Drug Development in Conformational Diseases: A Novel Family of Chemical Chaperones that Bind and Stabilise Several Polymorphic Amyloid Structures

The increasing prevalence of conformational diseases, including Alzheimer's disease, type 2 Diabetes Mellitus and Cancer, poses a global challenge at many different levels. It has devastating effects on the sufferers as well as a tremendous economic impact on families and the health system. In...

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Autores principales: Sablón-Carrazana, Marquiza, Fernández, Isaac, Bencomo, Alberto, Lara-Martínez, Reyna, Rivera-Marrero, Suchitil, Domínguez, Guadalupe, Pérez-Perera, Rafaela, Jiménez-García, Luis Felipe, Altamirano-Bustamante, Nelly F., Diaz-Delgado, Massiel, Vedrenne, Fernand, Rivillas-Acevedo, Lina, Pasten-Hidalgo, Karina, Segura-Valdez, María de Lourdes, Islas-Andrade, Sergio, Garrido-Magaña, Eulalia, Perera-Pintado, Alejandro, Prats-Capote, Anaís, Rodríguez-Tanty, Chryslaine, Altamirano-Bustamante, Myriam M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4556714/
https://www.ncbi.nlm.nih.gov/pubmed/26327208
http://dx.doi.org/10.1371/journal.pone.0135292
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author Sablón-Carrazana, Marquiza
Fernández, Isaac
Bencomo, Alberto
Lara-Martínez, Reyna
Rivera-Marrero, Suchitil
Domínguez, Guadalupe
Pérez-Perera, Rafaela
Jiménez-García, Luis Felipe
Altamirano-Bustamante, Nelly F.
Diaz-Delgado, Massiel
Vedrenne, Fernand
Rivillas-Acevedo, Lina
Pasten-Hidalgo, Karina
Segura-Valdez, María de Lourdes
Islas-Andrade, Sergio
Garrido-Magaña, Eulalia
Perera-Pintado, Alejandro
Prats-Capote, Anaís
Rodríguez-Tanty, Chryslaine
Altamirano-Bustamante, Myriam M.
author_facet Sablón-Carrazana, Marquiza
Fernández, Isaac
Bencomo, Alberto
Lara-Martínez, Reyna
Rivera-Marrero, Suchitil
Domínguez, Guadalupe
Pérez-Perera, Rafaela
Jiménez-García, Luis Felipe
Altamirano-Bustamante, Nelly F.
Diaz-Delgado, Massiel
Vedrenne, Fernand
Rivillas-Acevedo, Lina
Pasten-Hidalgo, Karina
Segura-Valdez, María de Lourdes
Islas-Andrade, Sergio
Garrido-Magaña, Eulalia
Perera-Pintado, Alejandro
Prats-Capote, Anaís
Rodríguez-Tanty, Chryslaine
Altamirano-Bustamante, Myriam M.
author_sort Sablón-Carrazana, Marquiza
collection PubMed
description The increasing prevalence of conformational diseases, including Alzheimer's disease, type 2 Diabetes Mellitus and Cancer, poses a global challenge at many different levels. It has devastating effects on the sufferers as well as a tremendous economic impact on families and the health system. In this work, we apply a cross-functional approach that combines ideas, concepts and technologies from several disciplines in order to study, in silico and in vitro, the role of a novel chemical chaperones family (NCHCHF) in processes of protein aggregation in conformational diseases. Given that Serum Albumin (SA) is the most abundant protein in the blood of mammals, and Bovine Serum Albumin (BSA) is an off-the-shelf protein available in most labs around the world, we compared the ligandability of BSA:NCHCHF with the interaction sites in the Human Islet Amyloid Polypeptide (hIAPP):NCHCHF, and in the amyloid pharmacophore fragments (Aβ17–42 and Aβ16–21):NCHCHF. We posit that the merging of this interaction sites is a meta-structure of pharmacophore which allows the development of chaperones that can prevent protein aggregation at various states from: stabilizing the native state to destabilizing oligomeric state and protofilament. Furthermore to stabilize fibrillar structures, thus decreasing the amount of toxic oligomers in solution, as is the case with the NCHCHF. The paper demonstrates how a set of NCHCHF can be used for studying and potentially treating the various physiopathological stages of a conformational disease. For instance, when dealing with an acute phase of cytotoxicity, what is needed is the recruitment of cytotoxic oligomers, thus chaperone F, which accelerates fiber formation, would be very useful; whereas in a chronic stage it is better to have chaperones A, B, C, and D, which stabilize the native and fibril structures halting self-catalysis and the creation of cytotoxic oligomers as a consequence of fiber formation. Furthermore, all the chaperones are able to protect and recondition the cerebellar granule cells (CGC) from the cytotoxicity produced by the hIAPP(20–29) fragment or by a low potassium medium, regardless of their capacity for accelerating or inhibiting in vitro formation of fibers. In vivo animal experiments are required to study the impact of chemical chaperones in cognitive and metabolic syndromes.
