Dendrimers Improve Apolipoprotein Nanoparticle mRNA Delivery to Immune Cells

Mirre M. Trines; Daniek Hoorn; Stijn R.J. Hofstraat; Robby C. Zwolsman; Tom Anbergen; Iris Versteeg; Yuri van Elsas; Jeroen Deckers; Merel M.A. Hendrikx; Teun Kleuskens; Youssef B. Darwish; Gijs W.B. Ros; Sjoerd F. Dijkstra; Bram Priem; Matt Timmers; P. Michel Fransen; Maarten J. Pouderoijen; Bas F.M. de Waal; E.W. Meijer; Thijs J. Beldman; Yohana C. Toner; Ewelina Kluza; Willem J.M. Mulder; Henk M. Janssen; Roy van der Meel

doi:10.1002/adma.202504830

Dendrimers Improve Apolipoprotein Nanoparticle mRNA Delivery to Immune Cells

Mirre M. Trines
, Daniek Hoorn
, Stijn R.J. Hofstraat
, Robby C. Zwolsman
, Tom Anbergen
, Iris Versteeg
, Yuri van Elsas
, Jeroen Deckers
, Merel M.A. Hendrikx
, Teun Kleuskens
, Youssef B. Darwish
, Gijs W.B. Ros
, Sjoerd F. Dijkstra
, Bram Priem
, Matt Timmers
, P. Michel Fransen
, Maarten J. Pouderoijen
, Bas F.M. de Waal
, E.W. Meijer
, Thijs J. Beldman

Yohana C. Toner, Ewelina Kluza, Willem J.M. Mulder, Henk M. Janssen (Corresponding author), Roy van der Meel (Corresponding author)

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

1 Citation (Scopus)

Abstract

Employing messenger RNA (mRNA) for protein production in the liver or for vaccine purposes is a promising therapeutic approach. However, unlocking mRNA's full therapeutic potential requires systemic delivery platform technology with controllable biodistribution features. Apolipoprotein nanoparticles (aNP) containing monovalent ionizable cationic lipids have been shown to functionally deliver mRNA to myeloid progenitor cells in the bone marrow after intravenous administration. Here, the development of polyvalent ionizable cationic dendrimers is reported for incorporation in aNPs to enable efficient mRNA complexation and functional delivery. A library of dendrimers is first rationally designed with diverse hydrophobic core units, a number of branching units, and functionalized terminal units. Upon incorporation, eleven distinct dendrimer-based aNP-mRNA formulations are screened and characterized in vitro for their properties. Based on the screening outcome, four formulations are selected and evaluated their ability to induce functional gene expression in vivo. The results indicate that the lead polyvalent dendrimer-based aNP formulation outperformed formulations containing a clinically approved ionizable cationic lipid regarding gene expression in hematopoietic stem and progenitor cells in the bone marrow after intravenous administration.

Original language	English
Article number	e04830
Number of pages	11
Journal	Advanced Materials
Volume	38
Issue number	3
Early online date	12 Sept 2025
DOIs	https://doi.org/10.1002/adma.202504830
Publication status	Published - 13 Jan 2026

Bibliographical note

Funding

M.M.T., D.H., and S.R.J.H. contributed equally to this work. Research reported in this publication was supported by a Dutch Research Council (NWO) Vidi grant (no. 19681) to R.v.d.M., and an NWO Vici grant (no. 91818622) and the ERC Advanced grant (no. 101019807) to W.J.M.M.

Funders	Funder number
Nederlandse Organisatie voor Wetenschappelijk Onderzoek	19681, 91818622

Keywords

ionizable cationic lipids
dendrimers
apolipoprotein nanoparticles
mRNA delivery

UN SDGs

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

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Trines, M. M., Hoorn, D., Hofstraat, S. R. J., Zwolsman, R. C., Anbergen, T., Versteeg, I., van Elsas, Y., Deckers, J., Hendrikx, M. M. A., Kleuskens, T., Darwish, Y. B., Ros, G. W. B., Dijkstra, S. F., Priem, B., Timmers, M., Fransen, P. M., Pouderoijen, M. J., de Waal, B. F. M., Meijer, E. W., ... van der Meel, R. (2026). Dendrimers Improve Apolipoprotein Nanoparticle mRNA Delivery to Immune Cells. Advanced Materials, 38(3), Article e04830. https://doi.org/10.1002/adma.202504830

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title = "Dendrimers Improve Apolipoprotein Nanoparticle mRNA Delivery to Immune Cells",

abstract = "Employing messenger RNA (mRNA) for protein production in the liver or for vaccine purposes is a promising therapeutic approach. However, unlocking mRNA's full therapeutic potential requires systemic delivery platform technology with controllable biodistribution features. Apolipoprotein nanoparticles (aNP) containing monovalent ionizable cationic lipids have been shown to functionally deliver mRNA to myeloid progenitor cells in the bone marrow after intravenous administration. Here, the development of polyvalent ionizable cationic dendrimers is reported for incorporation in aNPs to enable efficient mRNA complexation and functional delivery. A library of dendrimers is first rationally designed with diverse hydrophobic core units, a number of branching units, and functionalized terminal units. Upon incorporation, eleven distinct dendrimer-based aNP-mRNA formulations are screened and characterized in vitro for their properties. Based on the screening outcome, four formulations are selected and evaluated their ability to induce functional gene expression in vivo. The results indicate that the lead polyvalent dendrimer-based aNP formulation outperformed formulations containing a clinically approved ionizable cationic lipid regarding gene expression in hematopoietic stem and progenitor cells in the bone marrow after intravenous administration.",

