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Target Concepts:
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Query: UMLS:C0017636 (
glioblastoma
)
18,345
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
In the effort to improve treatment effectiveness in
glioblastoma
, this short note reviewed collected data on the pathophysiology of
glioblastoma
with particular reference to intersections with the pharmacology of perphenazine. That study identified five areas of potentially beneficial intersection. Data showed seemingly 5 independent perphenazine attributes of benefit to
glioblastoma
treatment - i) blocking dopamine receptor 2, ii) reducing centrifugal migration of subventricular zone cells by blocking dopamine receptor 3, iii) blocking serotonin receptor 7, iv) activation of protein phosphatase 2, and v) nausea reduction.
Perphenazine
is fully compatible with current chemoirradiation protocols and with the commonly used ancillary medicines used in clinical practice during the course of
glioblastoma
. All these attributes argue for a trial of perphenazine's addition to current standard treatment with temozolomide and irradiation. The subventricular zone seeds the brain with mutated cells that become recurrent
glioblastoma
after centrifugal migration. The current paper shows how perphenazine might reduce that contribution.
Perphenazine
is an old, generic, cheap, phenothiazine antipsychotic drug that has been in continuous clinical use worldwide since the 1950's. Clinical experience and research data over these decades have shown perphenazine to be well-tolerated in psychiatric populations, in normals, and in non-psychiatric, medically ill populations for whom perphenazine is used to reduce nausea. For now (Summer, 2020) the nature of
glioblastoma
requires a polypharmacy approach until/unless a core feature and means to address it can be identified in the future. Conclusions:
Perphenazine
possesses a remarkable constellation of attributes that recommend its use in GB treatment.
...
PMID:Adding perphenazine to increase effectiveness of standard glioblastoma chemoirradiation. 3309 1