Asymmetric syncytial expression of GLUT9 splice variants in human term placenta and alterations in diabetic pregnancies

Kristin P. Bibee; Nicholas P. Illsley; Kelle H. Moley

doi:10.1177/1933719110380276

Asymmetric syncytial expression of GLUT9 splice variants in human term placenta and alterations in diabetic pregnancies

Kristin P. Bibee, Nicholas P. Illsley, Kelle H. Moley

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

36 Scopus citations

Abstract

Glucose transport from the maternal to fetal side of the placenta is critical for fetal growth and development due to the absence of fetal gluconeogenesis. Human GLUT9, existing as 2 isoforms, is a novel member of the transporter family. This study investigated the localization and relative expression levels of these isoforms in the human term placenta from both control and diabetic patients. Placenta samples were collected from normal pregnancies and those complicated by maternal diabetes (White classifications A1, A2, and B). Antibodies specific for the different isoforms were used to detect expression. Both forms of the protein are expressed in syncytiotrophoblast cells. Subcellular fractionation revealed an asymmetrical expression pattern with GLUT9a on basal membranes, whereas GLUT9b localizes to microvillus membranes. Expression of both isoforms is significantly increased in placental tissue from diabetic pregnancies. Altered expression of GLUT9 in the placenta may play a role in the fetal pathophysiology associated with diabetes-complicated pregnancies.

Original language	English (US)
Pages (from-to)	20-27
Number of pages	8
Journal	Reproductive Sciences
Volume	18
Issue number	1
DOIs	https://doi.org/10.1177/1933719110380276
State	Published - Jan 2011
Externally published	Yes

Keywords

Basal membrane
Glucose transport
Maternal diabetes
Microvillus membrane
Syncytiotrophoblast

ASJC Scopus subject areas

Obstetrics and Gynecology

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10.1177/1933719110380276

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title = "Asymmetric syncytial expression of GLUT9 splice variants in human term placenta and alterations in diabetic pregnancies",

abstract = "Glucose transport from the maternal to fetal side of the placenta is critical for fetal growth and development due to the absence of fetal gluconeogenesis. Human GLUT9, existing as 2 isoforms, is a novel member of the transporter family. This study investigated the localization and relative expression levels of these isoforms in the human term placenta from both control and diabetic patients. Placenta samples were collected from normal pregnancies and those complicated by maternal diabetes (White classifications A1, A2, and B). Antibodies specific for the different isoforms were used to detect expression. Both forms of the protein are expressed in syncytiotrophoblast cells. Subcellular fractionation revealed an asymmetrical expression pattern with GLUT9a on basal membranes, whereas GLUT9b localizes to microvillus membranes. Expression of both isoforms is significantly increased in placental tissue from diabetic pregnancies. Altered expression of GLUT9 in the placenta may play a role in the fetal pathophysiology associated with diabetes-complicated pregnancies.",

keywords = "Basal membrane, Glucose transport, Maternal diabetes, Microvillus membrane, Syncytiotrophoblast",

author = "Bibee, {Kristin P.} and Illsley, {Nicholas P.} and Moley, {Kelle H.}",

note = "Funding Information: The author(s) disclosed receipt of the following financial support for the research and/or authorship of this article: Grant from NIH R01 HD04390 (KHM) and a research grant from the American Diabetes Association (KHM) .",

year = "2011",

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language = "English (US)",

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AU - Bibee, Kristin P.

AU - Illsley, Nicholas P.

AU - Moley, Kelle H.

N1 - Funding Information: The author(s) disclosed receipt of the following financial support for the research and/or authorship of this article: Grant from NIH R01 HD04390 (KHM) and a research grant from the American Diabetes Association (KHM) .

PY - 2011/1

Y1 - 2011/1

N2 - Glucose transport from the maternal to fetal side of the placenta is critical for fetal growth and development due to the absence of fetal gluconeogenesis. Human GLUT9, existing as 2 isoforms, is a novel member of the transporter family. This study investigated the localization and relative expression levels of these isoforms in the human term placenta from both control and diabetic patients. Placenta samples were collected from normal pregnancies and those complicated by maternal diabetes (White classifications A1, A2, and B). Antibodies specific for the different isoforms were used to detect expression. Both forms of the protein are expressed in syncytiotrophoblast cells. Subcellular fractionation revealed an asymmetrical expression pattern with GLUT9a on basal membranes, whereas GLUT9b localizes to microvillus membranes. Expression of both isoforms is significantly increased in placental tissue from diabetic pregnancies. Altered expression of GLUT9 in the placenta may play a role in the fetal pathophysiology associated with diabetes-complicated pregnancies.

AB - Glucose transport from the maternal to fetal side of the placenta is critical for fetal growth and development due to the absence of fetal gluconeogenesis. Human GLUT9, existing as 2 isoforms, is a novel member of the transporter family. This study investigated the localization and relative expression levels of these isoforms in the human term placenta from both control and diabetic patients. Placenta samples were collected from normal pregnancies and those complicated by maternal diabetes (White classifications A1, A2, and B). Antibodies specific for the different isoforms were used to detect expression. Both forms of the protein are expressed in syncytiotrophoblast cells. Subcellular fractionation revealed an asymmetrical expression pattern with GLUT9a on basal membranes, whereas GLUT9b localizes to microvillus membranes. Expression of both isoforms is significantly increased in placental tissue from diabetic pregnancies. Altered expression of GLUT9 in the placenta may play a role in the fetal pathophysiology associated with diabetes-complicated pregnancies.

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KW - Maternal diabetes

KW - Microvillus membrane

KW - Syncytiotrophoblast

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Asymmetric syncytial expression of GLUT9 splice variants in human term placenta and alterations in diabetic pregnancies

Abstract

Keywords

ASJC Scopus subject areas

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