Identification and characterization of new isoforms of human fas apoptotic inhibitory molecule (FAIM)

Fas Apoptosis Inhibitory Molecule (FAIM) is an evolutionarily highly conserved death receptor antagonist, widely expressed and known to participate in physiological and pathological processes. Two FAIM transcript variants have been characterized to date, namely FAIM short (FAIM-S) and FAIM long (FAI...

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Autores principales: Coccia, Elena, Calleja-Yagüe, Isabel, Planells-Ferrer, Laura, Sanuy, Blanca, Sanz, Belen, López-Soriano, Joaquin, Moubarak, Rana S., Munell, Francina, Barneda-Zahonero, Bruna, Comella, Joan X., Pérez-García, M. Jose
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5628826/
https://www.ncbi.nlm.nih.gov/pubmed/28981531
http://dx.doi.org/10.1371/journal.pone.0185327
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author Coccia, Elena
Calleja-Yagüe, Isabel
Planells-Ferrer, Laura
Sanuy, Blanca
Sanz, Belen
López-Soriano, Joaquin
Moubarak, Rana S.
Munell, Francina
Barneda-Zahonero, Bruna
Comella, Joan X.
Pérez-García, M. Jose
author_facet Coccia, Elena
Calleja-Yagüe, Isabel
Planells-Ferrer, Laura
Sanuy, Blanca
Sanz, Belen
López-Soriano, Joaquin
Moubarak, Rana S.
Munell, Francina
Barneda-Zahonero, Bruna
Comella, Joan X.
Pérez-García, M. Jose
author_sort Coccia, Elena
collection PubMed
description Fas Apoptosis Inhibitory Molecule (FAIM) is an evolutionarily highly conserved death receptor antagonist, widely expressed and known to participate in physiological and pathological processes. Two FAIM transcript variants have been characterized to date, namely FAIM short (FAIM-S) and FAIM long (FAIM-L). FAIM-S is ubiquitously expressed and serves as an anti-apoptotic protein in the immune system. Furthermore, in neurons, this isoform promotes NGF-induced neurite outgrowth through NF-кB and ERK signaling. In contrast FAIM-L is found only in neurons, where it exerts anti-apoptotic activity against several stimuli. In addition to these two variants, in silico studies point to the existence of two additional isoforms, neither of which have been characterized to date. In this regard, here we confirm the presence of these two additional FAIM isoforms in human fetal brain, fetal and adult testes, and placenta tissues. We named them FAIM-S_2a and FAIM-L_2a since they have the same sequence as FAIM-S and FAIM-L, but include exon 2a. PCR and western blot revealed that FAIM-S_2a shows ubiquitous expression in all the tissues and cellular models tested, while FAIM-L_2a is expressed exclusively in tissues of the nervous system. In addition, we found that, when overexpressed in non-neuronal cells, the splicing factor nSR100 induces the expression of the neuronal isoforms, thus identifying it as responsible for the generation of FAIM-L and FAIM-L_2a. Functionally, FAIM-S_2a and FAIM-L_2a increased neurite outgrowth in response to NGF stimulation in a neuronal model. This observation thus, supports the notion that these two isoforms are involved in neuronal differentiation. Furthermore, subcellular fractionation experiments revealed that, in contrast to FAIM-S and FAIM-L, FAIM-S_2a and FAIM-L_2a are able to localize to the nucleus, where they may have additional functions. In summary, here we report on two novel FAIM isoforms that may have relevant roles in the physiology and pathology of the nervous system.
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spelling pubmed-56288262017-10-20 Identification and characterization of new isoforms of human fas apoptotic inhibitory molecule (FAIM) Coccia, Elena Calleja-Yagüe, Isabel Planells-Ferrer, Laura Sanuy, Blanca Sanz, Belen López-Soriano, Joaquin Moubarak, Rana S. Munell, Francina Barneda-Zahonero, Bruna Comella, Joan X. Pérez-García, M. Jose PLoS One Research Article Fas Apoptosis Inhibitory Molecule (FAIM) is an evolutionarily highly conserved death receptor antagonist, widely expressed and known to participate in physiological and pathological processes. Two FAIM transcript variants have been characterized to date, namely FAIM short (FAIM-S) and FAIM long (FAIM-L). FAIM-S is ubiquitously expressed and serves as an anti-apoptotic protein in the immune system. Furthermore, in neurons, this isoform promotes NGF-induced neurite outgrowth through NF-кB and ERK signaling. In contrast FAIM-L is found only in neurons, where it exerts anti-apoptotic activity against several stimuli. In addition to these two variants, in silico studies point to the existence of two additional isoforms, neither of which have been characterized to date. In this regard, here we confirm the presence of these two additional FAIM isoforms in human fetal brain, fetal and adult testes, and placenta tissues. We named them FAIM-S_2a and FAIM-L_2a since they have the same sequence as FAIM-S and FAIM-L, but include exon 2a. PCR and western blot revealed that FAIM-S_2a shows ubiquitous expression in all the tissues and cellular models tested, while FAIM-L_2a is expressed exclusively in tissues of the nervous system. In addition, we found that, when overexpressed in non-neuronal cells, the splicing factor nSR100 induces the expression of the neuronal isoforms, thus identifying it as responsible for the generation of FAIM-L and FAIM-L_2a. Functionally, FAIM-S_2a and FAIM-L_2a increased neurite outgrowth in response to NGF stimulation in a neuronal model. This observation thus, supports the notion that these two isoforms are involved in neuronal differentiation. Furthermore, subcellular fractionation experiments revealed that, in contrast to FAIM-S and FAIM-L, FAIM-S_2a and FAIM-L_2a are able to localize to the nucleus, where they may have additional functions. In summary, here we report on two novel FAIM isoforms that may have relevant roles in the physiology and pathology of the nervous system. Public Library of Science 2017-10-05 /pmc/articles/PMC5628826/ /pubmed/28981531 http://dx.doi.org/10.1371/journal.pone.0185327 Text en © 2017 Coccia 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 (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Coccia, Elena
Calleja-Yagüe, Isabel
Planells-Ferrer, Laura
Sanuy, Blanca
Sanz, Belen
López-Soriano, Joaquin
Moubarak, Rana S.
Munell, Francina
Barneda-Zahonero, Bruna
Comella, Joan X.
Pérez-García, M. Jose
Identification and characterization of new isoforms of human fas apoptotic inhibitory molecule (FAIM)
title Identification and characterization of new isoforms of human fas apoptotic inhibitory molecule (FAIM)
title_full Identification and characterization of new isoforms of human fas apoptotic inhibitory molecule (FAIM)
title_fullStr Identification and characterization of new isoforms of human fas apoptotic inhibitory molecule (FAIM)
title_full_unstemmed Identification and characterization of new isoforms of human fas apoptotic inhibitory molecule (FAIM)
title_short Identification and characterization of new isoforms of human fas apoptotic inhibitory molecule (FAIM)
title_sort identification and characterization of new isoforms of human fas apoptotic inhibitory molecule (faim)
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5628826/
https://www.ncbi.nlm.nih.gov/pubmed/28981531
http://dx.doi.org/10.1371/journal.pone.0185327
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