Photodynamic therapy offers a novel approach to managing miltefosine-resistant cutaneous leishmaniasis

dc.contributor.authorCABRAL, FERNANDA V.
dc.contributor.authorRIAHI, MINA
dc.contributor.authorPERSHEYEV, SAYDULLA
dc.contributor.authorLIAN, CHENG
dc.contributor.authorCORTEZ, MAURO
dc.contributor.authorSAMUEL, IFOR D.W.
dc.contributor.authorRIBEIRO, MARTHA S.
dc.coverageInternacional
dc.date.accessioned2024-12-13T11:13:31Z
dc.date.available2024-12-13T11:13:31Z
dc.date.issued2024
dc.description.abstractCutaneous leishmaniasis (CL) is a neglected disease caused by Leishmania parasites. The oral drug miltefosine is effective, but there is a growing problem of drug resistance, which has led to increasing treatment failure rates and relapse of infections. Photodynamic therapy (PDT) combines a light source and a photoactive drug to promote cell death by oxidative stress. Although PDT is effective against several pathogens, its use against drug-resistant Leishmania parasites remains unexplored. Herein, we investigated the potential of organic light-emitting diodes (OLEDs) as wearable light sources, which would enable at-home use or ambulatory treatment of CL. We also assessed its impact on combating miltefosine resistance in Leishmania amazonensis-induced CL in mice. The in vitro activity of OLEDs combined with 1,9-dimethyl-methylene blue (DMMB) (OLED-PDT) was evaluated against wild-type and miltefosine-resistant L. amazonensis strains in promastigote (EC50 = 0.034 μM for both strains) and amastigote forms (EC50 = 0.052 μM and 0.077 μM, respectively). Cytotoxicity in macrophages and fibroblasts was also evaluated. In vivo, we investigated the potential of OLED-PDT in combination with miltefosine using different protocols. Our results demonstrate that OLED-PDT is effective in killing both strains of L. amazonensis by increasing reactive oxygen species and stimulating nitric oxide production. Moreover, OLED-PDT showed great antileishmanial activity in vivo, allowing the reduction of miltefosine dose by half in infected mice using a light dose of 7.8 J/cm2 and 15 μM DMMB concentration. In conclusion, OLED-PDT emerges as a new avenue for at-home care and allows a combination therapy to overcome drug resistance in cutaneous leishmaniasis.
dc.description.sponsorshipEngineering and Physical Sciences Research Council (EPSRC)
dc.description.sponsorshipScottish Funding Council (SFC)
dc.description.sponsorshipConselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq)
dc.description.sponsorshipIDEPSRC: EP/R035164/1; EP/L015110/1
dc.description.sponsorshipIDSFC: SFC/AN/12/2017
dc.description.sponsorshipIDCNPq: 465763/2014-6; 440228/2021-2
dc.format.extent1-13
dc.identifier.citationCABRAL, FERNANDA V.; RIAHI, MINA; PERSHEYEV, SAYDULLA; LIAN, CHENG; CORTEZ, MAURO; SAMUEL, IFOR D.W.; RIBEIRO, MARTHA S. Photodynamic therapy offers a novel approach to managing miltefosine-resistant cutaneous leishmaniasis. <b>Biomedicine and Pharmacotherapy</b>, v. 177, p. 1-13, 2024. DOI: <a href="https://dx.doi.org/10.1016/j.biopha.2024.116881">10.1016/j.biopha.2024.116881</a>. Disponível em: https://repositorio.ipen.br/handle/123456789/48772.
dc.identifier.doi10.1016/j.biopha.2024.116881
dc.identifier.issn0753-3322
dc.identifier.orcidhttps://orcid.org/0000-0002-4203-1134
dc.identifier.percentilfi92.3
dc.identifier.percentilfiCiteScore91.00
dc.identifier.urihttps://repositorio.ipen.br/handle/123456789/48772
dc.identifier.vol177
dc.relation.ispartofBiomedicine and Pharmacotherapy
dc.rightsopenAccess
dc.titlePhotodynamic therapy offers a novel approach to managing miltefosine-resistant cutaneous leishmaniasis
dc.typeArtigo de periódico
dspace.entity.typePublication
ipen.autorFERNANDA VIANA CABRAL
ipen.autorMARTHA SIMOES RIBEIRO
ipen.codigoautor12732
ipen.codigoautor574
ipen.contributor.ipenauthorFERNANDA VIANA CABRAL
ipen.contributor.ipenauthorMARTHA SIMOES RIBEIRO
ipen.identifier.fi6.9
ipen.identifier.fiCiteScore11.9
ipen.identifier.ipendoc30826
ipen.identifier.iwosWoS
ipen.range.fi6.000 ou mais
ipen.range.percentilfi75.00 - 100.00
ipen.type.genreArtigo
relation.isAuthorOfPublication622f5d85-e9c4-40d7-a55f-873e2a346f55
relation.isAuthorOfPublication36215a53-0150-4910-91d7-9559717b62d7
relation.isAuthorOfPublication.latestForDiscovery622f5d85-e9c4-40d7-a55f-873e2a346f55
sigepi.autor.atividadeFERNANDA VIANA CABRAL:12732:920:S
sigepi.autor.atividadeMARTHA SIMOES RIBEIRO:574:920:N

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