Defect density in multiwalled carbon nanotubes influences ovalbumin adsorption and promotes macrophage activation and CD4+ T-cell proliferation

Wei Bai,1 Achyut Raghavendra,2 Ramakrishna Podila,2,* Jared M Brown1,* 1Department of Pharmaceutical Sciences, Skaggs School of Pharmacy and Pharmaceutical Sciences, University of Colorado-Anschutz Medical Campus, Aurora, CO, 2Laboratory of Nano-Biophysics, Department of Physics and Astronomy, Clem...

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Autores principales: Bai W, Raghavendra A, Podila R, Brown JM
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Publicado: Dove Medical Press 2016
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spelling oai:doaj.org-article:cc01207bb258413fadf437b3343485ca2021-12-02T07:13:45ZDefect density in multiwalled carbon nanotubes influences ovalbumin adsorption and promotes macrophage activation and CD4+ T-cell proliferation1178-2013https://doaj.org/article/cc01207bb258413fadf437b3343485ca2016-09-01T00:00:00Zhttps://www.dovepress.com/defect-density-in-multiwalled-carbon-nanotubes-influences-ovalbumin-ad-peer-reviewed-article-IJNhttps://doaj.org/toc/1178-2013Wei Bai,1 Achyut Raghavendra,2 Ramakrishna Podila,2,* Jared M Brown1,* 1Department of Pharmaceutical Sciences, Skaggs School of Pharmacy and Pharmaceutical Sciences, University of Colorado-Anschutz Medical Campus, Aurora, CO, 2Laboratory of Nano-Biophysics, Department of Physics and Astronomy, Clemson Nanomaterials Center and COMSET, Clemson University, Clemson, SC, USA *These authors contributed equally to this manuscript Abstract: Carbon nanotubes (CNTs) are of great interest for the development of drugs and vaccines due to their unique physicochemical properties. The high surface area to volume ratio and delocalized pi-electron cloud of CNTs promote binding of proteins to the surface forming a protein corona. This unique feature of CNTs has been recognized for potential delivery of antigens for strong and long-lasting antigen-specific immune responses. Based on an earlier study that demonstrated increased protein binding, we propose that carboxylated multiwalled CNTs (MWCNTs) can function as an improved carrier to deliver antigens such as ovalbumin (OVA). To test this hypothesis, we coated carboxylated MWCNTs with OVA and measured uptake and activation of antigen-presenting cells (macrophages) and their ability to stimulate CD4+ T-cell proliferation. We employed two types of carboxylated MWCNTs with different surface areas and defects (MWCNT-2 and MWCNT-30). MWCNT-2 and MWCNT-30 have surface areas of ~215 m2/g and 94 m2/g, respectively. The ratios of D- to G-band areas (ID/IG) were 0.97 and 1.37 for MWCNT-2 and MWCNT-30, respectively, samples showing that MWCNT-30 contained more defects. The increase in defects in MWCNT-30 led to increased binding of OVA as compared to MWCNT-2 (1,066±182 µg/mL vs 582±41 µg/mL, respectively). Both types of MWCNTs, along with MWCNT–OVA complexes, showed no observable toxicity to bone-marrow-derived macrophages up to 5 days. Surprisingly, we found that MWCNT–OVA complex significantly increased the expression of major histocompatibility complex class II on macrophages and production of pro-inflammatory cytokines (tumor necrosis factor-α and interleukin 6), while MWCNTs without OVA protein corona did not. The coculture of MWCNT–OVA-complex-treated macrophages and OVA-specific CD4+ T-cells isolated from OT-II mice demonstrated robust proliferation of CD4+ T-cells. This study provides strong evidence for a role for defects in carboxylated MWCNTs and their use in the efficient delivery of antigens for the development of next-generation vaccines. Keywords: MWCNT, protein corona, nanoparticle, defect, carboxylation, antigen presentation, immune responseBai WRaghavendra APodila RBrown JMDove Medical PressarticleMWCNTprotein coronananoparticledefectcarboxylationantigen presentationimmune responseMedicine (General)R5-920ENInternational Journal of Nanomedicine, Vol Volume 11, Pp 4357-4371 (2016)
institution DOAJ
collection DOAJ
language EN
topic MWCNT
protein corona
nanoparticle
defect
carboxylation
antigen presentation
immune response
Medicine (General)
R5-920
spellingShingle MWCNT
protein corona
nanoparticle
defect
carboxylation
antigen presentation
immune response
Medicine (General)
R5-920
Bai W
Raghavendra A
Podila R
Brown JM
