Inclusion of Nitrofurantoin into the Realm of Cancer Chemotherapy via Biology-Oriented Synthesis and Drug Repurposing

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dc.contributor.authorElzahhar, Perihan A.
dc.contributor.authorNematalla, Hisham A.
dc.contributor.authorAl-Koussa, Houssam
dc.contributor.authorAbrahamian, Carla
dc.contributor.authorEl-Yazbi, Amira F.
dc.contributor.authorBodgi, Larry
dc.contributor.authorBou-Gharios, Jolie
dc.contributor.authorAzzi, Joyce
dc.contributor.authorAl-Choboq, Joelle
dc.contributor.authorLabib, Hala F.
dc.contributor.authorAbou-Kheir, Wassim G.
dc.contributor.authorAbu-Serie, Marwa M.
dc.contributor.authorElrewiny, Mohamed A.
dc.contributor.authorEl-Yazbi, Ahmed F.
dc.contributor.authorBelal, Ahmed Saied F.
dc.contributor.departmentPharmacology and Toxicology
dc.contributor.departmentRadiation Oncology
dc.contributor.departmentAnatomy, Cell Biology, and Physiological Sciences
dc.contributor.facultyFaculty of Medicine (FM)
dc.contributor.institutionAmerican University of Beirut
dc.date.accessioned2025-01-24T11:40:03Z
dc.date.available2025-01-24T11:40:03Z
dc.date.issued2023
dc.description.abstractStructural modifications of the antibacterial drug nitrofurantoin were envisioned, employing drug repurposing and biology-oriented drug synthesis, to serve as possible anticancer agents. Eleven compounds showed superior safety in non-cancerous human cells. Their antitumor efficacy was assessed on colorectal, breast, cervical, and liver cancer cells. Three compounds induced oxidative DNA damage in cancer cells with subsequent cellular apoptosis. They also upregulated the expression of Bax while downregulated that of Bcl-2 along with activating caspase 3/7. The DNA damage induced by these compounds, demonstrated by pATM nuclear shuttling, was comparable in both MCF7 and MDA-MB-231 (p53 mutant) cell lines. Mechanistic studies confirmed the dependence of these compounds on p53-mediated pathways as they suppressed the p53-MDM2 interaction. Indeed, exposure of radiosensitive prostatic cancer cells to low non-cytotoxic concentrations of compound 1 enhanced the cytotoxic response to radiation indicating a possible synergistic effect. In vivo antitumor activity was verified in an MCF7-xenograft animal model. © 2023 American Chemical Society.
dc.identifier.doihttps://doi.org/10.1021/acs.jmedchem.2c01408
dc.identifier.eid2-s2.0-85150421693
dc.identifier.pmid36921275
dc.identifier.urihttp://hdl.handle.net/10938/29420
dc.language.isoen
dc.publisherAmerican Chemical Society
dc.relation.ispartofJournal of Medicinal Chemistry
dc.sourceScopus
dc.subjectAnimals
dc.subjectAntineoplastic agents
dc.subjectApoptosis
dc.subjectBiology
dc.subjectBreast neoplasms
dc.subjectCell line, tumor
dc.subjectCell proliferation
dc.subjectDrug repositioning
dc.subjectFemale
dc.subjectHumans
dc.subjectNitrofurantoin
dc.subjectTumor suppressor protein p53
dc.subject1 [[(5 nitrofuran 2 yl)methylene]amino] 3 (2 oxo 2 phenylethyl)imidazolidine 2,4 dione
dc.subject1 [[(5 nitrofuran 2 yl)methylene]amino] 3 [(1 phenyl 1h 1,2,3 triazol 4 yl)methyl]imidazolidine 2,4 dione
dc.subject1 [[(5 nitrofuran 2 yl)methylene]amino] 3 [2 oxo 2 (4 tolyl)ethyl]imidazolidine 2,4 dione
dc.subject1 [[(5 nitrofuran 2 yl)methylene]amino] 3 [[1 (4 nitrophenyl) 1h 1,2,3 triazol 4 yl]methyl]imidazolidine 2,4 dione
dc.subject1 [[(5 nitrofuran 2 yl)methylene]amino] 3 [[1 (4 tolyl) 1h 1,2,3 triazol 4 yl]methyl]imidazolidine 2,4 dione
dc.subject3 (4 bromobenzyl) 1 [[(5 nitrofuran 2 yl)methylene]amino]imidazolidine 2,4 dione
dc.subject3 (4 nitrobenzyl) 1 [[(5 nitrofuran 2 yl)methylene]amino]imidazolidine 2,4 dione
dc.subject3 benzyl 1 [[(5 nitrofuran 2 yl)methylene]amino]imidazolidine 2,4 dione
dc.subject3 [2 (4 bromophenyl) 2 oxoethyl] 1 [[(5 nitrofuran 2 yl)methylene]amino]imidazolidine 2,4 dione
dc.subject3 [2 (4 chlorophenyl) 2 oxoethyl] 1 [[(5 nitrofuran 2 yl)methylene]amino]imidazolidine 2,4 dione
dc.subject3 [2 (4 methoxyphenyl) 2 oxoethyl] 1 [[(5 nitrofuran 2 yl)methylene]amino]imidazolidine 2,4 dione
dc.subject3 [[1 (4 chlorophenyl) 1h 1,2,3 triazol 4 yl]methyl]1 [[(5 nitrofuran 2 yl)methylene]amino]imidazolidine 2,4 dione
dc.subject4 [4 [[3 [[(5 nitrofuran 2 yl)methylene]amino] 2,5 dioxoimidazolidin 1 yl]methyl] 1h 1,2,3 triazol 1 yl] n (thiazol 2 yl)benzenesulfonamide
dc.subject4 [4 [[3 [[(5 nitrofuran 2 yl)methylene]amino] 2,5 dioxoimidazolidin 1 yl]methyl] 1h 1,2,3 triazol 1 yl]benzenesulfonamide
dc.subjectAntineoplastic agent
dc.subjectCaspase 3
dc.subjectCaspase 7
dc.subjectFluorouracil
dc.subjectMouse double minute 2 homolog
dc.subjectProtein bax
dc.subjectProtein bcl 2
dc.subjectProtein p53
dc.subjectUnclassified drug
dc.subjectAdult
dc.subjectAnimal experiment
dc.subjectAnimal model
dc.subjectAntineoplastic activity
dc.subjectArticle
dc.subjectCancer chemotherapy
dc.subjectControlled study
dc.subjectCytotoxicity
dc.subjectDna damage
dc.subjectDrug efficacy
dc.subjectDrug synthesis
dc.subjectEnzyme activity
dc.subjectHuman
dc.subjectHuman cell
dc.subjectIn vivo study
dc.subjectMale
dc.subjectMalignant neoplasm
dc.subjectMcf-7 cell line
dc.subjectMda-mb-231 cell line
dc.subjectNonhuman
dc.subjectNucleocytoplasmic transport
dc.subjectOxidation
dc.subjectProtein expression
dc.subjectTumor volume
dc.subjectUpregulation
dc.subjectAnimal
dc.subjectBreast tumor
dc.subjectChemistry
dc.subjectGenetics
dc.subjectTumor cell line
dc.titleInclusion of Nitrofurantoin into the Realm of Cancer Chemotherapy via Biology-Oriented Synthesis and Drug Repurposing
dc.typeArticle

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