Personalization of Complex Vaginal Inserts of Ethylene Vinyl Acetate via 3D-Printing

Publikationen: Beitrag in FachzeitschriftArtikelForschung(peer-reviewed)

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Personalization of Complex Vaginal Inserts of Ethylene Vinyl Acetate via 3D-Printing. / Eder, Simone; Kuchler, Lisa; Katschnig, Matthias et al.
in: Advanced Materials Technologies, Jahrgang 8.2023, Nr. 17, 2300237, 13.07.2023.

Publikationen: Beitrag in FachzeitschriftArtikelForschung(peer-reviewed)

Harvard

Eder, S, Kuchler, L, Katschnig, M, Brandl, B, Wolfgang, M, Koutsamanis, I, Hentschel, L, Arbeiter, F, Roblegg, E & Spoerk, M 2023, 'Personalization of Complex Vaginal Inserts of Ethylene Vinyl Acetate via 3D-Printing', Advanced Materials Technologies, Jg. 8.2023, Nr. 17, 2300237. https://doi.org/10.1002/admt.202300237

APA

Eder, S., Kuchler, L., Katschnig, M., Brandl, B., Wolfgang, M., Koutsamanis, I., Hentschel, L., Arbeiter, F., Roblegg, E., & Spoerk, M. (2023). Personalization of Complex Vaginal Inserts of Ethylene Vinyl Acetate via 3D-Printing. Advanced Materials Technologies, 8.2023(17), Artikel 2300237. https://doi.org/10.1002/admt.202300237

Vancouver

Eder S, Kuchler L, Katschnig M, Brandl B, Wolfgang M, Koutsamanis I et al. Personalization of Complex Vaginal Inserts of Ethylene Vinyl Acetate via 3D-Printing. Advanced Materials Technologies. 2023 Jul 13;8.2023(17):2300237. doi: 10.1002/admt.202300237

Author

Eder, Simone ; Kuchler, Lisa ; Katschnig, Matthias et al. / Personalization of Complex Vaginal Inserts of Ethylene Vinyl Acetate via 3D-Printing. in: Advanced Materials Technologies. 2023 ; Jahrgang 8.2023, Nr. 17.

Bibtex - Download

@article{f3eeaa28c8e243b68e5f4be88fc699e3,
title = "Personalization of Complex Vaginal Inserts of Ethylene Vinyl Acetate via 3D-Printing",
abstract = "Ethylene vinyl acetate (EVA) with a vinyl acetate (VA) content of 28 wt.%(EVA28) is frequently used in vaginal inserts and subcutaneous implants dueto its biocompatibility and drug-releasing properties. Traditionally beingprocessed via hot melt extrusion, its processibility via filament-based3D-printing was reported to be impossible. Consequently, no applicablecustomization concepts for vaginal inserts exist. For the first time, thefabrication of 3D-printed vaginal inserts (urethra pessaries) of EVA28 isdemonstrated by optimizing its viscosity, employing 3D-printer adaptations,and carefully selecting printing parameters. The infill pattern of fully filledmono-material pessaries (determining the number and orientation of weldlines) significantly affects the in vitro release of the model drug progesterone(P4), while other critical parameters (the pessary{\textquoteright}s mechanical properties andappearance) remain unaffected. Weld lines act as diffusion barriers fordissolved P4 molecules. Hence, a high number of weld lines to be crossedreduces the overall P4 diffusivity in EVA28, decreasing the P4 release rate. Tofurther control the P4 release, innovative multi-material pessary designs(additionally comprising EVA with a VA content of 9 wt.% that is also used invaginal inserts) allow to tailor the in vitro drug release and the mechanicsindividually. Thereby, this work highly improves the mechanisticunderstanding on drug release modifications from 3D-printednon-biodegradable devices. The findings build the basis for the firstapplication of customized vaginal inserts, as they are based on polymers usedin corresponding marketed products for more than 20 years.",
keywords = "3D-printing, drug releases, ethylene vinyl acetate, EVA, extrusion-based additive manufacturing, fused deposition modeling, fused filament fabrications, pessaries, progesterone",
author = "Simone Eder and Lisa Kuchler and Matthias Katschnig and Bianca Brandl and Matthias Wolfgang and Ioannis Koutsamanis and Lukas Hentschel and Florian Arbeiter and Eva Roblegg and Martin Spoerk",
note = "Funding Information: This work was funded through the FFG as part of the PolyPrint project within the FEMtech program. The Research Center Pharmaceutical Engineering (RCPE) is funded within the framework of COMET – Competence Centers for Excellent Technologies by BMK, BMAW, Land Steiermark, and SFG. The COMET program is managed by the FFG. Clara Roblegg and the analytical lab team (all RCPE GmbH) are acknowledged for their support during the in‐vitro drug release studies. Ferdinand Klug and Christoph Lichal (both Hage3D GmbH) are thanked for their assistance during 3D‐printing process design. Publisher Copyright: {\textcopyright} 2023 Wiley-VCH GmbH.",
year = "2023",
month = jul,
day = "13",
doi = "10.1002/admt.202300237",
language = "English",
volume = "8.2023",
journal = "Advanced Materials Technologies",
issn = "2365-709X",
publisher = "Wiley-VCH ",
number = "17",

