Proteomic identification of Placental Protein 1 (PP1), PP8, and PP22 and characterization of their placental expression in healthy pregnancies and in preeclampsia

Szilvia Szabo; Katalin Karaszi; Roberto Romero; Eszter Toth; Andras Szilagyi; Zsolt Gelencser; Yi Xu; Andrea Balogh; Gabor Szalai; Petronella Hupuczi; Beata Hargitai; Tibor Krenacs; Eva Hunyadi-Gulyas; Zsuzsanna Darula; Katalin A. Kekesi; Adi L. Tarca; Offer Erez; Gabor Juhasz; Ilona Kovalszky; Zoltan Papp; Nandor Gabor Than

doi:10.1016/j.placenta.2020.05.013

Proteomic identification of Placental Protein 1 (PP1), PP8, and PP22 and characterization of their placental expression in healthy pregnancies and in preeclampsia

Szilvia Szabo, Katalin Karaszi, Roberto Romero, Eszter Toth, Andras Szilagyi, Zsolt Gelencser, Yi Xu, Andrea Balogh, Gabor Szalai, Petronella Hupuczi, Beata Hargitai, Tibor Krenacs, Eva Hunyadi-Gulyas, Zsuzsanna Darula, Katalin A. Kekesi, Adi L. Tarca, Offer Erez, Gabor Juhasz, Ilona Kovalszky, Zoltan PappNandor Gabor Than

Medical School for International Health

Research output: Contribution to journal › Article › peer-review

3 Scopus citations

Abstract

Introduction: Placental Protein 1 (PP1), PP8, and PP22 were isolated from the placenta. Herein, we aimed to identify PP1, PP8, and PP22 proteins and their placental and trophoblastic expression patterns to reveal potential involvement in pregnancy complications. Methods: We analyzed PP1, PP8, and PP22 proteins with LC-MS. We compared the placental behaviors of PP1, PP8, and PP22 to the predominantly placenta-expressed PP5/TFPI-2. Placenta-specificity scores were generated from microarray data. Trophoblasts were isolated from healthy placentas and differentiated; total RNA was isolated and subjected to microarray analysis. We assigned the placentas to the following groups: preterm controls, early-onset preeclampsia, early-onset preeclampsia with HELLP syndrome, term controls, and late-onset preeclampsia. After histopathologic examination, placentas were used for tissue microarray construction, immunostaining with anti-PP1, anti-PP5, anti-PP8, or anti-PP22 antibodies, and immunoscoring. Results: PP1, PP8, and PP22 were identified as ‘nicotinate-nucleotide pyrophosphorylase’, ‘serpin B6’, and ‘protein disulfide-isomerase’, respectively. Genes encoding PP1, PP8, and PP22 are not predominantly placenta-expressed, in contrast with PP5. PP1, PP8, and PP22 mRNA expression levels did not increase during trophoblast differentiation, in contrast with PP5. PP1, PP8, and PP22 immunostaining were detected primarily in trophoblasts, while PP5 expression was restricted to the syncytiotrophoblast. The PP1 immunoscore was higher in late-onset preeclampsia, while the PP5 immunoscore was higher in early-onset preeclampsia. Discussion: PP1, PP8, and PP22 are expressed primarily in trophoblasts but do not have trophoblast-specific regulation or functions. The distinct dysregulation of PP1 and PP5 expression in either late-onset or early-onset preeclampsia reflects different pathophysiological pathways in these preeclampsia subsets.

Original language	English
Pages (from-to)	197-207
Number of pages	11
Journal	Placenta
Volume	99
DOIs	https://doi.org/10.1016/j.placenta.2020.05.013
State	Published - 15 Sep 2020

Keywords

Biomarkers
HELLP syndrome
Immunohistochemistry
Liver dysfunction
Mass spectrometry
Placenta
Preeclampsia
Pregnancy
Small for gestational age
Syncytiotrophoblast
Thrombocytopenia
Tissue microarray
Trophoblast

ASJC Scopus subject areas

Reproductive Medicine
Obstetrics and Gynecology
Developmental Biology

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10.1016/j.placenta.2020.05.013

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Szabo, S., Karaszi, K., Romero, R., Toth, E., Szilagyi, A., Gelencser, Z., Xu, Y., Balogh, A., Szalai, G., Hupuczi, P., Hargitai, B., Krenacs, T., Hunyadi-Gulyas, E., Darula, Z., Kekesi, K. A., Tarca, A. L., Erez, O., Juhasz, G., Kovalszky, I., ... Than, N. G. (2020). Proteomic identification of Placental Protein 1 (PP1), PP8, and PP22 and characterization of their placental expression in healthy pregnancies and in preeclampsia. Placenta, 99, 197-207. https://doi.org/10.1016/j.placenta.2020.05.013

