Increased Growth Differentiation Factor 15 in Patients with Hypoleptinemia-Associated Lipodystrophy

Kralisch, Susan, Hoffmann, Annett, Estrada-Kunz, Juliana, Stumvoll, Michael, Fasshauer, Mathias, Tönjes, Anke, Miehle, Konstanze

02 February 2024

Objective. Similar to obesity, lipodystrophy (LD) causes adipose tissue dysfunction and severe metabolic complications. Growth differentiation factor 15 (GDF15) belongs to the transforming growth factor superfamily and is dysregulated in metabolic disease including obesity and diabetes mellitus. Circulating levels in LDand the impact of leptin treatment have not been investigated so far.Material and Methods. GDF15 serum levels were quantified in 60 LD patients without human immunodeficiency virus infection and 60 controlsmatched for age, gender, and bodymass index. The impact ofmetreleptin treatment on circulating GDF15 was assessed in a subgroup of patients. GDF15 mRNA expression was determined in metabolic tissues of leptin-deficient lipodystrophic aP2-nSREBP1c-Tg mice, obese ob/ob mice, and control C57Bl6 mice. Results. Median GDF15 serum concentrations were significantly higher in LD patients (819 ng/L) as compared to the control group (415 ng/L) (p < 0.001). In multiple linear regression analysis, an independent and positive association remained between GDF15 on one hand and age, patient group, hemoglobin A1c, triglycerides, and C-reactive protein on the other hand. Moreover, there was an independent negative association between GFD15 and estimated glomerular filtration rate. Circulating GDF15 was not significantly affected by metreleptin treatment in LD patients. Gdf15 was upregulated in leptin-deficient lipodystrophic mice as compared to controls. Moreover, Gdf15 mRNA expression was downregulated by leptin treatment in lipodystrophic and obese animals. Conclusions. Serum concentrations of GDF15 are elevated in LD patients and independently associated withmarkers of metabolic dysfunction. Gdf15 expression is higher in lipodystrophic mice and downregulated by leptin treatment.

info:eu-repo/classification/ddc/610

ddc:610

Roles of Adipose Tissue-Derived Factors in Adipose Tissue Development and Lipid Metabolism

Ahn, Jinsoo

13 August 2015

No description available.

Nutrition

Animal Sciences

obesity

adipokine

adipogenesis

marbling

lipolysis

adipose-specific gene

promoter

lipid metabolism

adipocyte differentiation

The Influence of Obstructive Sleep Apnea Syndrome on Insulin Resistance, Metabolic Syndrome, and Endothelial Dysfunction in Young Men

