Differential effects of leptin on thermoregulation and uncoupling protein abundance in the neonatal lamb

Mostyn, A; Bispham, J; Pearce, Sarah; Evens, Yvonne; Raver, N; Keisler, D.H.; Webb, Robert I.; Stephenson, Terence; Symonds, Michael

doi:10.1096/fj.02-0077fje

Cited by 41 publications

(60 citation statements)

References 50 publications

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“…This could either be a direct response or by promoting the conversion of T 4 to triiodothyronine by the enzyme 5 0 -monodeiodinase within BAT (Hall et al 2010). The effect of leptin on perirenal adipose tissue in piglets appears to persist well after its administration had ceased and the magnitude of responses both acutely on body temperature and in the longer term on UCP1 were much greater than those observed previously in neonatal sheep that were normal sized and female (Mostyn et al 2002). This could be because, in young sheep, the rate of loss of BAT and its subsequent replacement with white adipose tissue are possibly much more rapid when compared with pigs, due in part to the concomitant growth of wool, widening of the thermoneutral zone (Symonds 2013) and replacement of non-shivering with shivering thermogenesis as the dominant response to acute cold exposure (Symonds et al 1989).…”

Section: Discussionmentioning

confidence: 74%

“…When administered to female postnatal sheep, leptin improves thermoregulation in the newborn and then subsequently promotes the normal loss of UCP1 in the main fat depot (i.e. perirenal) over the first week of life (Mostyn et al 2002). Daily administration of leptin to piglets showing intrauterine growth restriction (IUGR) between day 2 and day 10 after birth can partially rectify this adverse metabolic phenotype although its effects on adipose tissue appear to be confined to white adipocytes (Attig et al 2008).…”

Section: Introductionmentioning

confidence: 99%

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UCP1 is present in porcine adipose tissue and is responsive to postnatal leptin

Mostyn¹,

Attig²,

Larcher³

et al. 2014

Journal of Endocrinology

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Intrauterine growth restriction (IUGR) may be accompanied by inadequate thermoregulation, especially in piglets that are not considered to possess any brown adipose tissue (BAT) and are thus entirely dependent on shivering thermogenesis in order to maintain body temperature after birth. Leptin can stimulate heat production by promoting non-shivering thermogenesis in BAT, but whether this response occurs in piglets is unknown. Newborn female piglets that were characterised as showing IUGR (mean birth weight of approximately 0.98 kg) were therefore administered injections of either saline or leptin once a day for the first 5 days of neonatal life. The dose of leptin was 0.5 mg/kg, which is sufficient to increase plasma leptin by approximately tenfold and on the day of birth induced a rapid increase in body temperature to values similar to those of normal-sized 'control' piglets (mean birth weight of w1.47 kg). Perirenal adipose tissue was then sampled from all offspring at 21 days of age and the presence of the BAT-specific uncoupling protein 1 (UCP1) was determined by immunohistochemistry and immunoblotting. UCP1 was clearly detectable in all samples analysed and its abundance was significantly reduced in the IUGR piglets that had received saline compared with controls, but was raised to the same amount as in controls in those IUGR females given leptin. There were no differences in gene expression between primary markers of brown and white adipose tissues between groups. In conclusion, piglets possess BAT that when stimulated exogenously by leptin can promote increased body temperature. IntroductionBrown adipose tissue (BAT) is essential for effective adaptation to cold exposure of the extra-uterine environment in precocial species such as sheep in which there is rapid activation of BAT around the time of birth (Clarke et al. 1997). In pigs, however, it has long been considered that BAT is not present (Trayhurn et al. 1989) and the newborn is Journal of Endocrinology Thematic ResearchA MOSTYN and others UCP1 and leptin in porcine 223:1 M31-M38http://joe.endocrinology-journals.org Ñ 2014 Society for Endocrinology DOI: 10.1530/JOE-14-0155Printed in Great BritainPublished by Bioscientifica Ltd.primarily dependent on shivering thermogenesis in muscle in order to prevent hypothermia at birth (Symonds & Lomax 1992). This due to an open reading frame on the BAT-specific uncoupling protein 1 (UCP1) gene in the porcine species meaning that UCP1 is not expressed (Berg et al. 2006). However, it has more recently been suggested that BAT is present in young piglets because of the different morphological appearances of adipocytes within perirenal adipose tissue in 2-week-old females (Attig et al. 2008). However, this remains to be confirmed by direct measurements of UCP1. Moreover, our understanding of BAT has now been transformed as a consequence of the discovery of beige adipocytes that express UCP1 at approximately 10% of the amount observed in classical BAT , Wu et al. 2013, but whether comparable depots are be pr...