@article{1b8d4e898c87464b8b2419cb18c571e2,

title = "Proteomic identification of Placental Protein 1 (PP1), PP8, and PP22 and characterization of their placental expression in healthy pregnancies and in preeclampsia",

abstract = "Introduction: Placental Protein 1 (PP1), PP8, and PP22 were isolated from the placenta. Herein, we aimed to identify PP1, PP8, and PP22 proteins and their placental and trophoblastic expression patterns to reveal potential involvement in pregnancy complications. Methods: We analyzed PP1, PP8, and PP22 proteins with LC-MS. We compared the placental behaviors of PP1, PP8, and PP22 to the predominantly placenta-expressed PP5/TFPI-2. Placenta-specificity scores were generated from microarray data. Trophoblasts were isolated from healthy placentas and differentiated; total RNA was isolated and subjected to microarray analysis. We assigned the placentas to the following groups: preterm controls, early-onset preeclampsia, early-onset preeclampsia with HELLP syndrome, term controls, and late-onset preeclampsia. After histopathologic examination, placentas were used for tissue microarray construction, immunostaining with anti-PP1, anti-PP5, anti-PP8, or anti-PP22 antibodies, and immunoscoring. Results: PP1, PP8, and PP22 were identified as {\textquoteleft}nicotinate-nucleotide pyrophosphorylase{\textquoteright}, {\textquoteleft}serpin B6{\textquoteright}, and {\textquoteleft}protein disulfide-isomerase{\textquoteright}, respectively. Genes encoding PP1, PP8, and PP22 are not predominantly placenta-expressed, in contrast with PP5. PP1, PP8, and PP22 mRNA expression levels did not increase during trophoblast differentiation, in contrast with PP5. PP1, PP8, and PP22 immunostaining were detected primarily in trophoblasts, while PP5 expression was restricted to the syncytiotrophoblast. The PP1 immunoscore was higher in late-onset preeclampsia, while the PP5 immunoscore was higher in early-onset preeclampsia. Discussion: PP1, PP8, and PP22 are expressed primarily in trophoblasts but do not have trophoblast-specific regulation or functions. The distinct dysregulation of PP1 and PP5 expression in either late-onset or early-onset preeclampsia reflects different pathophysiological pathways in these preeclampsia subsets.",

keywords = "Biomarkers, HELLP syndrome, Immunohistochemistry, Liver dysfunction, Mass spectrometry, Placenta, Preeclampsia, Pregnancy, Small for gestational age, Syncytiotrophoblast, Thrombocytopenia, Tissue microarray, Trophoblast",

author = "Szilvia Szabo and Katalin Karaszi and Roberto Romero and Eszter Toth and Andras Szilagyi and Zsolt Gelencser and Yi Xu and Andrea Balogh and Gabor Szalai and Petronella Hupuczi and Beata Hargitai and Tibor Krenacs and Eva Hunyadi-Gulyas and Zsuzsanna Darula and Kekesi, {Katalin A.} and Tarca, {Adi L.} and Offer Erez and Gabor Juhasz and Ilona Kovalszky and Zoltan Papp and Than, {Nandor Gabor}",

note = "Publisher Copyright: {\textcopyright} 2020",

year = "2020",

month = sep,

day = "15",

doi = "10.1016/j.placenta.2020.05.013",

language = "English",

volume = "99",

pages = "197--207",

journal = "Placenta",

issn = "0143-4004",

publisher = "W.B. Saunders Ltd",

}

Szabo, S, Karaszi, K, Romero, R, Toth, E, Szilagyi, A, Gelencser, Z, Xu, Y, Balogh, A, Szalai, G, Hupuczi, P, Hargitai, B, Krenacs, T, Hunyadi-Gulyas, E, Darula, Z, Kekesi, KA, Tarca, AL, Erez, O, Juhasz, G, Kovalszky, I, Papp, Z & Than, NG 2020, 'Proteomic identification of Placental Protein 1 (PP1), PP8, and PP22 and characterization of their placental expression in healthy pregnancies and in preeclampsia', Placenta, vol. 99, pp. 197-207. https://doi.org/10.1016/j.placenta.2020.05.013

TY - JOUR

T1 - Proteomic identification of Placental Protein 1 (PP1), PP8, and PP22 and characterization of their placental expression in healthy pregnancies and in preeclampsia

AU - Szabo, Szilvia

AU - Karaszi, Katalin

AU - Romero, Roberto

AU - Toth, Eszter

AU - Szilagyi, Andras

AU - Gelencser, Zsolt

AU - Xu, Yi

AU - Balogh, Andrea

AU - Szalai, Gabor

AU - Hupuczi, Petronella

AU - Hargitai, Beata

AU - Krenacs, Tibor

AU - Hunyadi-Gulyas, Eva

AU - Darula, Zsuzsanna

AU - Kekesi, Katalin A.

AU - Tarca, Adi L.