Guill, Stephen Gregory

30 April 2007

Obstructive sleep apnea syndrome (OSAS), a chronic respiratory disorder affecting as many as 1 in 5 adults, is associated with repetitive collapse of the upper airway during sleep and results in fragmented sleep and intermittent periods of hypoxia and hypercapnia. If left untreated, OSAS increases the risk for hypertension, insulin resistance, metabolic syndrome (MetS) in a manner that is independent of obesity in mid-adulthood. However, it is still unknown if evidence of these relationships is apparent in young adults with OSAS who are otherwise healthy and free of other chronic comorbidities. Objectives: To determine if functional and biochemical evidence of insulin resistance, MetS, and vascular endothelial dysfunction (VED) exists in young, overweight men with OSAS and if the combined effects of obesity and OSAS augments the evidence of chronic disease pathogenesis beyond the effects of obesity alone. Subjects: Subjects were 12 overweight men with OSAS (age = 22.8 ± 0.8; BMI = 32.4 ± 1.0; apnea-hypopnea index (AHI) = 25.4 ± 5.4), 17 overweight men without OSAS (age = 22.5 ± 0.7; BMI = 31.6 ± 1.1; AHI = 2.2 ± 0.3), and 18 normal weight men without OSAS (age = 21.1 ± 0.5; BMI = 22.4 ± 0.4; AHI = 1.9 ± 0.3). Methods: Subjects were evaluated for OSAS using an unsupervised, portable polysomnography test. Total fat and central abdominal fat (CAF) were assessed using dual energy x-ray absorptiometry (DEXA). Fasting blood samples were used to quantify biochemical markers for insulin resistance (glucose, insulin, adiponectin, IL-6, and TNF-á) and endothelial dysfunction (CRP, VEGF, and VEGFR2) using ELISA, RIA, and flow cytometry. MetS was defined according to Adult Treatment Panel III (ATP III) clinical standards. Triglycerides, HDL cholesterol, and glucose were measured using a commercial lipid panel. Resting blood pressure was obtained manually via auscultation. VED was measured via strain gauge plethysmography, with endothelium-dependent vasodilatation being assessed from forearm reactive hyperemia after a 5-minute period of upper arm occlusion. Statistics: One-way ANOVA was used to determine group differences in variables. Two-way ANOVA was used to evaluate group x time interactions during the 2-minute recovery period following upper arm occlusion. Pearson partial correlation was used to assess relationships between continuous variables, with analyses being controlled for CAF or OSAS severity. Spearman correlation was used to assess relationships between number of MetS components present and both indices of adiposity and OSAS severity. Stepwise multiple linear regression analysis was used to determine significant predictors of OSAS severity, insulin resistance, components of the MetS, and endothelial dysfunction. Results: Overweight subjects with OSAS had more CAF, higher fasting triglycerides, and lower serum adiponectin concentrations than both overweight and normal weight non-apneic controls. Furthermore, fasting triglycerides were directly correlated to OSAS severity, even after the influence of central abdominal fat was removed. OSAS severity was an independent predictor of triglyceride levels, and vice versa. Insulin resistance, leptin, insulin, and CRP were all higher in overweight subjects than controls, but no further differences were attributable to severity of OSAS. No differences in IL-6, TNF-á, ADMA, and expression of VEGFR2 were noted between any groups. No group or group x time interaction differences existed in regards to postocclusive reactive hyperemia responses. Conclusions: Young men with OSAS exhibit several unique anthropometric and biochemical abnormalities that may indicate early pathogenesis of or increased risk for future development for cardiovascular and metabolic disorders. Identification and treatment of OSAS at this age may be critical to prevent the onset and progression of these chronic disorders. / Ph. D.

Obstructive Sleep Apnea Syndrome

Insulin Resistance

Metabolic Syndrome

Endothelial Dysfunction

Adipokine

Central Abdominal Fat

Glycosylation of human vaspin (SERPINA12) and its impact on serpin activity, heparin binding and thermal stability

Oertwig, Kathrin, Ulbricht, David, Hanke, Stefanie, Pippel, Jan, Bellmann-Sickert, Kathrin, Sträter, Norbert, Heiker, John T.

06 March 2019

Vaspin is a glycoprotein with three predicted glycosylation sites at asparagine residues located in proximity to the reactive center loop and close to domains that play important roles in conformational changes underlying serpin function. In this study, we have investigated the glycosylation of human vaspin and its effects on biochemical properties relevant to vaspin function. We show that vaspin is modified at all three sites and biochemical data demonstrate that glycosylation does not hinder inhibition of the target protease kallikrein 7. Although binding affinity to heparin is slightly decreased, the protease inhibition reaction is still significantly accelerated in the presence of heparin. Glycosylation did not affect thermal stability.

info:eu-repo/classification/ddc/572

ddc:572

Association between TGFb1 levels in cord blood and weight progress in the first year of life

