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Title:In vitro functional validation of an anti-FREM2 nanobody for glioblastoma cell targeting
Authors:ID Krapež, Gloria (Author)
ID Šamec, Neja (Author)
ID Zottel, Alja (Author)
ID Katrašnik, Mojca (Author)
ID Kump, Ana (Author)
ID Šribar, Jernej (Author)
ID Križaj, Igor (Author)
ID Stojan, Jure (Author)
ID Romih, Rok (Author)
ID Bajc, Gregor (Author)
ID Butala, Matej (Author)
ID Muyldermans, Serge (Author)
ID Jovchevska, Ivana (Author)
Files:.pdf PDF - Presentation file, download (23,98 MB)
MD5: FE32B13E77C5359E862E2F83D949ADC7
 
URL URL - Source URL, visit https://www.mdpi.com/2073-4468/14/1/8
 
Language:English
Typology:1.01 - Original Scientific Article
Organization:Logo UKC LJ - Ljubljana University Medical Centre
Abstract:Background/Objectives: Glioblastomas are the most common brain malignancies. Despite the implementation of multimodal therapy, patient life expectancy after diagnosis is barely 12 to 18 months. Glioblastomas are highly heterogeneous at the genetic and epigenetic level and comprise multiple different cell subpopulations. Therefore, small molecules such as nanobodies, able to target membrane proteins specific to glioblastoma cells or specific cell types within the tumor are being investigated as novel tools to treat glioblastomas. Methods: Here, we describe the identification of such a nanobody and its in silico and in vitro validation. NB3F18, as we named it, is directed against the membrane-associated protein FREM2, overexpressed in glioblastoma stem cells. Results: Three dimensional in silico modeling indicated that NB3F18 and FREM2 form a stable complex. Surface plasmon resonance confirmed their interaction with moderate affinity. As we demonstrated by flow cytometry, NB3F18 binds to glioblastoma stem cells to a greater extent than to differentiated glioblastoma cells and astrocytes. Immunocytochemistry revealed surface localization of NB3F18 on glioblastoma stem cells, whereas cytoplasmic localization of NB3F18 was observed in other cell lines. NB3F18 was detected by transmission electron microscopy on the plasma membrane and in various compartments of the endocytic pathway, from endocytic vesicles to multivesicular bodies (endosomes) and lysosomes. Interestingly, NB3F18 was cytotoxic to glioblastoma stem cells. Conclusions: Collectively, NB3F18 has been qualified as an interesting tool to target glioblastoma cells and as a potential vehicle to deliver biological or pharmaceutical agents to these cells.
Keywords:brain cancer, membrane-bound protein, cytotoxicity, molecular tool, subcellular localization
Publication status:Published
Publication version:Version of Record
Year of publishing:2025
Number of pages:str. 1-30
Numbering:Vol. 14, iss. 1 [article no.] 8
PID:20.500.12556/DiRROS-28844 New window
UDC:577.2
ISSN on article:2073-4468
DOI:10.3390/antib14010008 New window
COBISS.SI-ID:225693187 New window
Note:Nasl. z nasl. zaslona; Opis vira z dne 10. 2. 2025;
Publication date in DiRROS:09.04.2026
Views:189
Downloads:119
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Record is a part of a journal

Title:Antibodies
Shortened title:Antibodies
Publisher:MDPI
ISSN:2073-4468
COBISS.SI-ID:3289339 New window

Document is financed by a project

Funder:ARIS - Slovenian Research and Innovation Agency
Project number:Z3-1869-2019
Name:Razvoj anti-FREM2 nanotelesa in njegova uporaba pri ciljanju glioblastomskih celic.

Funder:ARIS - Slovenian Research and Innovation Agency
Project number:P1-0207-2020
Name:Toksini in biomembrane

Funder:ARIS - Slovenian Research and Innovation Agency
Project number:P3-0108-2018
Name:Celična biologija in molekularna genetika v biomedicini

Funder:ARIS - Slovenian Research and Innovation Agency
Project number:P1-0390-2015
Name:Funkcijska genomika in biotehnologija za zdravje

Funder:Other - Other funder or multiple funders
Project number:I0- 0022
Name:Mreža raziskovalnih infrastrukturnih centrov Univerze v Ljubljani (MRIC UL)
Acronym:MRIC UL

Licences

License:CC BY 4.0, Creative Commons Attribution 4.0 International
Link:http://creativecommons.org/licenses/by/4.0/
Description:This is the standard Creative Commons license that gives others maximum freedom to do what they want with the work as long as they credit the author.

Secondary language

Language:Slovenian
Keywords:možganski rak, membransko vezan protein, citotoksičnost, molekularno orodje, subcelična lokalizacija


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