Investigation of antitumor activity of modified citrus pectin

SILVA, FABIO F. A. da; SANTOS, SOFIA N. dos; PEDROSA, LUCAS de F.; RODRIGUES, VINICIUS G.; PEREIRA, JONATHAS X.; PEREIRA, JHONATAS P. M.; GUSHIKEN JUNIOR, DINO S.; ROSALES, THIECLA K. O.; DIAS, LUIS A. P.; SPENCER, PATRICK J.; FABI, JOAO P.; BERNARDES, EMERSON S.

doi:10.1021/acs.biomac.5c00915

Investigation of antitumor activity of modified citrus pectin

dc.contributor.author	SILVA, FABIO F. A. da
dc.contributor.author	SANTOS, SOFIA N. dos
dc.contributor.author	PEDROSA, LUCAS de F.
dc.contributor.author	RODRIGUES, VINICIUS G.
dc.contributor.author	PEREIRA, JONATHAS X.
dc.contributor.author	PEREIRA, JHONATAS P. M.
dc.contributor.author	GUSHIKEN JUNIOR, DINO S.
dc.contributor.author	ROSALES, THIECLA K. O.
dc.contributor.author	DIAS, LUIS A. P.
dc.contributor.author	SPENCER, PATRICK J.
dc.contributor.author	FABI, JOAO P.
dc.contributor.author	BERNARDES, EMERSON S.
dc.coverage	Internacional
dc.date.accessioned	2026-06-16T12:44:23Z
dc.date.available	2026-06-16T12:44:23Z
dc.date.issued	2026
dc.description.abstract	This study employed molecular imaging to evaluate MCP (PectaSol-C, modified citrus pectin, a complex polysaccharide with antitumor potential) absorption and pharmacokinetics following oral and intravenous (IV) administration. MCP was radiolabeled with technetium-99m (99mTc) ([99mTc]MCP), allowing precise in vivo tracking. Imaging and biodistribution analyzes revealed low tumor uptake of IV [99mTc]MCP, with predominant renal and hepatobiliary clearance. Within tumors, MCP was detected at low levels and did not bind to viable cells. Consistent with these findings, IV administration produced only modest antitumor effects (∼50% tumor growth reduction) in SKOV-3 (ovarian), MKN45 (gastric), and 4T1 (breast) grafts, whereas oral administration was ineffective due to extremely poor absorption (bioavailability <0.01%). Notably, faster clearance of [99mTc]MCP in galectin-3 (Gal-3) knockout mice suggests a role for Gal-3 in systemic retention or an indirect contribution to antitumor activity. These findings provide new insights into MCP pharmacological profile, highlight the limitations of oral delivery, and underscore the need for improved delivery strategies to enhance the therapeutic potential of pectin-based cancer treatments.
dc.description.sponsorship	Conselho Nacional de Desenvolvimento Científico e Tecnológico (CNPq)
dc.description.sponsorship	Fundação de Amparo à Pesquisa do Estado de São Paulo (FAPESP)
dc.description.sponsorshipID	CNPq: 307842/2022-3
dc.description.sponsorshipID	FAPESP: 13/07914-8; 22/12834-2; 21/10265-8; 25/26469-2
dc.format.extent	2449-2465
dc.identifier.citation	SILVA, FABIO F. A. da; SANTOS, SOFIA N. dos; PEDROSA, LUCAS de F.; RODRIGUES, VINICIUS G.; PEREIRA, JONATHAS X.; PEREIRA, JHONATAS P. M.; GUSHIKEN JUNIOR, DINO S.; ROSALES, THIECLA K. O.; DIAS, LUIS A. P.; SPENCER, PATRICK J.; FABI, JOAO P.; BERNARDES, EMERSON S. Investigation of antitumor activity of modified citrus pectin: oral and intravenous administration assessed via molecular imaging. <b>Biomacromolecules</b>, v. 27, n. 4, p. 2449-2465, 2026. DOI: <a href="https://dx.doi.org/10.1021/acs.biomac.5c00915">10.1021/acs.biomac.5c00915</a>. Disponível em: https://repositorio.ipen.br/handle/123456789/49978.
dc.identifier.doi	10.1021/acs.biomac.5c00915
dc.identifier.fasciculo	4
dc.identifier.issn	1525-7797
dc.identifier.orcid	https://orcid.org/0000-0001-8949-7735
dc.identifier.orcid	https://orcid.org/0000-0002-0029-7313
dc.identifier.percentilfi	87.8
dc.identifier.percentilfiCiteScore	76.50
dc.identifier.uri	https://repositorio.ipen.br/handle/123456789/49978
dc.identifier.vol	27
dc.language.iso	eng
dc.relation.ispartof	Biomacromolecules
dc.rights	openAccess
dc.title	Investigation of antitumor activity of modified citrus pectin
dc.type	Artigo de periódico
dspace.entity.type	Publication
ipen.autor	FABIO FERNANDO ALVES DA SILVA
ipen.autor	JHONATAS PEDROSA MARIM PEREIRA
ipen.autor	DINO SEIGO GUSHIKEN JUNIOR
ipen.autor	LUIS ALBERTO PEREIRA DIAS
ipen.autor	PATRICK JACK SPENCER
ipen.autor	EMERSON SOARES BERNARDES
ipen.codigoautor	15003
ipen.codigoautor	15034
ipen.codigoautor	15448
ipen.codigoautor	796
ipen.codigoautor	910
ipen.codigoautor	12099
ipen.contributor.ipenauthor	FABIO FERNANDO ALVES DA SILVA
ipen.contributor.ipenauthor	JHONATAS PEDROSA MARIM PEREIRA
ipen.contributor.ipenauthor	DINO SEIGO GUSHIKEN JUNIOR
ipen.contributor.ipenauthor	LUIS ALBERTO PEREIRA DIAS
ipen.contributor.ipenauthor	PATRICK JACK SPENCER
ipen.contributor.ipenauthor	EMERSON SOARES BERNARDES
ipen.identifier.fi	5.4
ipen.identifier.fiCiteScore	8.8
ipen.identifier.ipendoc	32028
ipen.identifier.iwos	WoS
ipen.range.fi	4.500 - 5.999
ipen.range.percentilfi	75.00 - 100.00
ipen.subtitulo	oral and intravenous administration assessed via molecular imaging
ipen.type.genre	Artigo
relation.isAuthorOfPublication	b51bcd24-7448-4b37-a79f-30d59d968a88
relation.isAuthorOfPublication	73a6c0f6-9570-4008-85cc-10096512ac59
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relation.isAuthorOfPublication	50b3adab-a651-4225-a05c-ec1b1e37e921
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relation.isAuthorOfPublication	8115c8bd-822c-4f5a-9f49-3c12570ed40a
relation.isAuthorOfPublication.latestForDiscovery	b51bcd24-7448-4b37-a79f-30d59d968a88
sigepi.autor.atividade	FABIO FERNANDO ALVES DA SILVA:15003:110:S
sigepi.autor.atividade	JHONATAS PEDROSA MARIM PEREIRA:15034:110:N
sigepi.autor.atividade	DINO SEIGO GUSHIKEN JUNIOR:15448:-1:N
sigepi.autor.atividade	LUIS ALBERTO PEREIRA DIAS:796:120:N
sigepi.autor.atividade	PATRICK JACK SPENCER:910:830:N
sigepi.autor.atividade	EMERSON SOARES BERNARDES:12099:110:N

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