Kabbani, Noura

05 March 2025

Transforming growth factor beta-1 (TGFβ1) is an adipokine secreted by adipose tissue, placental tissue, and immune cells, playing a role in cell proliferation, apoptosis, and angiogenesis. However, its role in pregnancy and child growth, as well as the primary source of cord TGFβ1, remains unclear. This study aimed to investigate the relationship between TGFβ1 levels and intrauterine growth parameters, as well as child growth during the first year of life, while also determining whether its primary origin is fetal or maternal. Serum samples and anthropometric measurements were collected from 79 healthy mother–child pairs within the LIFE Child cohort. TGFβ1 concentrations were measured using enzyme-linked immunosorbent assays (ELISA), and statistical analyses—including the Mann–Whitney U-test, correlation analyses, and linear regression—were performed using GraphPad Prism and R. Results showed that TGFβ1 levels were significantly higher in cord serum compared to maternal serum, suggesting a predominantly fetal origin. Multivariate regression analyses identified a strong positive association between cord TGFβ1 levels at birth and child weight at U6. Additionally, cord TGFβ1 levels were significantly correlated with child weight at approximately one year of age. An increase of 10,000 pg/mL in cord TGFβ1 at birth was associated with a 201 g higher body weight at one year, after adjusting for sex.:Introduction Paper Manuscript Manuscript Summary References Supplementary Materials Presentation of own Contributions Appendices

info:eu-repo/classification/ddc/610

ddc:610

Die Regulation von Preadipocyte factor-1 bei Gestationsdiabetes mellitus und Präeklampsie

Wurst, Ulrike

19 December 2016

Adipositas und die damit verbundenen Begleiterkrankungen zeigen einen deutlichen Anstieg der Prävalenz in der Bevölkerung. Auch für die Schwangerschaft gilt starkes Übergewicht als Risikofaktor für metabolische und vaskuläre Komplikationen wie Gestationsdiabetes mellitus (GDM) und Präeklampsie (PE). In den letzten 20 Jahren wurde eindrücklich nachgewiesen, dass eine Dysregulation von Fettzell-sezernierten Proteinen, sogenannten Adipokinen, ursächlich zu GDM und PE beitragen könnte. Zu Beginn der Dissertation lagen jedoch nur unzureichende Daten über die Regulation des Insulinresistenz-induzierenden, anti-adipogenen und anti-angiogenen Adipokins Preadipocyte factor-1 (Pref-1) bei GDM und PE vor. Die vorliegende Arbeit untersucht daher die Regulation von zirkulierendem Pref-1 bei GDM und PE sowie seine Expression in der Plazenta. Bei 74 Patientinnen mit GDM konnte kein signifikanter Unterschied der Pref-1 Konzentrationen (0.40 µg/l) verglichen zu 74 Gesunden (0.42 µg/l) (p = 0.655) festgestellt werden (Wurst U et al., Cytokine 2015; 71: 161–164). Es zeigte sich in der Kohorte eine unabhängige Assoziation zwischen Pref-1 und Schwangerschaftsalter bei der Blutentnahme, Triglyzeriden, Kreatinin, Body Mass Index und C reaktivem Protein (p < 0.05). In einer Studienkohorte von 51 Schwangeren mit PE wurden signifikant niedrigere Serumspiegel von Pref-1 (0.49 µg/l) im Vergleich zu 51 gesunden Schwangeren (0.68 µg/l) (p < 0.001) gemessen (Schrey S, Wurst U, et al., Cytokine 2015; 75: 338–343). In der multiplen Regressionsanalyse waren PE, Schwangerschaftsalter zum Zeitpunkt der Blutentnahme sowie zirkulierendes Leptin unabhängige Prädiktoren für Pref-1. Im peripartalen Zeitraum zeigte sich ein akuter und deutlicher Abfall von zirkulierendem Pref-1 im mütterlichen Blut und das Adipokin wurde immunhistochemisch im Plazentagewebe nachgewiesen. Die Daten dieser Studien sind vereinbar mit den Hypothesen, dass Pref-1 mit fortschreitender Schwangerschaft zunehmend produziert wird, die Plazenta zur Sekretion des Adipokins aktiv beiträgt sowie das Adipokin bei PE dysreguliert ist. Weiterführende Untersuchungen im Tiermodell sowie prospektive Studien sind notwendig, um die Signifikanz von Pref-1 bei GDM und PE näher zu untersuchen.

