Negatively charged AuNP modified with monoclonal antibody against novel tumor antigen FAT1 for tumor targeting

BACKGROUND: Herein, we demonstrated the use of a newly generated anti FAT1 antibody (clone mAB198.3) for intracellular delivery of anionic gold NPs, to form active targeting Au nanoparticles with high payload characteristics. METHODS: In vitro characterizations were determined by DLS, confocal micro...

Descripción completa

Detalles Bibliográficos
Autores principales: Fan, Li, Campagnoli, Susanna, Wu, Hong, Grandi, Alberto, Parri, Matteo, De Camilli, Elisa, Grandi, Guido, Viale, Giuseppe, Pileri, Piero, Grifantini, Renata, Song, Chaojun, Jin, Boquan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2015
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4570718/
https://www.ncbi.nlm.nih.gov/pubmed/26373379
http://dx.doi.org/10.1186/s13046-015-0214-x
_version_ 1782390251390500864
author Fan, Li
Campagnoli, Susanna
Wu, Hong
Grandi, Alberto
Parri, Matteo
De Camilli, Elisa
Grandi, Guido
Viale, Giuseppe
Pileri, Piero
Grifantini, Renata
Song, Chaojun
Jin, Boquan
author_facet Fan, Li
Campagnoli, Susanna
Wu, Hong
Grandi, Alberto
Parri, Matteo
De Camilli, Elisa
Grandi, Guido
Viale, Giuseppe
Pileri, Piero
Grifantini, Renata
Song, Chaojun
Jin, Boquan
author_sort Fan, Li
collection PubMed
description BACKGROUND: Herein, we demonstrated the use of a newly generated anti FAT1 antibody (clone mAB198.3) for intracellular delivery of anionic gold NPs, to form active targeting Au nanoparticles with high payload characteristics. METHODS: In vitro characterizations were determined by DLS, confocal microscopy, TEM, western blot, MALDI-TOF MS/MS analysis, MTT, ICP-MS and flow cytometry analysis. In vivo targeting efficacy was investigated by in vivo bio-imaging study and ICP-MS. RESULTS: The specificity of the FAT1 recognition in colon cancer was confirmed by pre-adsorbing mAb198.3, adsorption dramatically abolished the antibody reactivity on colon cancer, thus confirming the binding specificity. The DLS size distribution profile of the AuCOOH, AuCOOH(Cy5)_ mAb198.3, AuCOOH(Cy5)_isotype has showed that the modified gold nanoparticles are well dispersed in water, PBS buffer and cell culture medium with 10 % FBS. By TEM measurement, the size of Au nanoparticles with spherical morphology is about 10–20 nm. AuCOOH_198.3 NPs were stable in an acidic environment, as well as in PBS buffer, cell culture media and media with 10 % serum. MTT results revealed that Au nanoparticles have well biocompatibility. TEM results indicated that conjugation of mAb198.3 on Au nanoparticles can be an effective delivery vehicle for negatively charged gold nanoparticles and increased its intracellular transport. It was also demonstrated by confocal microscopy that AuCOOH(Cy5)_mAb198.3 could attach to the cell membrane in very short time, then gradually delivered into cells. After 4 h incubation, almost all AuCOOH(Cy5)_mAb198.3 have been uptaken into or surrounding the cytoplasm and nucleus. In vivo results showed that only about 20 % of AuCOOH accumulated in tumor site due to EPR effect, while nearly 90 % of AuCOOH_mAb198.3 was found in tumor, providing sufficient evidence for receptor-specific targeting by mAb198.3. CONCLUSION: According to in vitro and in vivo research results, the intracellular uptake of negatively charged AuCOOH_mAB198.3 particles is enhanced to a greater extent. Thus, AuCOOH_mAb198.3 holds significant potential to improve the treatment of cancer. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s13046-015-0214-x) contains supplementary material, which is available to authorized users.
format Online
Article
Text
id pubmed-4570718
institution National Center for Biotechnology Information
language English
publishDate 2015
publisher BioMed Central
record_format MEDLINE/PubMed