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doi = "10.1002/adma.202504830",

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Trines, MM , Hoorn, D , Hofstraat, SRJ, Zwolsman, RC, Anbergen, T, Versteeg, I, van Elsas, Y, Deckers, J, Hendrikx, MMA, Kleuskens, T, Darwish, YB, Ros, GWB, Dijkstra, SF, Priem, B, Timmers, M , Fransen, PM , Pouderoijen, MJ, de Waal, BFM, Meijer, EW, Beldman, TJ, Toner, YC, Kluza, E , Mulder, WJM, Janssen, HM & van der Meel, R 2026, 'Dendrimers Improve Apolipoprotein Nanoparticle mRNA Delivery to Immune Cells', Advanced Materials, vol. 38, no. 3, e04830. https://doi.org/10.1002/adma.202504830

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AU - Trines, Mirre M.

AU - Hoorn, Daniek

AU - Hofstraat, Stijn R.J.

AU - Zwolsman, Robby C.

AU - Anbergen, Tom

AU - Versteeg, Iris

AU - van Elsas, Yuri

AU - Deckers, Jeroen

AU - Hendrikx, Merel M.A.

AU - Kleuskens, Teun

AU - Darwish, Youssef B.

AU - Ros, Gijs W.B.

AU - Dijkstra, Sjoerd F.

AU - Priem, Bram

AU - Timmers, Matt

AU - Fransen, P. Michel

AU - Pouderoijen, Maarten J.

AU - de Waal, Bas F.M.

AU - Meijer, E.W.

AU - Beldman, Thijs J.

AU - Toner, Yohana C.

AU - Kluza, Ewelina

AU - Mulder, Willem J.M.

AU - Janssen, Henk M.

AU - van der Meel, Roy

PY - 2026/1/13

Y1 - 2026/1/13

N2 - Employing messenger RNA (mRNA) for protein production in the liver or for vaccine purposes is a promising therapeutic approach. However, unlocking mRNA's full therapeutic potential requires systemic delivery platform technology with controllable biodistribution features. Apolipoprotein nanoparticles (aNP) containing monovalent ionizable cationic lipids have been shown to functionally deliver mRNA to myeloid progenitor cells in the bone marrow after intravenous administration. Here, the development of polyvalent ionizable cationic dendrimers is reported for incorporation in aNPs to enable efficient mRNA complexation and functional delivery. A library of dendrimers is first rationally designed with diverse hydrophobic core units, a number of branching units, and functionalized terminal units. Upon incorporation, eleven distinct dendrimer-based aNP-mRNA formulations are screened and characterized in vitro for their properties. Based on the screening outcome, four formulations are selected and evaluated their ability to induce functional gene expression in vivo. The results indicate that the lead polyvalent dendrimer-based aNP formulation outperformed formulations containing a clinically approved ionizable cationic lipid regarding gene expression in hematopoietic stem and progenitor cells in the bone marrow after intravenous administration.

AB - Employing messenger RNA (mRNA) for protein production in the liver or for vaccine purposes is a promising therapeutic approach. However, unlocking mRNA's full therapeutic potential requires systemic delivery platform technology with controllable biodistribution features. Apolipoprotein nanoparticles (aNP) containing monovalent ionizable cationic lipids have been shown to functionally deliver mRNA to myeloid progenitor cells in the bone marrow after intravenous administration. Here, the development of polyvalent ionizable cationic dendrimers is reported for incorporation in aNPs to enable efficient mRNA complexation and functional delivery. A library of dendrimers is first rationally designed with diverse hydrophobic core units, a number of branching units, and functionalized terminal units. Upon incorporation, eleven distinct dendrimer-based aNP-mRNA formulations are screened and characterized in vitro for their properties. Based on the screening outcome, four formulations are selected and evaluated their ability to induce functional gene expression in vivo. The results indicate that the lead polyvalent dendrimer-based aNP formulation outperformed formulations containing a clinically approved ionizable cationic lipid regarding gene expression in hematopoietic stem and progenitor cells in the bone marrow after intravenous administration.

KW - ionizable cationic lipids

KW - dendrimers

KW - apolipoprotein nanoparticles

KW - mRNA delivery

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DO - 10.1002/adma.202504830

M3 - Article

C2 - 40937965

SN - 0935-9648

VL - 38

JO - Advanced Materials

JF - Advanced Materials

IS - 3

M1 - e04830

ER -

Dendrimers Improve Apolipoprotein Nanoparticle mRNA Delivery to Immune Cells

Abstract

Bibliographical note

Funding

Keywords

UN SDGs

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