Preadipocyte factor-1

Gestationsdiabetes mellitus

Präeklampsie

Adipokine

Preadipocyte factor-1

Gestational diabetes mellitus

Preeclampsia

Adipokines

ddc:610

Étude des interactions entre les cellules progénitrices endothéliales et l’adiponectine

Lavoie, Véronique

11 1900

L’adiponectine, une adipokine aux niveaux plasmatiques inversement associés aux composantes du syndrome métabolique, protège contre l’athérosclérose et réduit les risques d’infarctus du myocarde. Les cellules progénitrices endothéliales (EPCs) jouent un rôle dans la réparation vasculaire et leur nombre est réduit chez les patients atteints de maladies cardiovasculaires. Nous croyons que les effets de l’adiponectine peuvent s’expliquer entre autres via ses interactions avec les EPCs. Trois sous-population d’EPCs, isolées du sang de donneurs sains, ont été caractérisées par immunophénotypage par cytométrie en flux. L’expression des récepteurs de l’adiponectine, AdipoR1, AdipoR2 et H-cadherin par les EPCs et les cellules endothéliales a été évaluée par qPCR. Les effets de l’adiponectine sur la migration et l’apoptose des EPCs et sur l’apoptose des HUVECs ont été étudiés. L’expression de l’élastase des neutrophiles par les EPCs et son activité ont été testées. Les résultats de qPCR montrent que l’AdipoR1 est plus fortement exprimé que l’AdipoR2 alors qu’H-cadhérine n’est pas détectable dans les EPCs. Les EPCs précoces expriment aussi l’élastase. L’expression d’AdipoR1 a été confirmée par immunobuvardage. L’adiponectine augmente de façon significative la survie de deux sous-populations d’EPCs, mais pas celle des HUVECs, en condition de privation de sérum. L’activité de l’élastase a été confirmée dans le milieu conditionné par les EPCs. Les EPCs expriment les récepteurs de l’adiponectine et l’élastase. L’adiponectine protège les EPCs contre l’apoptose et pourrait augmenter leur capacité de réparation vasculaire. L’activité élastase des EPCs pourrait moduler localement l’activité de l’adiponectine par la génération de sa forme globulaire. / Adiponectin, an adipokine whose plasma levels are inversely correlated to metabolic syndrome components, protects against atherosclerosis and reduces myocardium infarction-associated risks. Endothelial progenitor cells (EPCs) are involved in vascular repair and their number is reduced in patients with cardiovascular disease. We hypothesized that positive effects of adiponectin against atherosclerosis are explained in part by its interaction with EPCs. EPCs were obtained from healthy volunteers’ venous blood by mononuclear cell isolation and plating on collagen-coated dishes. Three subpopulations of EPCs were characterized by flow cytometry immunophenotyping. Expression of adiponectin receptors, AdipoR1, AdipoR2 and H-cadherin was evaluated by qPCR in EPCs and endothelial cells. Effects of recombinant adiponectin on apoptosis of EPCs and HUVECs were assessed. Expression of neutrophil elastase by EPCs and enzymatic activity on adiponectin processing were assessed. Quantitative PCR of EPCs and HUVECs mRNA showed a higher expression of AdipoR1 compared to AdipoR2 and no expression of H-cadherin in EPCs. Expression of AdipoR1 in EPCs was confirmed by Western Blot. We demonstrated that early EPCs express neutrophil elastase. Adiponectin significantly increased survival of two subpopulations of EPCs in condition of serum deprivation but had no effects on HUVECs. Neutrophil elastase activity was confirmed in EPCs conditioned media. Adiponectin protects some EPCs subpopulations against apoptosis and therefore could modulate their involvement in vascular repair. Neutrophil elastase activity of EPCs could locally modify adiponectin activity by its ability to generate the globular form of adiponectin.

athérosclérose

apoptose

réparation vasculaire

adipokine

élastase des neutrophiles

atherosclerosis

apoptosis

vascular repair

neutrophil elastase

Étude des interactions entre les cellules progénitrices endothéliales et l’adiponectine

