Circulating syndecan-1 is reduced in pregnancies with poor fetal growth and its secretion regulated by matrix metalloproteinases and the mitochondria

D. Garcha; S.P. Walker; T.M. MacDonald; J. Hyett; J. Jellins; J. Myers; S.E. Illanes; J.K. Nien; M. Schepeler; E. Keenan; C.-A. Whigham; P. Cannon; E. Murray; T.-V. Nguyen; M. Kandel; J. Masci; C. Murphy; T. Cruickshank; N. Pritchard; N.J. Hannan; F. Brownfoot; A. Roddy Mitchell; A. Middleton; G. Pell; G.P. Wong; S. Tong; T.J. Kaitu’u-Lino

doi:10.1038/s41598-021-96077-1

Circulating syndecan-1 is reduced in pregnancies with poor fetal growth and its secretion regulated by matrix metalloproteinases and the mitochondria

D. Garcha, S.P. Walker, T.M. MacDonald, J. Hyett, J. Jellins, J. Myers, S.E. Illanes, J.K. Nien, M. Schepeler, E. Keenan, C.-A. Whigham, P. Cannon, E. Murray, T.-V. Nguyen, M. Kandel, J. Masci, C. Murphy, T. Cruickshank, N. Pritchard, N.J. HannanF. Brownfoot, A. Roddy Mitchell, A. Middleton, G. Pell, G.P. Wong, S. Tong, T.J. Kaitu’u-Lino

Division of Developmental Biology & Medicine (L5)

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Abstract

Fetal growth restriction is a leading cause of stillbirth that often remains undetected during pregnancy. Identifying novel biomarkers may improve detection of pregnancies at risk. This study aimed to assess syndecan-1 as a biomarker for small for gestational age (SGA) or fetal growth restricted (FGR) pregnancies and determine its molecular regulation. Circulating maternal syndecan-1 was measured in several cohorts; a large prospective cohort collected around 36 weeks’ gestation (n = 1206), a case control study from the Manchester Antenatal Vascular service (285 women sampled at 24–34 weeks’ gestation); two prospective cohorts collected on the day of delivery (36 + 3–41 + 3 weeks’ gestation, n = 562 and n = 405 respectively) and a cohort who delivered for preterm FGR (< 34 weeks). Circulating syndecan-1 was consistently reduced in women destined to deliver growth restricted infants and those delivering for preterm disease. Syndecan-1 secretion was reduced by hypoxia, and its loss impaired proliferation. Matrix metalloproteinases and mitochondrial electron transport chain inhibitors significantly reduced syndecan-1 secretion, an effect that was rescued by coadministration of succinate, a mitochondrial electron transport chain activator. In conclusion, circulating syndecan-1 is reduced among cases of term and preterm growth restriction and has potential for inclusion in multi-marker algorithms to improve detection of poorly grown fetuses.

Original language	English
Article number	16595
Journal	Scientific Reports
Volume	11
Issue number	1
DOIs	https://doi.org/10.1038/s41598-021-96077-1
Publication status	Published - 16 Aug 2021

Keywords

Adult
Area Under Curve
Birth Weight
Cell Hypoxia
Delivery, Obstetric
Diabetes, Gestational/blood
Electron Transport/drug effects
Female
Fetal Growth Retardation/blood
Gestational Age
Humans
Hypertension/blood
Infant, Newborn
Infant, Small for Gestational Age
Matrix Metalloproteinases/physiology
Metformin/pharmacology
Mitochondria/drug effects
Organ Size
Overweight/blood
Placenta/metabolism
Pre-Eclampsia/blood
Pregnancy
Pregnancy Complications/blood
ROC Curve
Smoking/blood
Syndecan-1/blood
Trophoblasts/enzymology

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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Garcha, D., Walker, S. P., MacDonald, T. M., Hyett, J., Jellins, J., Myers, J., Illanes, S. E., Nien, J. K., Schepeler, M., Keenan, E., Whigham, C.-A., Cannon, P., Murray, E., Nguyen, T.-V., Kandel, M., Masci, J., Murphy, C., Cruickshank, T., Pritchard, N., ... Kaitu’u-Lino, T. J. (2021). Circulating syndecan-1 is reduced in pregnancies with poor fetal growth and its secretion regulated by matrix metalloproteinases and the mitochondria. Scientific Reports, 11(1), Article 16595. https://doi.org/10.1038/s41598-021-96077-1

