On the role of protein disulfide isomerase in the retrograde cell transport of secreted phospholipases A2.

On the role of protein disulfide isomerase in the retrograde cell transport of secreted phospholipases A2.

Following the finding that ammodytoxin (Atx), a neurotoxic secreted phospholipase A2 (sPLA2) in snake venom, binds specifically to protein disulfide isomerase (PDI) in vitro we show that these proteins also interact in living rat PC12 cells that are able to internalize this group IIA (GIIA) sPLA2. A...

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Main Authors: Jernej Oberčkal, Lidija Kovačič, Jernej Šribar, Adrijana Leonardi, Klemen Dolinar, Anja Pucer Janež, Igor Križaj
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2015-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4357439?pdf=render
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spelling doaj-ae00c74f6bc84ca69ad9d11c0b73bf132020-11-24T21:30:29ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-01103e012069210.1371/journal.pone.0120692On the role of protein disulfide isomerase in the retrograde cell transport of secreted phospholipases A2.Jernej OberčkalLidija KovačičJernej ŠribarAdrijana LeonardiKlemen DolinarAnja Pucer JanežIgor KrižajFollowing the finding that ammodytoxin (Atx), a neurotoxic secreted phospholipase A2 (sPLA2) in snake venom, binds specifically to protein disulfide isomerase (PDI) in vitro we show that these proteins also interact in living rat PC12 cells that are able to internalize this group IIA (GIIA) sPLA2. Atx and PDI co-localize in both differentiated and non-differentiated PC12 cells, as shown by fluorescence microscopy. Based on a model of the complex between Atx and yeast PDI (yPDI), a three-dimensional model of the complex between Atx and human PDI (hPDI) was constructed. The Atx binding site on hPDI is situated between domains b and b'. Atx interacts hPDI with an extensive area on its interfacial binding surface. The mammalian GIB, GIIA, GV and GX sPLA2s have the same fold as Atx. The first three sPLA2s have been detected intracellularly but not the last one. The models of their complexes with hPDI were constructed by replacement of Atx with the respective mammalian sPLA2 in the Atx-hPDI complex and molecular docking of the structures. According to the generated models, mammalian GIB, GIIA and GV sPLA2s form complexes with hPDI very similar to that with Atx. The contact area between GX sPLA2 and hPDI is however different from that of the other sPLA2s. Heterologous competition of Atx binding to hPDI with GV and GX sPLA2s confirmed the model-based expectation that GV sPLA2 was a more effective inhibitor than GX sPLA2, thus validating our model. The results suggest a role of hPDI in the (patho)physiology of some snake venom and mammalian sPLA2s by assisting the retrograde transport of these molecules from the cell surface. The sPLA2-hPDI model constitutes a valuable tool to facilitate further insights into this process and into the (patho)physiology of sPLA2s in relation to their action intracellularly.http://europepmc.org/articles/PMC4357439?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Jernej Oberčkal
Lidija Kovačič
Jernej Šribar
Adrijana Leonardi
Klemen Dolinar
Anja Pucer Janež
Igor Križaj
spellingShingle Jernej Oberčkal
Lidija Kovačič
Jernej Šribar
Adrijana Leonardi
Klemen Dolinar
Anja Pucer Janež
Igor Križaj
On the role of protein disulfide isomerase in the retrograde cell transport of secreted phospholipases A2.
PLoS ONE
author_facet Jernej Oberčkal
Lidija Kovačič
Jernej Šribar
Adrijana Leonardi
Klemen Dolinar
Anja Pucer Janež
Igor Križaj
author_sort Jernej Oberčkal
title On the role of protein disulfide isomerase in the retrograde cell transport of secreted phospholipases A2.
title_short On the role of protein disulfide isomerase in the retrograde cell transport of secreted phospholipases A2.
title_full On the role of protein disulfide isomerase in the retrograde cell transport of secreted phospholipases A2.
title_fullStr On the role of protein disulfide isomerase in the retrograde cell transport of secreted phospholipases A2.
title_full_unstemmed On the role of protein disulfide isomerase in the retrograde cell transport of secreted phospholipases A2.
title_sort on the role of protein disulfide isomerase in the retrograde cell transport of secreted phospholipases a2.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2015-01-01
description Following the finding that ammodytoxin (Atx), a neurotoxic secreted phospholipase A2 (sPLA2) in snake venom, binds specifically to protein disulfide isomerase (PDI) in vitro we show that these proteins also interact in living rat PC12 cells that are able to internalize this group IIA (GIIA) sPLA2. Atx and PDI co-localize in both differentiated and non-differentiated PC12 cells, as shown by fluorescence microscopy. Based on a model of the complex between Atx and yeast PDI (yPDI), a three-dimensional model of the complex between Atx and human PDI (hPDI) was constructed. The Atx binding site on hPDI is situated between domains b and b'. Atx interacts hPDI with an extensive area on its interfacial binding surface. The mammalian GIB, GIIA, GV and GX sPLA2s have the same fold as Atx. The first three sPLA2s have been detected intracellularly but not the last one. The models of their complexes with hPDI were constructed by replacement of Atx with the respective mammalian sPLA2 in the Atx-hPDI complex and molecular docking of the structures. According to the generated models, mammalian GIB, GIIA and GV sPLA2s form complexes with hPDI very similar to that with Atx. The contact area between GX sPLA2 and hPDI is however different from that of the other sPLA2s. Heterologous competition of Atx binding to hPDI with GV and GX sPLA2s confirmed the model-based expectation that GV sPLA2 was a more effective inhibitor than GX sPLA2, thus validating our model. The results suggest a role of hPDI in the (patho)physiology of some snake venom and mammalian sPLA2s by assisting the retrograde transport of these molecules from the cell surface. The sPLA2-hPDI model constitutes a valuable tool to facilitate further insights into this process and into the (patho)physiology of sPLA2s in relation to their action intracellularly.
url http://europepmc.org/articles/PMC4357439?pdf=render
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