GLUT4 expression and subcellular localization in the intrauterine growth-restricted adult rat female offspring

Thamotharan, Manikkavasagar; Shin, Bo‐Chul; Suddirikku, Dilika T.; Thamotharan, Shanthie; Garg, Meena; Devaskar, Sherin U.

doi:10.1152/ajpendo.00342.2004

Cited by 80 publications

(159 citation statements)

References 65 publications

(95 reference statements)

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“…Thamotharan et al (2005) demonstrated that maternal caloric restriction programmed aberrant SLC2A4 cellular distribution, but in this case skeletal muscle SLC2A4 was concentrated in the plasma membrane rather than the cytoplasm, and further translocation was not induced by insulin. These authors suggested that this aberration reflects heightened basal insulin sensitivity in the face of caloric restriction that leads to subsequent glucose intolerance when postnatal nutrition is adequate (Thamotharan et al 2005).…”

Section: Discussionmentioning

confidence: 81%

“…Similar impairment in SLC2A4 translocation occurs in adipocytes isolated from the s.c. fat of diabetic patients (Maianu et al 2001), and it has been suggested that impaired ATP synthesis in skeletal muscle of rats following intrauterine growth retardation may compromise energy-dependent SLC2A4 recruitment to the cell surface (Selak et al 2003). Thamotharan et al (2005) demonstrated that maternal caloric restriction programmed aberrant SLC2A4 cellular distribution, but in this case skeletal muscle SLC2A4 was concentrated in the plasma membrane rather than the cytoplasm, and further translocation was not induced by insulin. These authors suggested that this aberration reflects heightened basal insulin sensitivity in the face of caloric restriction that leads to subsequent glucose intolerance when postnatal nutrition is adequate (Thamotharan et al 2005).…”

Section: Discussionmentioning

confidence: 98%

“…Alterations in skeletal muscle insulin regulated Slc2a4 expression and/or function may also be central to programmed disturbances in glycemic control, since prenatal ethanol exposure in rats (Chen & Nyomba 2003) and nutrient restriction in sheep (Gardner et al 2005) both reduce Slc2a4 expression in glucose-intolerant offspring. Maternal calorie restriction has also been shown to compromise insulininduced translocation of SLC2A4 to the plasma membrane (Thamotharan et al 2005).…”

Section: Introductionmentioning

confidence: 99%

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Developmental programming of adult hyperinsulinemia, increased proinflammatory cytokine production, and altered skeletal muscle expression of SLC2A4 (GLUT4) and uncoupling protein 3

Wyrwoll¹,

Mark²,

Mori³

et al. 2008

Journal of Endocrinology

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Fetal glucocorticoid excess programs detrimental effects in the adult phenotype including hyperleptinemia and aberrant glycemic control. In this study, we determined the interactive effects of maternal dexamethasone (Dex) treatment and postnatal dietary u-3 (n-3) fatty acids on adult proinflammatory cytokine production and skeletal muscle expression of genes central to glucose handling and fatty acid metabolism. Dex acetate was administered to pregnant rats (0 . 75 mg/ml drinking water) from day 13 to term. Offspring of treated and control mothers were cross-fostered to mothers on either a standard (Std) or high n-3 (Hn3) diet, and remained on these diets postweaning. Adult offspring exposed to Dex in utero exhibited fasting hyperinsulinemia when raised on the Std diet but not when raised on the Hn3 diet. Dex also programmed increased plasma tumour necrosis factora and interleukin 1b (IL-1b), but the increase in IL-1b was also prevented by the Hn3 diet. In skeletal muscle, expression of insulin regulated Slc2a4 (formerly known as GLUT4) was elevated (up to 15-fold) after Dex in utero, and this resulted in elevated intracellular, but not membrane-associated, SLC2A4 protein. Fetal glucocorticoid excess also reduced adult skeletal muscle Ucp3 expression in all offspring, whereas skeletal muscle expression of both Ppard and Ppargc1a were increased in females but not males. In conclusion, our data show that fetal glucocorticoid excess programs adult hyperinsulinemia and increased proinflammatory cytokine production. Related changes in the skeletal muscle Slc2a4, Ucp3, and Ppard indicate that fetal glucocorticoid excess disturbs adult glucose/fatty acid transport and metabolism.

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Section: Discussionmentioning

confidence: 81%

Section: Discussionmentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

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Developmental programming of adult hyperinsulinemia, increased proinflammatory cytokine production, and altered skeletal muscle expression of SLC2A4 (GLUT4) and uncoupling protein 3

Wyrwoll¹,

Mark²,

Mori³

et al. 2008

Journal of Endocrinology

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“…In the rat, fetal skeletal muscle GLUT4 expression is decreased, but the amount of GLUT4 present on the plasma membrane is increased, with diminished intracellular stores, suggesting a compensatory adaptation to low glucose availability. 13 In the adult IUGR rat, skeletal muscle GLUT4 continues to be increased on the plasma membrane but there is diminished translocation of additional GLUT4 to the plasma membrane in response to insulin. Adult IUGR human subjects with insulin resistance also demonstrated a failure to upregulate muscle GLUT4 after insulin stimulation.…”

