Pegylation of phenothiazine – A synthetic route towards potent anticancer drugs

Cibotaru, Sandu; Năstasă, Valentin; Sandu, Andreea-Isabela; Bostănaru, Andra-Cristina; Mareș, Mihai; Marin, Luminița

dc.contributor.author	Cibotaru, Sandu
dc.contributor.author	Năstasă, Valentin
dc.contributor.author	Sandu, Andreea-Isabela
dc.contributor.author	Bostănaru, Andra-Cristina
dc.contributor.author	Mareș, Mihai
dc.contributor.author	Marin, Luminița
dc.date.accessioned	2023-04-25T08:11:58Z
dc.date.available	2023-04-25T08:11:58Z
dc.date.issued	2022-03-07
dc.identifier.uri	https://www.sciencedirect.com/science/article/pii/S2090123221001375
dc.identifier.uri	https://repository.iuls.ro/xmlui/handle/20.500.12811/3209
dc.description.abstract	Introduction Cancer is a big challenge of the 21 century, whose defeat requires efficient antitumor drugs. Objectives The paper aims to investigate the synergistic effect of two structural building blocks, phenothiazine and poly(ethylene glycol), towards efficient antitumor drugs. Methods Two PEGylated phenothiazine derivatives were synthetized by attaching poly(ethylene glycol) of 550 Da to the nitrogen atom of phenothiazine by ether or ester linkage. Their antitumor activity has been investigated on five human tumour lines and a mouse tumor line as well, by determination of IC50. The in vivo toxicity was determined by measuring the LD50 in BALB/c mice by the sequential method and the in vivo antitumor potential was measured by the tumours growth test. The antitumor mechanism was investigated by complexation studies of zinc and magnesium ions characteristic to the farnesyltransferase enzyme, by studies of self-aggregation in the cells proximity and by investigation of the antitumor properties of the acid species resulted by enzymatic cleavage of the PEGylated derivatives. Results The two compounds showed antitumor activity, with IC50 against mouse colon carcinoma cell line comparable with that of the traditional antitumor drugs 5-Fluorouracil and doxorubicin. The phenothiazine PEGylation resulted in a significant toxicity diminishing, the LD50 in BALB/c mice increasing from 952.38 up to 1450 mg/kg, in phenothiazine equivalents. Both compounds inflicted a 92% inhibition of the tumour growth for doses much smaller than LD50. The investigation of the possible tumour inhibition mechanism suggested the nanoaggregate formation and the cleavage of ester bonds as key factors for the inhibition of cancer cell proliferation and biocompatibility improvement. Conclusion Phenothiazine and PEG building blocks have a synergetic effect working for both tumour growth inhibition and biocompatibility improvement. All these findings recommend the PEGylated phenothiazine derivatives as a valuable workbench for a next generation of antitumor drugs.	en_US
dc.language.iso	en	en_US
dc.publisher	Elsevier	en_US
dc.rights
dc.rights.uri
dc.subject	Tumour growth inhibition	en_US
dc.subject	Poly(ethylene glycol)	en_US
dc.subject	Phenothiazine	en_US
dc.title	Pegylation of phenothiazine – A synthetic route towards potent anticancer drugs	en_US
dc.type	Article	en_US
dc.author.affiliation	Sandu Cibotaru, Andreea-Isabela Sandu, Luminita Marin, Petru Poni” Institute of Macromolecular Chemistry of Romanian Academy, Iasi, Romania
dc.author.affiliation	Valentin Nastasa, Andra-Cristina Bostanaru, Mihai Mares, Ion Ionescu de la Brad” University, Laboratory of Antimicrobial Chemotherapy, Iasi, Romania
dc.publicationName	Journal of Advanced Research
dc.volume	37
dc.publicationDate	2022
dc.startingPage	279
dc.endingPage	290
dc.identifier.eissn	2090-1224
dc.identifier.doi	https://doi.org/10.1016/j.jare.2021.07.003