AU - Erez, Offer

AU - Juhasz, Gabor

AU - Kovalszky, Ilona

AU - Papp, Zoltan

AU - Than, Nandor Gabor

PY - 2020/9/15

Y1 - 2020/9/15

N2 - Introduction: Placental Protein 1 (PP1), PP8, and PP22 were isolated from the placenta. Herein, we aimed to identify PP1, PP8, and PP22 proteins and their placental and trophoblastic expression patterns to reveal potential involvement in pregnancy complications. Methods: We analyzed PP1, PP8, and PP22 proteins with LC-MS. We compared the placental behaviors of PP1, PP8, and PP22 to the predominantly placenta-expressed PP5/TFPI-2. Placenta-specificity scores were generated from microarray data. Trophoblasts were isolated from healthy placentas and differentiated; total RNA was isolated and subjected to microarray analysis. We assigned the placentas to the following groups: preterm controls, early-onset preeclampsia, early-onset preeclampsia with HELLP syndrome, term controls, and late-onset preeclampsia. After histopathologic examination, placentas were used for tissue microarray construction, immunostaining with anti-PP1, anti-PP5, anti-PP8, or anti-PP22 antibodies, and immunoscoring. Results: PP1, PP8, and PP22 were identified as ‘nicotinate-nucleotide pyrophosphorylase’, ‘serpin B6’, and ‘protein disulfide-isomerase’, respectively. Genes encoding PP1, PP8, and PP22 are not predominantly placenta-expressed, in contrast with PP5. PP1, PP8, and PP22 mRNA expression levels did not increase during trophoblast differentiation, in contrast with PP5. PP1, PP8, and PP22 immunostaining were detected primarily in trophoblasts, while PP5 expression was restricted to the syncytiotrophoblast. The PP1 immunoscore was higher in late-onset preeclampsia, while the PP5 immunoscore was higher in early-onset preeclampsia. Discussion: PP1, PP8, and PP22 are expressed primarily in trophoblasts but do not have trophoblast-specific regulation or functions. The distinct dysregulation of PP1 and PP5 expression in either late-onset or early-onset preeclampsia reflects different pathophysiological pathways in these preeclampsia subsets.

AB - Introduction: Placental Protein 1 (PP1), PP8, and PP22 were isolated from the placenta. Herein, we aimed to identify PP1, PP8, and PP22 proteins and their placental and trophoblastic expression patterns to reveal potential involvement in pregnancy complications. Methods: We analyzed PP1, PP8, and PP22 proteins with LC-MS. We compared the placental behaviors of PP1, PP8, and PP22 to the predominantly placenta-expressed PP5/TFPI-2. Placenta-specificity scores were generated from microarray data. Trophoblasts were isolated from healthy placentas and differentiated; total RNA was isolated and subjected to microarray analysis. We assigned the placentas to the following groups: preterm controls, early-onset preeclampsia, early-onset preeclampsia with HELLP syndrome, term controls, and late-onset preeclampsia. After histopathologic examination, placentas were used for tissue microarray construction, immunostaining with anti-PP1, anti-PP5, anti-PP8, or anti-PP22 antibodies, and immunoscoring. Results: PP1, PP8, and PP22 were identified as ‘nicotinate-nucleotide pyrophosphorylase’, ‘serpin B6’, and ‘protein disulfide-isomerase’, respectively. Genes encoding PP1, PP8, and PP22 are not predominantly placenta-expressed, in contrast with PP5. PP1, PP8, and PP22 mRNA expression levels did not increase during trophoblast differentiation, in contrast with PP5. PP1, PP8, and PP22 immunostaining were detected primarily in trophoblasts, while PP5 expression was restricted to the syncytiotrophoblast. The PP1 immunoscore was higher in late-onset preeclampsia, while the PP5 immunoscore was higher in early-onset preeclampsia. Discussion: PP1, PP8, and PP22 are expressed primarily in trophoblasts but do not have trophoblast-specific regulation or functions. The distinct dysregulation of PP1 and PP5 expression in either late-onset or early-onset preeclampsia reflects different pathophysiological pathways in these preeclampsia subsets.

KW - Biomarkers

KW - HELLP syndrome

KW - Immunohistochemistry

KW - Liver dysfunction

KW - Mass spectrometry

KW - Placenta

KW - Preeclampsia

KW - Pregnancy

KW - Small for gestational age

KW - Syncytiotrophoblast

KW - Thrombocytopenia

KW - Tissue microarray

KW - Trophoblast

UR - http://www.scopus.com/inward/record.url?scp=85088863894&partnerID=8YFLogxK

U2 - 10.1016/j.placenta.2020.05.013

DO - 10.1016/j.placenta.2020.05.013

M3 - Article

C2 - 32747003

AN - SCOPUS:85088863894

SN - 0143-4004

VL - 99

SP - 197

EP - 207

JO - Placenta

JF - Placenta

ER -

Proteomic identification of Placental Protein 1 (PP1), PP8, and PP22 and characterization of their placental expression in healthy pregnancies and in preeclampsia

Abstract

Keywords

ASJC Scopus subject areas

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