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title = "Circulating syndecan-1 is reduced in pregnancies with poor fetal growth and its secretion regulated by matrix metalloproteinases and the mitochondria",

abstract = "Fetal growth restriction is a leading cause of stillbirth that often remains undetected during pregnancy. Identifying novel biomarkers may improve detection of pregnancies at risk. This study aimed to assess syndecan-1 as a biomarker for small for gestational age (SGA) or fetal growth restricted (FGR) pregnancies and determine its molecular regulation. Circulating maternal syndecan-1 was measured in several cohorts; a large prospective cohort collected around 36 weeks{\textquoteright} gestation (n = 1206), a case control study from the Manchester Antenatal Vascular service (285 women sampled at 24–34 weeks{\textquoteright} gestation); two prospective cohorts collected on the day of delivery (36 + 3–41 + 3 weeks{\textquoteright} gestation, n = 562 and n = 405 respectively) and a cohort who delivered for preterm FGR (< 34 weeks). Circulating syndecan-1 was consistently reduced in women destined to deliver growth restricted infants and those delivering for preterm disease. Syndecan-1 secretion was reduced by hypoxia, and its loss impaired proliferation. Matrix metalloproteinases and mitochondrial electron transport chain inhibitors significantly reduced syndecan-1 secretion, an effect that was rescued by coadministration of succinate, a mitochondrial electron transport chain activator. In conclusion, circulating syndecan-1 is reduced among cases of term and preterm growth restriction and has potential for inclusion in multi-marker algorithms to improve detection of poorly grown fetuses.",

keywords = "Adult, Area Under Curve, Birth Weight, Cell Hypoxia, Delivery, Obstetric, Diabetes, Gestational/blood, Electron Transport/drug effects, Female, Fetal Growth Retardation/blood, Gestational Age, Humans, Hypertension/blood, Infant, Newborn, Infant, Small for Gestational Age, Matrix Metalloproteinases/physiology, Metformin/pharmacology, Mitochondria/drug effects, Organ Size, Overweight/blood, Placenta/metabolism, Pre-Eclampsia/blood, Pregnancy, Pregnancy Complications/blood, ROC Curve, Smoking/blood, Syndecan-1/blood, Trophoblasts/enzymology",

author = "D. Garcha and S.P. Walker and T.M. MacDonald and J. Hyett and J. Jellins and J. Myers and S.E. Illanes and J.K. Nien and M. Schepeler and E. Keenan and C.-A. Whigham and P. Cannon and E. Murray and T.-V. Nguyen and M. Kandel and J. Masci and C. Murphy and T. Cruickshank and N. Pritchard and N.J. Hannan and F. Brownfoot and {Roddy Mitchell}, A. and A. Middleton and G. Pell and G.P. Wong and S. Tong and T.J. Kaitu{\textquoteright}u-Lino",

note = "Funding Information: Funding for this work was provided by the National Health and Medical Research Council (#1065854, #1183854, #116071), an Australian Government Research Training Program Scholarship, and RANZCOG Taylor Hammond Scholarship to TM; National Health and Medical Research Council Fellowships to TKL (#1159261), NJH (#1146128), ST (#1136418). The funders played no role in study design or analysis. Funding Information: from the RIKEN BRC through the National BioResource Project of the MEXT/AMED, Japan and cultured according to the publication from Okae and colleagues28. Syncytiotrophoblasts were differentiated from cyto-trophoblasts as previously described28. Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = aug,

day = "16",

doi = "10.1038/s41598-021-96077-1",

language = "English",

volume = "11",

journal = "Scientific Reports",

issn = "2045-2322",

publisher = "Nature Research",

number = "1",

}

Garcha, D, Walker, SP, MacDonald, TM, Hyett, J, Jellins, J, Myers, J, Illanes, SE, Nien, JK, Schepeler, M, Keenan, E, Whigham, C-A, Cannon, P, Murray, E, Nguyen, T-V, Kandel, M, Masci, J, Murphy, C, Cruickshank, T, Pritchard, N, Hannan, NJ, Brownfoot, F, Roddy Mitchell, A, Middleton, A, Pell, G, Wong, GP, Tong, S & Kaitu’u-Lino, TJ 2021, 'Circulating syndecan-1 is reduced in pregnancies with poor fetal growth and its secretion regulated by matrix metalloproteinases and the mitochondria', Scientific Reports, vol. 11, no. 1, 16595. https://doi.org/10.1038/s41598-021-96077-1

TY - JOUR

T1 - Circulating syndecan-1 is reduced in pregnancies with poor fetal growth and its secretion regulated by matrix metalloproteinases and the mitochondria

AU - Garcha, D.

AU - Walker, S.P.

AU - MacDonald, T.M.

AU - Hyett, J.

AU - Jellins, J.

AU - Myers, J.

AU - Illanes, S.E.

AU - Nien, J.K.

AU - Schepeler, M.

AU - Keenan, E.

AU - Whigham, C.-A.

AU - Cannon, P.

AU - Murray, E.

AU - Nguyen, T.-V.

AU - Kandel, M.

AU - Masci, J.

AU - Murphy, C.

AU - Cruickshank, T.

AU - Pritchard, N.

AU - Hannan, N.J.

AU - Brownfoot, F.

AU - Roddy Mitchell, A.

AU - Middleton, A.

