Peptide Anchor for Folate-Targeted Liposomal Delivery

Eugénia Nogueira; Irene C. Mangialavori; Ana Loureiro; Nuno G. Azoia; Marisa P. Sárria; Patrícia Nogueira; Jaime Freitas; Johan Härmark; Ulyana Shimanovich; Alexandra Rollett; Ghislaine Lacroix; Gonçalo J.L. Bernardes; Georg Guebitz; Hans Hebert; Alexandra Moreira; Alexandre M. Carmo; Juan Pablo F.C. Rossi; Andreia C. Gomes; Ana Preto; Artur Cavaco-Paulo; Johan Harmark

doi:10.1021/acs.biomac.5b00823

Peptide Anchor for Folate-Targeted Liposomal Delivery

Eugénia Nogueira, Irene C. Mangialavori, Ana Loureiro, Nuno G. Azoia, Marisa P. Sárria, Patrícia Nogueira, Jaime Freitas, Johan Härmark, Ulyana Shimanovich, Alexandra Rollett, Ghislaine Lacroix, Gonçalo J.L. Bernardes, Georg Guebitz, Hans Hebert, Alexandra Moreira, Alexandre M. Carmo, Juan Pablo F.C. Rossi, Andreia C. Gomes, Ana Preto, Artur Cavaco-PauloJohan Harmark

Research output: Contribution to journal › Article › peer-review

Abstract

Specific folate receptors are abundantly overexpressed in chronically activated macrophages and in most cancer cells. Directed folate receptor targeting using liposomes is usually achieved using folate linked to a phospholipid or cholesterol anchor. This link is formed using a large spacer like polyethylene glycol. Here, we report an innovative strategy for targeted liposome delivery that uses a hydrophobic fragment of surfactant protein D linked to folate. Our proposed spacer is a small 4 amino acid residue linker. The peptide conjugate inserts deeply into the lipid bilayer without affecting liposomal integrity, with high stability and specificity. To compare the drug delivery potential of both liposomal targeting systems, we encapsulated the nuclear dye Hoechst 34580. The eventual increase in blue fluorescence would only be detectable upon liposome disruption, leading to specific binding of this dye to DNA. Our delivery system was proven to be more efficient (2-fold) in Caco-2 cells than classic systems where the folate moiety is linked to liposomes by polyethylene glycol.

Original language	English
Pages (from-to)	2904-2910
Number of pages	7
Journal	Biomacromolecules
Volume	16
Issue number	9
DOIs	https://doi.org/10.1021/acs.biomac.5b00823
State	Published - 14 Sep 2015
Externally published	Yes

All Science Journal Classification (ASJC) codes

Bioengineering
Biomaterials
Polymers and Plastics
Materials Chemistry

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1021/acs.biomac.5b00823

Cite this

Nogueira, E., Mangialavori, I. C., Loureiro, A., Azoia, N. G., Sárria, M. P., Nogueira, P., Freitas, J., Härmark, J., Shimanovich, U., Rollett, A., Lacroix, G., Bernardes, G. J. L., Guebitz, G., Hebert, H., Moreira, A., Carmo, A. M., Rossi, J. P. F. C., Gomes, A. C., Preto, A., ... Harmark, J. (2015). Peptide Anchor for Folate-Targeted Liposomal Delivery. Biomacromolecules, 16(9), 2904-2910. https://doi.org/10.1021/acs.biomac.5b00823

@article{1766fb28a20f48b39bcd5b2612ae6197,

title = "Peptide Anchor for Folate-Targeted Liposomal Delivery",

abstract = "Specific folate receptors are abundantly overexpressed in chronically activated macrophages and in most cancer cells. Directed folate receptor targeting using liposomes is usually achieved using folate linked to a phospholipid or cholesterol anchor. This link is formed using a large spacer like polyethylene glycol. Here, we report an innovative strategy for targeted liposome delivery that uses a hydrophobic fragment of surfactant protein D linked to folate. Our proposed spacer is a small 4 amino acid residue linker. The peptide conjugate inserts deeply into the lipid bilayer without affecting liposomal integrity, with high stability and specificity. To compare the drug delivery potential of both liposomal targeting systems, we encapsulated the nuclear dye Hoechst 34580. The eventual increase in blue fluorescence would only be detectable upon liposome disruption, leading to specific binding of this dye to DNA. Our delivery system was proven to be more efficient (2-fold) in Caco-2 cells than classic systems where the folate moiety is linked to liposomes by polyethylene glycol.",