Section: Diabetesmentioning

confidence: 99%

Adult Sequelae of Intrauterine Growth Restriction

Ross

Beall

2008

Seminars in Perinatology

158

111

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Fetal intrauterine growth restriction has been associated with adult disease in both human epidemiologic studies and in animal models. In some cases, intrauterine deprivation programs the fetus to develop increased appetite and obesity, hypertension and diabetes as an adult. Although the mechanisms responsible for fetal programming remain poorly understood, both anatomic and functional (cell signaling) changes have been described in affected individuals. In some animal models, aspects of fetal programming can be reversed postnatally, however at the present time the best strategy for avoiding the adult consequences of fetal growth restriction is prevention.Fetal intrauterine growth restriction (IUGR) occurs in humans as a consequence of poor maternal nutrition, placental insufficiency and diminished fetal oxygenation, or exposure to teratogens, among other causes. In animals, and in some cases in humans, IUGR from these causes has been associated with the development of adult diseases; this phenomenon is called "fetal programming". The association of maladaptive programming with adult disease has been termed the "Barker hypothesis". In general, the Barker hypothesis 1 contends that the malnourished fetus is programmed to exhibit a "thrifty phenotype" with increased food intake and fat deposition and possibly decreased energy output. Faced with ample available calories, such individuals develop obesity and other manifestations of the metabolic syndrome as adults due to alterations in homeostatic regulatory mechanisms. 2-4The issue of fetal programming is not merely of intellectual interest. Currently, 65% of adults in the United States are overweight and almost one in three are obese (BMI>30 kg/m 2 ), representing a modern health crisis. 5 Obesity and its related diseases are the leading cause of death in Western society, with associated risks of hypertension, coronary heart disease, stroke, diabetes, and breast, prostate and colon cancer. Evidence indicates a striking 25 to 63% of adult diabetes, hypertension and coronary heart disease can be attributed to the effects of low birthweight with accelerated newborn-to-adolescent weight gain. 2 therefore gestational programming of low birth weight/ IUGR has contributed importantly to the population shift towards obesity. In Western societies, the incidence of low birth weight infants has increased since the mid-twentieth century. Low birth weight infants are now being born to women with chronic diseases who would previously have had limited survival and reproductive capacity, while assisted reproductive technologies and increasing numbers of multiple gestations have resulted in both preterm and low birth weight offspring. When combined with improved

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“…Esto podría ser el resultado de alteraciones en la placenta o del metabolismo de la glucosa fetal (9). Niveles bajos de glucosa también han sido encontrados en niños con RCIU cuyas madres presentan niveles normales, sugiriendo disminución de la transferencia de glucosa a través de la placenta, presumiblemente debido a los transportadores de glucosa (10,11).…”

Section: Rciu Y Glucosaunclassified

Retardo de Crecimiento Intrauterino (Rciu) y Sus Alteraciones Bioquímicas.

Molina

Barbosa²

2005

nova

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IntroducciónEl RCIU se define como aquella circunstancia clínica en la cual el feto no alcanza su pleno potencial de crecimiento; como resultado final ocurre una disminución en el peso corporal, el cual queda por debajo del percentil 10 para la edad gestacional según tablas de crecimiento (1). Aunque la mayoría de los niños que nacen con RCIU alcanzan una talla adecuada, especialmente durante el primer año de vida (2), aproximadamente entre un 15-20 % presentan talla baja (3).Piel laxa, delgada, tejido graso subcutáneo reducido, abdomen excavado y grasa muscular de brazos, glúteos y muslos disminuida son características físi-cas de los neonatos con RCIU. Esta patología se considera una condición multifactorial donde están incluidos aspectos fisiopatológicos fetales, placentarios y maternos, entre los que se destacan reducción de nutrientes y disponibilidad de oxígeno, ingestión de drogas, disminución de la masa y flujo placentario, infección congénita y anomalías cromosómicas (4). El RCIU está asociado con un incremento en la morbilidad y mortalidad fetal antes y después del nacimiento (5,6). Basándose en el índice ponderal el RCIU puede presentarse bajo dos formas, RCIU simétrico y RCIU asimétrico (7). ResumenEl estudio del retardo de crecimiento intrauterino (RCIU) continúa siendo importante tanto a nivel obsté-trico como pediátrico. El interés se centra en los factores que inciden directamente en las fallas de crecimiento in útero y sobre sus consecuencias postnatales. Además del potencial genético, heredado de los padres, el desarrollo y supervivencia del feto depende directamente del suministro de los sustratos necesarios, como azúcares, ácidos grasos, proteínas, aminoácidos; de esta manera alcanza su peso potencial. Si la disponibilidad de estas fuentes disminuyen en forma persistente, la supervivencia del feto puede verse amenazada. En este artículo se hace una revisión sobre el papel que tienen dichas fuentes y sus alteraciones e implicaciones en los casos de RCIU. AbstractThe study of the retard of intra-uterine (RCIU) growth continues being important so much at obstetric level as pediatric. The interest is centered in the factors that impact directly in the flaws of growth in uterus and on its postnatal consequences. Besides the genetic potential, inherited of the parents, the development and survival of the fetus depends directly on the supply of the necessary substrates, as sugars, fatty acid, proteins, amino acids; this way it reaches its potential weight. If the readiness of these sources diminishes in persistent form, the survival of the fetus can it turns threatened. In this article a revision is made on the paper that have this sources and its alterations and implications in the cases of RCIU.

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GLUT4 expression and subcellular localization in the intrauterine growth-restricted adult rat female offspring

Cited by 80 publications

References 65 publications

Developmental programming of adult hyperinsulinemia, increased proinflammatory cytokine production, and altered skeletal muscle expression of SLC2A4 (GLUT4) and uncoupling protein 3

Developmental programming of adult hyperinsulinemia, increased proinflammatory cytokine production, and altered skeletal muscle expression of SLC2A4 (GLUT4) and uncoupling protein 3

Adult Sequelae of Intrauterine Growth Restriction

Retardo de Crecimiento Intrauterino (Rciu) y Sus Alteraciones Bioquímicas.

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