}

RIS (suitable for import to EndNote) - Download

TY - JOUR

T1 - Personalization of Complex Vaginal Inserts of Ethylene Vinyl Acetate via 3D-Printing

AU - Eder, Simone

AU - Kuchler, Lisa

AU - Katschnig, Matthias

AU - Brandl, Bianca

AU - Wolfgang, Matthias

AU - Koutsamanis, Ioannis

AU - Hentschel, Lukas

AU - Arbeiter, Florian

AU - Roblegg, Eva

AU - Spoerk, Martin

N1 - Funding Information: This work was funded through the FFG as part of the PolyPrint project within the FEMtech program. The Research Center Pharmaceutical Engineering (RCPE) is funded within the framework of COMET – Competence Centers for Excellent Technologies by BMK, BMAW, Land Steiermark, and SFG. The COMET program is managed by the FFG. Clara Roblegg and the analytical lab team (all RCPE GmbH) are acknowledged for their support during the in‐vitro drug release studies. Ferdinand Klug and Christoph Lichal (both Hage3D GmbH) are thanked for their assistance during 3D‐printing process design. Publisher Copyright: © 2023 Wiley-VCH GmbH.

PY - 2023/7/13

Y1 - 2023/7/13

N2 - Ethylene vinyl acetate (EVA) with a vinyl acetate (VA) content of 28 wt.%(EVA28) is frequently used in vaginal inserts and subcutaneous implants dueto its biocompatibility and drug-releasing properties. Traditionally beingprocessed via hot melt extrusion, its processibility via filament-based3D-printing was reported to be impossible. Consequently, no applicablecustomization concepts for vaginal inserts exist. For the first time, thefabrication of 3D-printed vaginal inserts (urethra pessaries) of EVA28 isdemonstrated by optimizing its viscosity, employing 3D-printer adaptations,and carefully selecting printing parameters. The infill pattern of fully filledmono-material pessaries (determining the number and orientation of weldlines) significantly affects the in vitro release of the model drug progesterone(P4), while other critical parameters (the pessary’s mechanical properties andappearance) remain unaffected. Weld lines act as diffusion barriers fordissolved P4 molecules. Hence, a high number of weld lines to be crossedreduces the overall P4 diffusivity in EVA28, decreasing the P4 release rate. Tofurther control the P4 release, innovative multi-material pessary designs(additionally comprising EVA with a VA content of 9 wt.% that is also used invaginal inserts) allow to tailor the in vitro drug release and the mechanicsindividually. Thereby, this work highly improves the mechanisticunderstanding on drug release modifications from 3D-printednon-biodegradable devices. The findings build the basis for the firstapplication of customized vaginal inserts, as they are based on polymers usedin corresponding marketed products for more than 20 years.

AB - Ethylene vinyl acetate (EVA) with a vinyl acetate (VA) content of 28 wt.%(EVA28) is frequently used in vaginal inserts and subcutaneous implants dueto its biocompatibility and drug-releasing properties. Traditionally beingprocessed via hot melt extrusion, its processibility via filament-based3D-printing was reported to be impossible. Consequently, no applicablecustomization concepts for vaginal inserts exist. For the first time, thefabrication of 3D-printed vaginal inserts (urethra pessaries) of EVA28 isdemonstrated by optimizing its viscosity, employing 3D-printer adaptations,and carefully selecting printing parameters. The infill pattern of fully filledmono-material pessaries (determining the number and orientation of weldlines) significantly affects the in vitro release of the model drug progesterone(P4), while other critical parameters (the pessary’s mechanical properties andappearance) remain unaffected. Weld lines act as diffusion barriers fordissolved P4 molecules. Hence, a high number of weld lines to be crossedreduces the overall P4 diffusivity in EVA28, decreasing the P4 release rate. Tofurther control the P4 release, innovative multi-material pessary designs(additionally comprising EVA with a VA content of 9 wt.% that is also used invaginal inserts) allow to tailor the in vitro drug release and the mechanicsindividually. Thereby, this work highly improves the mechanisticunderstanding on drug release modifications from 3D-printednon-biodegradable devices. The findings build the basis for the firstapplication of customized vaginal inserts, as they are based on polymers usedin corresponding marketed products for more than 20 years.

KW - 3D-printing

KW - drug releases

KW - ethylene vinyl acetate

KW - EVA

KW - extrusion-based additive manufacturing

KW - fused deposition modeling

KW - fused filament fabrications

KW - pessaries

KW - progesterone

UR - http://www.scopus.com/inward/record.url?scp=85159548835&partnerID=8YFLogxK

U2 - 10.1002/admt.202300237

DO - 10.1002/admt.202300237

M3 - Article

AN - SCOPUS:85159548835

VL - 8.2023

JO - Advanced Materials Technologies

JF - Advanced Materials Technologies

SN - 2365-709X

IS - 17

M1 - 2300237

ER -

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