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Massive Bioaccumulation and Self‐Assembly of Phenazine Compounds in Live Cells

Clofazimine is an orally administered drug that massively bioaccumulates in macrophages, forming membrane‐bound intracellular structures possessing nanoscale supramolecular features. Here, a library of phenazine compounds derived from clofazimine is synthesized and tested for ability to accumulate a...

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Autores principales: Min, Kyoung Ah, Rajeswaran, Walajapet G., Oldenbourg, Rudolf, Harris, Grant, Keswani, Rahul K., Chiang, Mason, Rzeczycki, Phillip, Talattof, Arjang, Hafeez, Mahwish, Horobin, Richard W., Larsen, Scott D., Stringer, Kathleen A., Rosania, Gus R.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4569013/
https://www.ncbi.nlm.nih.gov/pubmed/26380168
http://dx.doi.org/10.1002/advs.201500025
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author Min, Kyoung Ah
Rajeswaran, Walajapet G.
Oldenbourg, Rudolf
Harris, Grant
Keswani, Rahul K.
Chiang, Mason
Rzeczycki, Phillip
Talattof, Arjang
Hafeez, Mahwish
Horobin, Richard W.
Larsen, Scott D.
Stringer, Kathleen A.
Rosania, Gus R.
author_facet Min, Kyoung Ah
Rajeswaran, Walajapet G.
Oldenbourg, Rudolf
Harris, Grant
Keswani, Rahul K.
Chiang, Mason
Rzeczycki, Phillip
Talattof, Arjang
Hafeez, Mahwish
Horobin, Richard W.
Larsen, Scott D.
Stringer, Kathleen A.
Rosania, Gus R.
author_sort Min, Kyoung Ah
collection PubMed
description Clofazimine is an orally administered drug that massively bioaccumulates in macrophages, forming membrane‐bound intracellular structures possessing nanoscale supramolecular features. Here, a library of phenazine compounds derived from clofazimine is synthesized and tested for ability to accumulate and form ordered molecular aggregates inside cells. Regardless of chemical structure or physicochemical properties, bioaccumulation is consistently greater in macrophages than in epithelial cells. Microscopically, some self‐assembled structures exhibit a pronounced, diattenuation anisotropy signal, evident by the differential absorption of linearly polarized light, at the peak absorbance wavelength of the phenazine core. The measured anisotropy is well above the background anisotropy of endogenous cellular components, reflecting the self‐assembly of condensed, insoluble complexes of ordered phenazine molecules. Chemical variations introduced at the R‐imino position of the phenazine core lead to idiosyncratic effects on the compounds' bioaccumulation behavior as well as on the morphology and organization of the resulting intracellular structures. Beyond clofazimine, these results demonstrate how the self‐assembly of membrane permeant, orally bioavailable small molecule building blocks can endow cells with unnatural structural elements possessing chemical, physical, and functional characteristics unlike those of other natural cellular components.
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spelling pubmed-45690132015-09-14 Massive Bioaccumulation and Self‐Assembly of Phenazine Compounds in Live Cells Min, Kyoung Ah Rajeswaran, Walajapet G. Oldenbourg, Rudolf Harris, Grant Keswani, Rahul K. Chiang, Mason Rzeczycki, Phillip Talattof, Arjang Hafeez, Mahwish Horobin, Richard W. Larsen, Scott D. Stringer, Kathleen A. Rosania, Gus R. Adv Sci (Weinh) Full Papers Clofazimine is an orally administered drug that massively bioaccumulates in macrophages, forming membrane‐bound intracellular structures possessing nanoscale supramolecular features. Here, a library of phenazine compounds derived from clofazimine is synthesized and tested for ability to accumulate and form ordered molecular aggregates inside cells. Regardless of chemical structure or physicochemical properties, bioaccumulation is consistently greater in macrophages than in epithelial cells. Microscopically, some self‐assembled structures exhibit a pronounced, diattenuation anisotropy signal, evident by the differential absorption of linearly polarized light, at the peak absorbance wavelength of the phenazine core. The measured anisotropy is well above the background anisotropy of endogenous cellular components, reflecting the self‐assembly of condensed, insoluble complexes of ordered phenazine molecules. Chemical variations introduced at the R‐imino position of the phenazine core lead to idiosyncratic effects on the compounds' bioaccumulation behavior as well as on the morphology and organization of the resulting intracellular structures. Beyond clofazimine, these results demonstrate how the self‐assembly of membrane permeant, orally bioavailable small molecule building blocks can endow cells with unnatural structural elements possessing chemical, physical, and functional characteristics unlike those of other natural cellular components. John Wiley and Sons Inc. 2015-06-05 /pmc/articles/PMC4569013/ /pubmed/26380168 http://dx.doi.org/10.1002/advs.201500025 Text en © 2015 The Authors. Published by WILEY‐VCH Verlag GmbH & Co. KGaA, Weinheim This is an open access article under the terms of the Creative Commons Attribution (http://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Full Papers
Min, Kyoung Ah
Rajeswaran, Walajapet G.
Oldenbourg, Rudolf
Harris, Grant
Keswani, Rahul K.
Chiang, Mason
Rzeczycki, Phillip
Talattof, Arjang
Hafeez, Mahwish
Horobin, Richard W.
Larsen, Scott D.
Stringer, Kathleen A.
Rosania, Gus R.
Massive Bioaccumulation and Self‐Assembly of Phenazine Compounds in Live Cells
title Massive Bioaccumulation and Self‐Assembly of Phenazine Compounds in Live Cells
title_full Massive Bioaccumulation and Self‐Assembly of Phenazine Compounds in Live Cells
title_fullStr Massive Bioaccumulation and Self‐Assembly of Phenazine Compounds in Live Cells
title_full_unstemmed Massive Bioaccumulation and Self‐Assembly of Phenazine Compounds in Live Cells
title_short Massive Bioaccumulation and Self‐Assembly of Phenazine Compounds in Live Cells
title_sort massive bioaccumulation and self‐assembly of phenazine compounds in live cells
topic Full Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4569013/
https://www.ncbi.nlm.nih.gov/pubmed/26380168
http://dx.doi.org/10.1002/advs.201500025
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