AU - Pell, G.

AU - Wong, G.P.

AU - Tong, S.

AU - Kaitu’u-Lino, T.J.

N1 - Funding Information: Funding for this work was provided by the National Health and Medical Research Council (#1065854, #1183854, #116071), an Australian Government Research Training Program Scholarship, and RANZCOG Taylor Hammond Scholarship to TM; National Health and Medical Research Council Fellowships to TKL (#1159261), NJH (#1146128), ST (#1136418). The funders played no role in study design or analysis. Funding Information: from the RIKEN BRC through the National BioResource Project of the MEXT/AMED, Japan and cultured according to the publication from Okae and colleagues28. Syncytiotrophoblasts were differentiated from cyto-trophoblasts as previously described28. Publisher Copyright: © 2021, The Author(s).

PY - 2021/8/16

Y1 - 2021/8/16

N2 - Fetal growth restriction is a leading cause of stillbirth that often remains undetected during pregnancy. Identifying novel biomarkers may improve detection of pregnancies at risk. This study aimed to assess syndecan-1 as a biomarker for small for gestational age (SGA) or fetal growth restricted (FGR) pregnancies and determine its molecular regulation. Circulating maternal syndecan-1 was measured in several cohorts; a large prospective cohort collected around 36 weeks’ gestation (n = 1206), a case control study from the Manchester Antenatal Vascular service (285 women sampled at 24–34 weeks’ gestation); two prospective cohorts collected on the day of delivery (36 + 3–41 + 3 weeks’ gestation, n = 562 and n = 405 respectively) and a cohort who delivered for preterm FGR (< 34 weeks). Circulating syndecan-1 was consistently reduced in women destined to deliver growth restricted infants and those delivering for preterm disease. Syndecan-1 secretion was reduced by hypoxia, and its loss impaired proliferation. Matrix metalloproteinases and mitochondrial electron transport chain inhibitors significantly reduced syndecan-1 secretion, an effect that was rescued by coadministration of succinate, a mitochondrial electron transport chain activator. In conclusion, circulating syndecan-1 is reduced among cases of term and preterm growth restriction and has potential for inclusion in multi-marker algorithms to improve detection of poorly grown fetuses.

AB - Fetal growth restriction is a leading cause of stillbirth that often remains undetected during pregnancy. Identifying novel biomarkers may improve detection of pregnancies at risk. This study aimed to assess syndecan-1 as a biomarker for small for gestational age (SGA) or fetal growth restricted (FGR) pregnancies and determine its molecular regulation. Circulating maternal syndecan-1 was measured in several cohorts; a large prospective cohort collected around 36 weeks’ gestation (n = 1206), a case control study from the Manchester Antenatal Vascular service (285 women sampled at 24–34 weeks’ gestation); two prospective cohorts collected on the day of delivery (36 + 3–41 + 3 weeks’ gestation, n = 562 and n = 405 respectively) and a cohort who delivered for preterm FGR (< 34 weeks). Circulating syndecan-1 was consistently reduced in women destined to deliver growth restricted infants and those delivering for preterm disease. Syndecan-1 secretion was reduced by hypoxia, and its loss impaired proliferation. Matrix metalloproteinases and mitochondrial electron transport chain inhibitors significantly reduced syndecan-1 secretion, an effect that was rescued by coadministration of succinate, a mitochondrial electron transport chain activator. In conclusion, circulating syndecan-1 is reduced among cases of term and preterm growth restriction and has potential for inclusion in multi-marker algorithms to improve detection of poorly grown fetuses.

KW - Adult

KW - Area Under Curve

KW - Birth Weight

KW - Cell Hypoxia

KW - Delivery, Obstetric

KW - Diabetes, Gestational/blood

KW - Electron Transport/drug effects

KW - Female

KW - Fetal Growth Retardation/blood

KW - Gestational Age

KW - Humans

KW - Hypertension/blood

KW - Infant, Newborn

KW - Infant, Small for Gestational Age

KW - Matrix Metalloproteinases/physiology

KW - Metformin/pharmacology

KW - Mitochondria/drug effects

KW - Organ Size

KW - Overweight/blood

KW - Placenta/metabolism

KW - Pre-Eclampsia/blood

KW - Pregnancy

KW - Pregnancy Complications/blood

KW - ROC Curve

KW - Smoking/blood

KW - Syndecan-1/blood

KW - Trophoblasts/enzymology

U2 - 10.1038/s41598-021-96077-1

DO - 10.1038/s41598-021-96077-1

M3 - Article

C2 - 34400721

SN - 2045-2322

VL - 11

JO - Scientific Reports

JF - Scientific Reports

IS - 1

M1 - 16595

ER -

Circulating syndecan-1 is reduced in pregnancies with poor fetal growth and its secretion regulated by matrix metalloproteinases and the mitochondria

Abstract

Keywords

UN SDGs

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