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Section: Discussionmentioning

confidence: 74%

Section: Introductionmentioning

confidence: 99%

UCP1 is present in porcine adipose tissue and is responsive to postnatal leptin

Mostyn¹,

Attig²,

Larcher³

et al. 2014

Journal of Endocrinology

Self Cite

View full text Add to dashboard Cite

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“…In the human fetus, plasma leptin concentrations increase with gestational age (Yuen et al 1999, Cetin et al 2000. In the newborn sheep, plasma leptin concentrations decline during the immediate 6 h after birth to then increase up to 7 days of age (Bispham et al 2002). These temporal changes in leptin coincide with development of the hypothalamic-pituitary-adrenal axis with respect to the regulation of cortisol production coincident with the rapid activation of uncoupling protein (UCP)-1, which is unique to brown adipose tissue (BAT) (Clarke et al 1997a, Ricquier & Bouillaud 2000, and is followed by the gradual loss of UCP1 (Clarke et al 1997b).…”

Section: Introductionmentioning

confidence: 99%

“…These temporal changes in leptin coincide with development of the hypothalamic-pituitary-adrenal axis with respect to the regulation of cortisol production coincident with the rapid activation of uncoupling protein (UCP)-1, which is unique to brown adipose tissue (BAT) (Clarke et al 1997a, Ricquier & Bouillaud 2000, and is followed by the gradual loss of UCP1 (Clarke et al 1997b). In the neonatal sheep, leptin administration results in reduced UCP1 mRNA and protein abundance, in conjunction with maintained colonic temperature and plasma non-esterified fatty acid (NEFA) concentration, therefore not affecting thermogenic potential (Mostyn et al 2002). The peak in UCP1 abundance at birth is accompanied by parallel increases in other mitochondrial proteins including the voltage-dependent anion channel (VDAC) located on the outer mitochondrial membrane, and cytochrome c, present within the inter-membrane space (Mostyn et al 2003).…”

Section: Introductionmentioning

confidence: 99%

“…These changes in body temperature have been linked to increased abundance of UCP1 (Scarpace et al 1997) andUCP2 (Gong et al 1997) in BAT by some studies, but not by others (Memon et al 2000). Moreover, these changes appear to be unique to rodents, as leptin treatment of large mammals, such as sheep and pigs, has been found to have a minor role in thermogenesis (Mostyn et al 2002, Litten et al 2004.…”

Section: Introductionmentioning

confidence: 99%

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Tissue-specific effects of leptin administration on the abundance of mitochondrial proteins during neonatal development

Gnanalingham¹,

Mostyn²,

Wang³

et al. 2005

Journal of Endocrinology

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Many tissues undergo a rapid transition after birth, accompanied by dramatic changes in mitochondrial protein function. In particular, uncoupling protein (UCP) abundance increases at birth in the lung and adipose tissue, to then gradually decline, an adaptation that is important in enabling normal tissue function. Leptin potentially mediates some of these changes and is known to promote the loss of UCP1 from brown fat but its effects on UCP2 and related mitochondrial proteins (i.e. voltage-dependent anion channel (VDAC) and cytochrome c) in other tissues are unknown. We therefore determined the effects of once-daily jugular venous administration of ovine recombinant leptin on mitochondrial protein abundance as determined by immunoblotting in tissues that do (i.e. the brain and pancreas) and do not (i.e. liver and skeletal muscle) express UCP2. Eight pairs of 1-day-old lambs received either 100 µg leptin or vehicle daily for 6 days, before tissue sampling on day 7. Administration of leptin diminished UCP2 abundance in the pancreas, but not the brain. Leptin administration had no affect on the abundance of VDAC or cytochrome c in any tissue examined. In leptin-administered animals, but not controls, UCP2 abundance in the pancreas was positively correlated with VDAC and cytochrome c content, and UCP2 abundance in the brain with colonic temperature. In conclusion, leptin administration to neonatal lambs causes a tissuespecific loss of UCP2 from the pancreas. These effects may be important in the regulation of neonatal tissue development and potentially for optimising metabolic control mechanisms in later life.

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In utero substrate restriction by placental insufficiency or maternal undernutrition decreases optical redox ratio in foetal perirenal fat

Łaźniewska

Darby

Holman

et al. 2021

Journal of Biophotonics

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Intrauterine growth restriction (IUGR) can result from reduced delivery of substrates, including oxygen and glucose, during pregnancy and may be caused by either placental insufficiency or maternal undernutrition. As a consequence of IUGR, there is altered programming of adipose tissue and this can be associated with metabolic diseases later in life. We have utilised two sheep models of IUGR, placental restriction and late gestation undernutrition, to determine the metabolic effects of growth restriction on foetal perirenal adipose tissue (PAT). Two‐photon microscopy was employed to obtain an optical redox ratio, which gives an indication of cell metabolism. PAT of IUGR foetuses exhibited higher metabolic activity, altered lipid droplet morphology, upregulation of cytochrome c oxidase subunit genes and decreased expression of genes involved in growth and differentiation. Our results indicate that there are adaptations in PAT of IUGR foetuses that might be protective and ensure survival in response to an IUGR insult.

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Differential effects of leptin on thermoregulation and uncoupling protein abundance in the neonatal lamb

Cited by 41 publications

References 50 publications

UCP1 is present in porcine adipose tissue and is responsive to postnatal leptin

UCP1 is present in porcine adipose tissue and is responsive to postnatal leptin

Tissue-specific effects of leptin administration on the abundance of mitochondrial proteins during neonatal development

In utero substrate restriction by placental insufficiency or maternal undernutrition decreases optical redox ratio in foetal perirenal fat

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