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spelling pubmed-45567142015-09-10 Drug Development in Conformational Diseases: A Novel Family of Chemical Chaperones that Bind and Stabilise Several Polymorphic Amyloid Structures Sablón-Carrazana, Marquiza Fernández, Isaac Bencomo, Alberto Lara-Martínez, Reyna Rivera-Marrero, Suchitil Domínguez, Guadalupe Pérez-Perera, Rafaela Jiménez-García, Luis Felipe Altamirano-Bustamante, Nelly F. Diaz-Delgado, Massiel Vedrenne, Fernand Rivillas-Acevedo, Lina Pasten-Hidalgo, Karina Segura-Valdez, María de Lourdes Islas-Andrade, Sergio Garrido-Magaña, Eulalia Perera-Pintado, Alejandro Prats-Capote, Anaís Rodríguez-Tanty, Chryslaine Altamirano-Bustamante, Myriam M. PLoS One Research Article The increasing prevalence of conformational diseases, including Alzheimer's disease, type 2 Diabetes Mellitus and Cancer, poses a global challenge at many different levels. It has devastating effects on the sufferers as well as a tremendous economic impact on families and the health system. In this work, we apply a cross-functional approach that combines ideas, concepts and technologies from several disciplines in order to study, in silico and in vitro, the role of a novel chemical chaperones family (NCHCHF) in processes of protein aggregation in conformational diseases. Given that Serum Albumin (SA) is the most abundant protein in the blood of mammals, and Bovine Serum Albumin (BSA) is an off-the-shelf protein available in most labs around the world, we compared the ligandability of BSA:NCHCHF with the interaction sites in the Human Islet Amyloid Polypeptide (hIAPP):NCHCHF, and in the amyloid pharmacophore fragments (Aβ17–42 and Aβ16–21):NCHCHF. We posit that the merging of this interaction sites is a meta-structure of pharmacophore which allows the development of chaperones that can prevent protein aggregation at various states from: stabilizing the native state to destabilizing oligomeric state and protofilament. Furthermore to stabilize fibrillar structures, thus decreasing the amount of toxic oligomers in solution, as is the case with the NCHCHF. The paper demonstrates how a set of NCHCHF can be used for studying and potentially treating the various physiopathological stages of a conformational disease. For instance, when dealing with an acute phase of cytotoxicity, what is needed is the recruitment of cytotoxic oligomers, thus chaperone F, which accelerates fiber formation, would be very useful; whereas in a chronic stage it is better to have chaperones A, B, C, and D, which stabilize the native and fibril structures halting self-catalysis and the creation of cytotoxic oligomers as a consequence of fiber formation. Furthermore, all the chaperones are able to protect and recondition the cerebellar granule cells (CGC) from the cytotoxicity produced by the hIAPP(20–29) fragment or by a low potassium medium, regardless of their capacity for accelerating or inhibiting in vitro formation of fibers. In vivo animal experiments are required to study the impact of chemical chaperones in cognitive and metabolic syndromes. Public Library of Science 2015-09-01 /pmc/articles/PMC4556714/ /pubmed/26327208 http://dx.doi.org/10.1371/journal.pone.0135292 Text en © 2015 Sablón-Carrazana et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Sablón-Carrazana, Marquiza
Fernández, Isaac
Bencomo, Alberto
Lara-Martínez, Reyna
Rivera-Marrero, Suchitil
Domínguez, Guadalupe
Pérez-Perera, Rafaela
Jiménez-García, Luis Felipe
Altamirano-Bustamante, Nelly F.
Diaz-Delgado, Massiel
Vedrenne, Fernand
Rivillas-Acevedo, Lina
Pasten-Hidalgo, Karina
Segura-Valdez, María de Lourdes
Islas-Andrade, Sergio
Garrido-Magaña, Eulalia
Perera-Pintado, Alejandro
Prats-Capote, Anaís
Rodríguez-Tanty, Chryslaine
Altamirano-Bustamante, Myriam M.
Drug Development in Conformational Diseases: A Novel Family of Chemical Chaperones that Bind and Stabilise Several Polymorphic Amyloid Structures
title Drug Development in Conformational Diseases: A Novel Family of Chemical Chaperones that Bind and Stabilise Several Polymorphic Amyloid Structures
title_full Drug Development in Conformational Diseases: A Novel Family of Chemical Chaperones that Bind and Stabilise Several Polymorphic Amyloid Structures
title_fullStr Drug Development in Conformational Diseases: A Novel Family of Chemical Chaperones that Bind and Stabilise Several Polymorphic Amyloid Structures
title_full_unstemmed Drug Development in Conformational Diseases: A Novel Family of Chemical Chaperones that Bind and Stabilise Several Polymorphic Amyloid Structures
title_short Drug Development in Conformational Diseases: A Novel Family of Chemical Chaperones that Bind and Stabilise Several Polymorphic Amyloid Structures
title_sort drug development in conformational diseases: a novel family of chemical chaperones that bind and stabilise several polymorphic amyloid structures
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4556714/
https://www.ncbi.nlm.nih.gov/pubmed/26327208
http://dx.doi.org/10.1371/journal.pone.0135292
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