-brain barrier, and
in vivo
partition to mouse brain tissue after oral dosing.
In vitro
, small molecule activators of protein phosphatase 2A exhibit robust cell-killing activity against five established
glioblastoma
cell lines, and nine patient-derived primary glioma cell lines. Collectively, these cell lines have heterogeneous genetic background, kinase inhibitor resistance profile and stemness properties; and they represent different clinical
glioblastoma
subtypes. Moreover, small molecule activators of protein phosphatase 2A were found to be superior to a range of kinase inhibitors in their capacity to kill patient-derived primary glioma cells. Oral dosing of either of the small molecule activators of protein phosphatase 2A significantly reduced growth of infiltrative intracranial
glioblastoma
tumours.
DBK
-1154, with both higher degree of brain/blood distribution, and more potent
in vitro
activity against all tested
glioblastoma
cell lines, also significantly increased survival of mice bearing orthotopic
glioblastoma
xenografts. In summary, this report presents a proof-of-principle data for blood-brain barrier-permeable tumour suppressor reactivation therapy for
glioblastoma
cells of heterogenous molecular background. These results also provide the first indications that protein phosphatase 2A reactivation might be able to challenge the current paradigm in
glioblastoma
therapies which has been strongly focused on targeting specific genetically altered cancer drivers with highly specific inhibitors. Based on demonstrated role for protein phosphatase 2A inhibition in
glioblastoma
cell drug resistance, small molecule activators of protein phosphatase 2A may prove to be beneficial in future
glioblastoma
combination therapies.
...
PMID:Monotherapy efficacy of blood-brain barrier permeable small molecule reactivators of protein phosphatase 2A in glioblastoma. 3295 76
