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Identification of Novel Placentally Expressed Aspartic Proteinase in Humans

This study presents pioneering data concerning the human pregnancy-associated glycoprotein-Like family, identified in the genome, of the term placental transcriptome and proteome. RNA-seq allowed the identification of 1364 bp hPAG-L/pep cDNA with at least 56.5% homology with other aspartic proteinas...

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Autores principales: Majewska, Marta, Lipka, Aleksandra, Panasiewicz, Grzegorz, Gowkielewicz, Marek, Jozwik, Marcin, Majewski, Mariusz Krzysztof, Szafranska, Bozena
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5486050/
https://www.ncbi.nlm.nih.gov/pubmed/28594357
http://dx.doi.org/10.3390/ijms18061227
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author Majewska, Marta
Lipka, Aleksandra
Panasiewicz, Grzegorz
Gowkielewicz, Marek
Jozwik, Marcin
Majewski, Mariusz Krzysztof
Szafranska, Bozena
author_facet Majewska, Marta
Lipka, Aleksandra
Panasiewicz, Grzegorz
Gowkielewicz, Marek
Jozwik, Marcin
Majewski, Mariusz Krzysztof
Szafranska, Bozena
author_sort Majewska, Marta
collection PubMed
description This study presents pioneering data concerning the human pregnancy-associated glycoprotein-Like family, identified in the genome, of the term placental transcriptome and proteome. RNA-seq allowed the identification of 1364 bp hPAG-L/pep cDNA with at least 56.5% homology with other aspartic proteinases (APs). In silico analyses revealed 388 amino acids (aa) of full-length hPAG-L polypeptide precursor, with 15 aa-signal peptide, 47 aa-blocking peptide and 326 aa-mature protein, and two Asp residues (D), specific for a catalytic cleft of the APs (VVFDTGSSNLWV91-102 and AIVDTGTSLLTG274-285). Capillary sequencing identified 9330 bp of the hPAG-L gene (Gen Bank Acc. No. KX533473), composed of nine exons and eight introns. Heterologous Western blotting revealed the presence of one dominant 60 kDa isoform of the hPAG-L amongst cellular placental proteins. Detection with anti-pPAG-P and anti-Rec pPAG2 polyclonals allowed identification of the hPAG-L proteins located within regions of chorionic villi, especially within the syncytiotrophoblast of term singleton placentas. Our novel data extend the present knowledge about the human genome, as well as placental transcriptome and proteome during term pregnancy. Presumably, this may contribute to establishing a new diagnostic tool for examination of some disturbances during human pregnancy, as well as growing interest from both scientific and clinical perspectives.
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spelling pubmed-54860502017-06-29 Identification of Novel Placentally Expressed Aspartic Proteinase in Humans Majewska, Marta Lipka, Aleksandra Panasiewicz, Grzegorz Gowkielewicz, Marek Jozwik, Marcin Majewski, Mariusz Krzysztof Szafranska, Bozena Int J Mol Sci Article This study presents pioneering data concerning the human pregnancy-associated glycoprotein-Like family, identified in the genome, of the term placental transcriptome and proteome. RNA-seq allowed the identification of 1364 bp hPAG-L/pep cDNA with at least 56.5% homology with other aspartic proteinases (APs). In silico analyses revealed 388 amino acids (aa) of full-length hPAG-L polypeptide precursor, with 15 aa-signal peptide, 47 aa-blocking peptide and 326 aa-mature protein, and two Asp residues (D), specific for a catalytic cleft of the APs (VVFDTGSSNLWV91-102 and AIVDTGTSLLTG274-285). Capillary sequencing identified 9330 bp of the hPAG-L gene (Gen Bank Acc. No. KX533473), composed of nine exons and eight introns. Heterologous Western blotting revealed the presence of one dominant 60 kDa isoform of the hPAG-L amongst cellular placental proteins. Detection with anti-pPAG-P and anti-Rec pPAG2 polyclonals allowed identification of the hPAG-L proteins located within regions of chorionic villi, especially within the syncytiotrophoblast of term singleton placentas. Our novel data extend the present knowledge about the human genome, as well as placental transcriptome and proteome during term pregnancy. Presumably, this may contribute to establishing a new diagnostic tool for examination of some disturbances during human pregnancy, as well as growing interest from both scientific and clinical perspectives. MDPI 2017-06-08 /pmc/articles/PMC5486050/ /pubmed/28594357 http://dx.doi.org/10.3390/ijms18061227 Text en © 2017 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Majewska, Marta
Lipka, Aleksandra
Panasiewicz, Grzegorz
Gowkielewicz, Marek
Jozwik, Marcin
Majewski, Mariusz Krzysztof
Szafranska, Bozena
Identification of Novel Placentally Expressed Aspartic Proteinase in Humans
title Identification of Novel Placentally Expressed Aspartic Proteinase in Humans
title_full Identification of Novel Placentally Expressed Aspartic Proteinase in Humans
title_fullStr Identification of Novel Placentally Expressed Aspartic Proteinase in Humans
title_full_unstemmed Identification of Novel Placentally Expressed Aspartic Proteinase in Humans
title_short Identification of Novel Placentally Expressed Aspartic Proteinase in Humans
title_sort identification of novel placentally expressed aspartic proteinase in humans
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5486050/
https://www.ncbi.nlm.nih.gov/pubmed/28594357
http://dx.doi.org/10.3390/ijms18061227
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