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Hybrid Aptamer Molecularly Imprinted Polymer Nanoparticles for Reducing Oxidized Low-Density Lipoprotein Internalization by Macrophages

  • Suticha Chunta (Korresp. Autor*in)
  • , Soemwit Khongwichit
  • , Piyawut Swangphon
  • , Maliwan Srisuk
  • , Peter A. Lieberzeit
  • , Maliwan Amatatongchai

Veröffentlichungen: Beitrag in FachzeitschriftArtikelPeer Reviewed

Abstract

Oxidized low-density lipoprotein (oxLDL) is the most typical physiological trigger for the formation of macrophage foam cells, leading to atherosclerosis and coronary heart disease. The inhibition of internalized oxLDL in macrophages is a proven effective strategy for the prevention of atherosclerosis. A hybrid aptamer-molecularly imprinted polymer nanoparticle (AP-MIP NP) is a novel synthetic, biocompatible, selective material that can bind directly to oxLDL and decrease its uptake by macrophages by 62 ± 2% compared to oxLDL alone at a concentration of 8.25 × 107 particles/mL. Oil red O staining indicates that macrophages treated with a combination of AP-MIP NP and oxLDL exhibited a marked decrease in intracellular lipid accumulation compared to those treated with oxLDL alone, resulting in reduced foam cell formation and a decrease in the production of tumor necrosis factor-α and interleukin-6 inflammatory cytokines. The polymer nanoparticle matrix effectively serves as a protective shell for the aptamer at hazardous pH conditions of 4.0 and 10.0, as well as in the presence of DNase I at 100 Kunitz units. The AP-MIP NP bound to the oxLDL surface disrupts the interaction between oxLDL and the lectin-like oxLDL receptor-1 and the cluster of differentiation 36 scavenger receptors, as demonstrated by receptor-coupled ELISA. This restricts the ability of macrophages to uptake oxLDL. This hybrid AP-MIP NP shows promise as a future therapeutic agent to reduce oxLDL uptake and inhibit foam cell formation for atherosclerosis prevention.

OriginalspracheEnglisch
Seiten (von - bis)40101-40115
Seitenumfang15
FachzeitschriftACS Applied Materials and Interfaces
Jahrgang17
Ausgabenummer28
Frühes Online-Datum2025
DOIs
PublikationsstatusVeröffentlicht - 16 Juli 2025

Fördermittel

This project is funded by the National Research Council of Thailand (NRCT) (Contact no. N42A660972). Soemwit Khongwichit was supported by the Faculty of Medical Technology Research Fund, Prince of Songkla University; the Graduate Fellowship (Ph.D.), Faculty of Science Research Fund, Prince of Songkla University (Contact no. 1-2566-02-001); the Overseas Thesis Research Grant for Graduate Students, Graduate school, Prince of Songkla University (Contact no. OTR2567-002); and Ernst Mach Grant, weltweit, OeAD, Austria. Research reported in this publication was jointly supported by the ASEAN-European Academic University Network (ASEA-UNINET), the Austrian Federal Ministry of Education, Science and Research (BMBWF), and the OeAD\u2500Austria\u2019s Agency for Education and Internationalization. We acknowledge Natcha Keereeruk, Sorawit Raknui, Nuttawat Khatanan, and Nilutfee Nijinikaree for their contributions to cell culture operations.

ÖFOS 2012

  • 205019 Materialwissenschaften
  • 210004 Nanomaterialien
  • 104017 Physikalische Chemie

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