author = "Eug{\'e}nia Nogueira and Mangialavori, \{Irene C.\} and Ana Loureiro and Azoia, \{Nuno G.\} and S{\'a}rria, \{Marisa P.\} and Patr{\'i}cia Nogueira and Jaime Freitas and Johan H{\"a}rmark and Ulyana Shimanovich and Alexandra Rollett and Ghislaine Lacroix and Bernardes, \{Gon{\c c}alo J.L.\} and Georg Guebitz and Hans Hebert and Alexandra Moreira and Carmo, \{Alexandre M.\} and Rossi, \{Juan Pablo F.C.\} and Gomes, \{Andreia C.\} and Ana Preto and Artur Cavaco-Paulo and Johan Harmark",

note = "Publisher Copyright: {\textcopyright} 2015 American Chemical Society.",

year = "2015",

month = sep,

day = "14",

doi = "10.1021/acs.biomac.5b00823",

language = "الإنجليزيّة",

volume = "16",

pages = "2904--2910",

journal = "Biomacromolecules",

issn = "1525-7797",

publisher = "American Chemical Society",

number = "9",

}

Nogueira, E, Mangialavori, IC, Loureiro, A, Azoia, NG, Sárria, MP, Nogueira, P, Freitas, J, Härmark, J, Shimanovich, U, Rollett, A, Lacroix, G, Bernardes, GJL, Guebitz, G, Hebert, H, Moreira, A, Carmo, AM, Rossi, JPFC, Gomes, AC, Preto, A, Cavaco-Paulo, A & Harmark, J 2015, 'Peptide Anchor for Folate-Targeted Liposomal Delivery', Biomacromolecules, vol. 16, no. 9, pp. 2904-2910. https://doi.org/10.1021/acs.biomac.5b00823

TY - JOUR

T1 - Peptide Anchor for Folate-Targeted Liposomal Delivery

AU - Nogueira, Eugénia

AU - Mangialavori, Irene C.

AU - Loureiro, Ana

AU - Azoia, Nuno G.

AU - Sárria, Marisa P.

AU - Nogueira, Patrícia

AU - Freitas, Jaime

AU - Härmark, Johan

AU - Shimanovich, Ulyana

AU - Rollett, Alexandra

AU - Lacroix, Ghislaine

AU - Bernardes, Gonçalo J.L.

AU - Guebitz, Georg

AU - Hebert, Hans

AU - Moreira, Alexandra

AU - Carmo, Alexandre M.

AU - Rossi, Juan Pablo F.C.

AU - Gomes, Andreia C.

AU - Preto, Ana

AU - Cavaco-Paulo, Artur

AU - Harmark, Johan

PY - 2015/9/14

Y1 - 2015/9/14

N2 - Specific folate receptors are abundantly overexpressed in chronically activated macrophages and in most cancer cells. Directed folate receptor targeting using liposomes is usually achieved using folate linked to a phospholipid or cholesterol anchor. This link is formed using a large spacer like polyethylene glycol. Here, we report an innovative strategy for targeted liposome delivery that uses a hydrophobic fragment of surfactant protein D linked to folate. Our proposed spacer is a small 4 amino acid residue linker. The peptide conjugate inserts deeply into the lipid bilayer without affecting liposomal integrity, with high stability and specificity. To compare the drug delivery potential of both liposomal targeting systems, we encapsulated the nuclear dye Hoechst 34580. The eventual increase in blue fluorescence would only be detectable upon liposome disruption, leading to specific binding of this dye to DNA. Our delivery system was proven to be more efficient (2-fold) in Caco-2 cells than classic systems where the folate moiety is linked to liposomes by polyethylene glycol.

AB - Specific folate receptors are abundantly overexpressed in chronically activated macrophages and in most cancer cells. Directed folate receptor targeting using liposomes is usually achieved using folate linked to a phospholipid or cholesterol anchor. This link is formed using a large spacer like polyethylene glycol. Here, we report an innovative strategy for targeted liposome delivery that uses a hydrophobic fragment of surfactant protein D linked to folate. Our proposed spacer is a small 4 amino acid residue linker. The peptide conjugate inserts deeply into the lipid bilayer without affecting liposomal integrity, with high stability and specificity. To compare the drug delivery potential of both liposomal targeting systems, we encapsulated the nuclear dye Hoechst 34580. The eventual increase in blue fluorescence would only be detectable upon liposome disruption, leading to specific binding of this dye to DNA. Our delivery system was proven to be more efficient (2-fold) in Caco-2 cells than classic systems where the folate moiety is linked to liposomes by polyethylene glycol.

UR - http://www.scopus.com/inward/record.url?scp=84941584525&partnerID=8YFLogxK

U2 - 10.1021/acs.biomac.5b00823

DO - 10.1021/acs.biomac.5b00823

M3 - مقالة

C2 - 26241560

SN - 1525-7797

VL - 16

SP - 2904

EP - 2910

JO - Biomacromolecules

JF - Biomacromolecules

IS - 9

ER -

Peptide Anchor for Folate-Targeted Liposomal Delivery

Abstract

All Science Journal Classification (ASJC) codes

UN SDGs

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