HIV-1 Capsid Assembly Inhibitor (CAI) Peptide: Structural Preferences and Delivery into Human Embryonic Lung Cells and Lymphocytes

The Human immunodeficiency virus 1 derived capsid assembly inhibitor peptide (HIV-1 CAI-peptide) is a promising lead candidate for anti-HIV drug development. Its drawback, however, is that it cannot permeate cells directly. Here we report the transport of the pharmacologically active CAI-peptide int...

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Autores principales: Braun, Klaus, Frank, Martin, Pipkorn, Rüdiger, Reed, Jennifer, Spring, Herbert, Debus, Jürgen, Didinger, Bernd, von der Lieth, Claus-Wilhelm, Wiessler, Manfred, Waldeck, Waldemar
Formato: Texto
Lenguaje:English
Publicado: Ivyspring International Publisher 2008
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2500149/
https://www.ncbi.nlm.nih.gov/pubmed/18695744
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author Braun, Klaus
Frank, Martin
Pipkorn, Rüdiger
Reed, Jennifer
Spring, Herbert
Debus, Jürgen
Didinger, Bernd
von der Lieth, Claus-Wilhelm
Wiessler, Manfred
Waldeck, Waldemar
author_facet Braun, Klaus
Frank, Martin
Pipkorn, Rüdiger
Reed, Jennifer
Spring, Herbert
Debus, Jürgen
Didinger, Bernd
von der Lieth, Claus-Wilhelm
Wiessler, Manfred
Waldeck, Waldemar
author_sort Braun, Klaus
collection PubMed
description The Human immunodeficiency virus 1 derived capsid assembly inhibitor peptide (HIV-1 CAI-peptide) is a promising lead candidate for anti-HIV drug development. Its drawback, however, is that it cannot permeate cells directly. Here we report the transport of the pharmacologically active CAI-peptide into human lymphocytes and Human Embryonic Lung cells (HEL) using the BioShuttle platform. Generally, the transfer of pharmacologically active substances across membranes, demonstrated by confocal laser scanning microscopy (CLSM), could lead to a loss of function by changing the molecule's structure. Molecular dynamics (MD) simulations and circular dichroism (CD) studies suggest that the CAI-peptide has an intrinsic capacity to form a helical structure, which seems to be critical for the pharmacological effect as revealed by intensive docking calculations and comparison with control peptides. This coupling of the CAI-peptide to a BioShuttle-molecule additionally improved its solubility. Under the conditions described, the HIV-1 CAI peptide was transported into living cells and could be localized in the vicinity of the mitochondria.
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spelling pubmed-25001492008-08-11 HIV-1 Capsid Assembly Inhibitor (CAI) Peptide: Structural Preferences and Delivery into Human Embryonic Lung Cells and Lymphocytes Braun, Klaus Frank, Martin Pipkorn, Rüdiger Reed, Jennifer Spring, Herbert Debus, Jürgen Didinger, Bernd von der Lieth, Claus-Wilhelm Wiessler, Manfred Waldeck, Waldemar Int J Med Sci Research Paper The Human immunodeficiency virus 1 derived capsid assembly inhibitor peptide (HIV-1 CAI-peptide) is a promising lead candidate for anti-HIV drug development. Its drawback, however, is that it cannot permeate cells directly. Here we report the transport of the pharmacologically active CAI-peptide into human lymphocytes and Human Embryonic Lung cells (HEL) using the BioShuttle platform. Generally, the transfer of pharmacologically active substances across membranes, demonstrated by confocal laser scanning microscopy (CLSM), could lead to a loss of function by changing the molecule's structure. Molecular dynamics (MD) simulations and circular dichroism (CD) studies suggest that the CAI-peptide has an intrinsic capacity to form a helical structure, which seems to be critical for the pharmacological effect as revealed by intensive docking calculations and comparison with control peptides. This coupling of the CAI-peptide to a BioShuttle-molecule additionally improved its solubility. Under the conditions described, the HIV-1 CAI peptide was transported into living cells and could be localized in the vicinity of the mitochondria. Ivyspring International Publisher 2008-07-31 /pmc/articles/PMC2500149/ /pubmed/18695744 Text en © Ivyspring International Publisher. This is an open-access article distributed under the terms of the Creative Commons License (http://creativecommons.org/licenses/by-nc-nd/3.0/). Reproduction is permitted for personal, noncommercial use, provided that the article is in whole, unmodified, and properly cited.
spellingShingle Research Paper
Braun, Klaus
Frank, Martin
Pipkorn, Rüdiger
Reed, Jennifer
Spring, Herbert
Debus, Jürgen
Didinger, Bernd
von der Lieth, Claus-Wilhelm
Wiessler, Manfred
Waldeck, Waldemar
HIV-1 Capsid Assembly Inhibitor (CAI) Peptide: Structural Preferences and Delivery into Human Embryonic Lung Cells and Lymphocytes
title HIV-1 Capsid Assembly Inhibitor (CAI) Peptide: Structural Preferences and Delivery into Human Embryonic Lung Cells and Lymphocytes
title_full HIV-1 Capsid Assembly Inhibitor (CAI) Peptide: Structural Preferences and Delivery into Human Embryonic Lung Cells and Lymphocytes
title_fullStr HIV-1 Capsid Assembly Inhibitor (CAI) Peptide: Structural Preferences and Delivery into Human Embryonic Lung Cells and Lymphocytes
title_full_unstemmed HIV-1 Capsid Assembly Inhibitor (CAI) Peptide: Structural Preferences and Delivery into Human Embryonic Lung Cells and Lymphocytes
title_short HIV-1 Capsid Assembly Inhibitor (CAI) Peptide: Structural Preferences and Delivery into Human Embryonic Lung Cells and Lymphocytes
title_sort hiv-1 capsid assembly inhibitor (cai) peptide: structural preferences and delivery into human embryonic lung cells and lymphocytes
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2500149/
https://www.ncbi.nlm.nih.gov/pubmed/18695744
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