Lavoie, Véronique

11 1900

No description available.

athérosclérose

apoptose

réparation vasculaire

adipokine

élastase des neutrophiles

atherosclerosis

apoptosis

vascular repair

neutrophil elastase

Estudo do perfil clínico, metabólico, hormonal e inflamatório de crianças pré-púberes nascidas com baixo peso e sua relação com a prematuridade, retardo do crescimento intrauterino e ganho ponderal pós-natal / Study of clinical, metabolic, hormonal and inflammatory profile of prepubertal children born with low weight and its relationship with prematurity, intrauterine growth retardation and postnatal weight gain

Clarice Borschiver de Medeiros

03 October 2014

O baixo peso ao nascer (BPN) possui grande impacto na mortalidade neonatal, assim como no desenvolvimento de complicações futuras, como obesidade, hipertensão arterial sistêmica e resistência insulínica, condições relacionadas à doença cardiovascular aterosclerótica, principal causa de morbimortalidade no mundo. O objetivo desta pesquisa foi estudar o perfil clínico, metabólico, hormonal e inflamatório relacionado à doença cardiovascular em crianças pré-púberes de BPN, bem como avaliar a influência do BPN, prematuridade e restrição do crescimento intrauterino nas variáveis de interesse. Realizou-se estudo transversal com 58 crianças de dois a sete anos de BPN, sendo 32 prematuros adequados para idade gestacional (AIG), 17 prematuros pequenos para idade gestacional (PIG), 9 a termo PIG e 38 crianças de peso ao nascer adequado, nascidas no Hospital Universitário Pedro Ernesto da Universidade do Estado do Rio de janeiro, oriundas do Ambulatório de Pediatria Geral deste mesmo hospital. Frequências de perfil lipídico alterado, assim como medianas das variações no Z escore de peso e estatura do nascimento até o momento do estudo, do Z escore de índice de massa corporal (ZIMC), da circunferência da cintura, da pressão arterial sistólica e diastólica, do colesterol total, da lipoproteína de baixa densidade, da lipoproteína de baixa densidade, do triglicerídeo, da glicose, insulina, do Homeostasis Assessment for Insulin Resistance (HOMA-IR), da leptina, da adiponectina, da interleucina 6 e da proteína C reativa foram comparadas entre os dois grupos. No grupo de BPN, avaliou-se a correlação entre estas mesmas variáveis e peso de nascimento, idade gestacional, Z escores de peso e comprimento de nascimento e variações no Z escore de peso e comprimento até o primeiro ano, e até o momento do estudo, com ajuste para idade e sexo. O grupo de BPN apresentou maiores variações nos Z escore de peso (p-valor 0,0002) e estatura (p-valor 0,003) até o momento do estudo e menores níveis de adiponectina (p-valor 0,027). Não houve correlação entre as variáveis associadas ao risco cardiovascular e o grau de baixo peso, prematuridade ou crescimento intrauterino retardado. Os níveis de ZIMC (p-valor 0,0001), circunferência da cintura (p-valor 0,0008), pressão arterial diastólica (p-valor 0,046), insulina (p-valor 0,02), HOMA-IR (p-valor 0,016) e leptina (p-valor= 0,0008) se correlacionaram com a variação no Z escore de peso no primeiro ano. O ZIMC (p-valor 0,042) também se correlacionou com a variação do Z escore de comprimento no primeiro ano. Houve ainda correlação entre o ZIMC (p-valor 0,0001), circunferência da cintura (p-valor 0,0001), pressão arterial sistólica (p-valor 0,022), pressão arterial diastólica (p-valor 0,003), insulina (p-valor 0,007), HOMA-IR (p-valor 0,005) e leptina (p-valor 0,0001) com a variação no Z escore de peso até o momento do estudo. Os achados mostram que este grupo de crianças pré-púberes com BPN ainda não diferem do grupo de crianças nascidas com peso adequado exceto pelos níveis de adiponectina, sabidamente um protetor cardiovascular. Em relação às análises de correlação, nem o peso ao nascer, tampouco a prematuridade ou CIUR, influenciaram as variáveis de interesse. No entanto, fatores pós-natais como o ganho pondero-estatural se correlacionaram com o ZIMC, circunferência da cintura, pressão arterial sistólica e