spelling pubmed-45707182015-09-16 Negatively charged AuNP modified with monoclonal antibody against novel tumor antigen FAT1 for tumor targeting Fan, Li Campagnoli, Susanna Wu, Hong Grandi, Alberto Parri, Matteo De Camilli, Elisa Grandi, Guido Viale, Giuseppe Pileri, Piero Grifantini, Renata Song, Chaojun Jin, Boquan J Exp Clin Cancer Res Research BACKGROUND: Herein, we demonstrated the use of a newly generated anti FAT1 antibody (clone mAB198.3) for intracellular delivery of anionic gold NPs, to form active targeting Au nanoparticles with high payload characteristics. METHODS: In vitro characterizations were determined by DLS, confocal microscopy, TEM, western blot, MALDI-TOF MS/MS analysis, MTT, ICP-MS and flow cytometry analysis. In vivo targeting efficacy was investigated by in vivo bio-imaging study and ICP-MS. RESULTS: The specificity of the FAT1 recognition in colon cancer was confirmed by pre-adsorbing mAb198.3, adsorption dramatically abolished the antibody reactivity on colon cancer, thus confirming the binding specificity. The DLS size distribution profile of the AuCOOH, AuCOOH(Cy5)_ mAb198.3, AuCOOH(Cy5)_isotype has showed that the modified gold nanoparticles are well dispersed in water, PBS buffer and cell culture medium with 10 % FBS. By TEM measurement, the size of Au nanoparticles with spherical morphology is about 10–20 nm. AuCOOH_198.3 NPs were stable in an acidic environment, as well as in PBS buffer, cell culture media and media with 10 % serum. MTT results revealed that Au nanoparticles have well biocompatibility. TEM results indicated that conjugation of mAb198.3 on Au nanoparticles can be an effective delivery vehicle for negatively charged gold nanoparticles and increased its intracellular transport. It was also demonstrated by confocal microscopy that AuCOOH(Cy5)_mAb198.3 could attach to the cell membrane in very short time, then gradually delivered into cells. After 4 h incubation, almost all AuCOOH(Cy5)_mAb198.3 have been uptaken into or surrounding the cytoplasm and nucleus. In vivo results showed that only about 20 % of AuCOOH accumulated in tumor site due to EPR effect, while nearly 90 % of AuCOOH_mAb198.3 was found in tumor, providing sufficient evidence for receptor-specific targeting by mAb198.3. CONCLUSION: According to in vitro and in vivo research results, the intracellular uptake of negatively charged AuCOOH_mAB198.3 particles is enhanced to a greater extent. Thus, AuCOOH_mAb198.3 holds significant potential to improve the treatment of cancer. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (doi:10.1186/s13046-015-0214-x) contains supplementary material, which is available to authorized users. BioMed Central 2015-09-15 /pmc/articles/PMC4570718/ /pubmed/26373379 http://dx.doi.org/10.1186/s13046-015-0214-x Text en © Fan et al. 2015 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Fan, Li
Campagnoli, Susanna
Wu, Hong
Grandi, Alberto
Parri, Matteo
De Camilli, Elisa
Grandi, Guido
Viale, Giuseppe
Pileri, Piero
Grifantini, Renata
Song, Chaojun
Jin, Boquan
Negatively charged AuNP modified with monoclonal antibody against novel tumor antigen FAT1 for tumor targeting
title Negatively charged AuNP modified with monoclonal antibody against novel tumor antigen FAT1 for tumor targeting
title_full Negatively charged AuNP modified with monoclonal antibody against novel tumor antigen FAT1 for tumor targeting
title_fullStr Negatively charged AuNP modified with monoclonal antibody against novel tumor antigen FAT1 for tumor targeting
title_full_unstemmed Negatively charged AuNP modified with monoclonal antibody against novel tumor antigen FAT1 for tumor targeting
title_short Negatively charged AuNP modified with monoclonal antibody against novel tumor antigen FAT1 for tumor targeting
title_sort negatively charged aunp modified with monoclonal antibody against novel tumor antigen fat1 for tumor targeting
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4570718/
https://www.ncbi.nlm.nih.gov/pubmed/26373379
http://dx.doi.org/10.1186/s13046-015-0214-x
work_keys_str_mv AT fanli negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting
AT campagnolisusanna negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting
AT wuhong negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting
AT grandialberto negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting
AT parrimatteo negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting
AT decamillielisa negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting
AT grandiguido negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting
AT vialegiuseppe negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting
AT pileripiero negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting
AT grifantinirenata negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting
AT songchaojun negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting
AT jinboquan negativelychargedaunpmodifiedwithmonoclonalantibodyagainstnoveltumorantigenfat1fortumortargeting

Ejemplares similares