Defect density in multiwalled carbon nanotubes influences ovalbumin adsorption and promotes macrophage activation and CD4+ T-cell proliferation
description Wei Bai,1 Achyut Raghavendra,2 Ramakrishna Podila,2,* Jared M Brown1,* 1Department of Pharmaceutical Sciences, Skaggs School of Pharmacy and Pharmaceutical Sciences, University of Colorado-Anschutz Medical Campus, Aurora, CO, 2Laboratory of Nano-Biophysics, Department of Physics and Astronomy, Clemson Nanomaterials Center and COMSET, Clemson University, Clemson, SC, USA *These authors contributed equally to this manuscript Abstract: Carbon nanotubes (CNTs) are of great interest for the development of drugs and vaccines due to their unique physicochemical properties. The high surface area to volume ratio and delocalized pi-electron cloud of CNTs promote binding of proteins to the surface forming a protein corona. This unique feature of CNTs has been recognized for potential delivery of antigens for strong and long-lasting antigen-specific immune responses. Based on an earlier study that demonstrated increased protein binding, we propose that carboxylated multiwalled CNTs (MWCNTs) can function as an improved carrier to deliver antigens such as ovalbumin (OVA). To test this hypothesis, we coated carboxylated MWCNTs with OVA and measured uptake and activation of antigen-presenting cells (macrophages) and their ability to stimulate CD4+ T-cell proliferation. We employed two types of carboxylated MWCNTs with different surface areas and defects (MWCNT-2 and MWCNT-30). MWCNT-2 and MWCNT-30 have surface areas of ~215 m2/g and 94 m2/g, respectively. The ratios of D- to G-band areas (ID/IG) were 0.97 and 1.37 for MWCNT-2 and MWCNT-30, respectively, samples showing that MWCNT-30 contained more defects. The increase in defects in MWCNT-30 led to increased binding of OVA as compared to MWCNT-2 (1,066±182 µg/mL vs 582±41 µg/mL, respectively). Both types of MWCNTs, along with MWCNT–OVA complexes, showed no observable toxicity to bone-marrow-derived macrophages up to 5 days. Surprisingly, we found that MWCNT–OVA complex significantly increased the expression of major histocompatibility complex class II on macrophages and production of pro-inflammatory cytokines (tumor necrosis factor-α and interleukin 6), while MWCNTs without OVA protein corona did not. The coculture of MWCNT–OVA-complex-treated macrophages and OVA-specific CD4+ T-cells isolated from OT-II mice demonstrated robust proliferation of CD4+ T-cells. This study provides strong evidence for a role for defects in carboxylated MWCNTs and their use in the efficient delivery of antigens for the development of next-generation vaccines. Keywords: MWCNT, protein corona, nanoparticle, defect, carboxylation, antigen presentation, immune response
format article
author Bai W
Raghavendra A
Podila R
Brown JM
author_facet Bai W
Raghavendra A
Podila R
Brown JM
author_sort Bai W
title Defect density in multiwalled carbon nanotubes influences ovalbumin adsorption and promotes macrophage activation and CD4+ T-cell proliferation
title_short Defect density in multiwalled carbon nanotubes influences ovalbumin adsorption and promotes macrophage activation and CD4+ T-cell proliferation
title_full Defect density in multiwalled carbon nanotubes influences ovalbumin adsorption and promotes macrophage activation and CD4+ T-cell proliferation
title_fullStr Defect density in multiwalled carbon nanotubes influences ovalbumin adsorption and promotes macrophage activation and CD4+ T-cell proliferation
title_full_unstemmed Defect density in multiwalled carbon nanotubes influences ovalbumin adsorption and promotes macrophage activation and CD4+ T-cell proliferation
title_sort defect density in multiwalled carbon nanotubes influences ovalbumin adsorption and promotes macrophage activation and cd4+ t-cell proliferation
publisher Dove Medical Press
publishDate 2016
url https://doaj.org/article/cc01207bb258413fadf437b3343485ca
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AT raghavendraa defectdensityinmultiwalledcarbonnanotubesinfluencesovalbuminadsorptionandpromotesmacrophageactivationandnbspcd4nbsptcellproliferation
AT podilar defectdensityinmultiwalledcarbonnanotubesinfluencesovalbuminadsorptionandpromotesmacrophageactivationandnbspcd4nbsptcellproliferation
AT brownjm defectdensityinmultiwalledcarbonnanotubesinfluencesovalbuminadsorptionandpromotesmacrophageactivationandnbspcd4nbsptcellproliferation
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