Stable Conjugates of Peptides with Gold Nanorods for Biomedical Applications with Reduced Effects on Cell Viability
Author
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Adura, Carolina
Author
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Guerrero, Simón
es_CL
Author
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Salas, Edison
es_CL
Author
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Medel, Luis
es_CL
Author
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Riveros, Ana
es_CL
Author
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Mena, Juan
es_CL
Author
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Arbiol, Jordi
es_CL
Author
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Albericio, Fernando
es_CL
Author
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Giralt, Ernest
es_CL
Author
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Kogan Bocian, Marcelo
es_CL
Admission date
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2014-02-12T20:39:50Z
Available date
dc.date.available
2014-02-12T20:39:50Z
Publication date
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2013
Cita de ítem
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ACS Appl. Mater. Interfaces 2013, 5, 4076−4085
en_US
Identifier
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doi 10.1021/am3028537
Identifier
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https://repositorio.uchile.cl/handle/2250/121834
General note
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Artículo de publicación ISI
en_US
Abstract
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Gold nanorods used in therapy and diagnosis
must be nontoxic and stable in biological media and should be
specific for the target. The complete combination of these
three factors has hindered the use of gold nanorods as carriers
in biological and biomedical applications. In this study, we
produced a conjugate of gold nanorods with the peptide
CLPFFD that recognizes toxic β-amyloid aggregates present in
Alzheimer’s disease, demonstrates colloidal stability, maintains
plasmonic properties, and shows no effects on cell viability in
the SH-SY5Y cell line. Furthermore, the irradiation of β-
amyloid in the presence of the conjugate with near-infrared
region irradiation energy reduces the amyloidogenic process reducing also its cytotoxicity. The nanorods were synthesized
following the seed-mediated method in cetyltrimethylammonium bromide (CTAB) and were conjugated with the N-terminal
cysteine peptide, CLPFFD. The conjugate was exhaustively characterized using different techniques (Absorption spectroscopy,
X-ray photoelectron spectroscopy, electron energy loss spectroscopy, and zeta potential). The effects on cell viability and cell
penetration by transmission electron microscopy of the conjugate were evaluated. The chemisorption of the peptide on the
surface of gold nanorods increases their stability and reduces their effects on cell viability.