diastólica, insulina, HOMA-IR e leptina. Mais estudos são necessários para avaliar se os achados configuram risco cardiovascular aumentado neste grupo de pacientes. / Low birth weight (LBW) has been associated with increased neonatal mortality and long-term risks for central obesity, hypertension, insulin resistance, conditions related to cardiovascular disease, the leading cause of morbidity and mortality worldwide. The objective of this study was to evaluate clinical, metabolic, hormonal and inflammatory profile associated with cardiovascular risk in prepubertal LBW and to determine the influence of birth weight, prematurity and fetal growth restriction on this variables of interest. A cross-sectional study of 58 LBW children, between 2-7 years, including 32 preterm appropriate for gestational age (AGA), 17 preterm small for gestational age (SGA), 9 term SGA and 38 term AGA children born at the Pedro Ernesto University Hospital of the State University of Rio de Janeiro, derived from pediatric outpatient clinics of the same hospital. Frequency of altered lipid profile, as well as the median of change in weight and height SD score (SDS) between birth and the time of the study, body mass index SDS (BMI SDS), waist circumference, systolic and diastolic blood pressure, total cholesterol, low density lipoprotein, low density lipoprotein, triglyceride, glucose, insulin, Homeostasis Model Assessment for Insulin Resistance (HOMA-IR), leptin, adiponectin, interleukin-6 and C-reactive protein were compared between these two groups. In the LBW group, the correlation between these same variables and birth weight, gestational age, birth weight and length SDS and change in weight and length SDS between birth and the first year, and up to the time of the study, were evaluated after adjustment for age and sex. The LBW group showed greater variation in weight (p-value = 0.0002) and height SDS (p = 0.003) up to the time of the study and lower levels of adiponectin (p-value = 0.027). There were no correlation between the variables associated with cardiovascular risk and the degree of LBW, prematurity or fetal growth restriction. BMI SDS levels (p-value = 0.0001), waist circumference (p-value = 0.0008), diastolic blood pressure (p = 0.046), insulin (p = 0.02), HOMA -IR (p = 0.016) and leptin (p-value = 0.0008) correlated with the change in weight SDS in the first year. The BMI SDS (p-value = 0.042) also correlated with the change in length SDS in the first year. There was correlation between BMI SDS (p-value = 0.0001), waist circumference (p-value = 0.0001), systolic blood pressure (p = 0.022), diastolic blood pressure (p = 0.003), insulin (p = 0.007), HOMA-IR (p = 0.005) and leptin (p-value = 0.0001) with the change in weight SDS until the time of the study. These findings shows that prepubertal LBW children, do not differ from the group of children born with adequate weight, except for the levels of adiponectin, a known cardiovascular protective adipocitocin. Regarding the correlation analysis, neither birth weight, prematurity or fetal growth restriction influenced the variables of interest. However, postnatal factors, such as weight and height gain correlated with variables related to cardiovascular risk. Further studies are necessary to assess whether these findings constitute increased cardiovascular risk in this group of patients.

Baixo peso ao nascer

Prematuro

Resistência à insulina

Adipocinas

Low birth weight

Preterm birth

Insulin resistance

Adipokine

PEDIATRIA

Estudo do perfil clínico, metabólico, hormonal e inflamatório de crianças pré-púberes nascidas com baixo peso e sua relação com a prematuridade, retardo do crescimento intrauterino e ganho ponderal pós-natal / Study of clinical, metabolic, hormonal and inflammatory profile of prepubertal children born with low weight and its relationship with prematurity, intrauterine growth retardation and postnatal weight gain

Clarice Borschiver de Medeiros

03 October 2014

O baixo peso ao nascer (BPN) possui grande impacto na mortalidade neonatal, assim como no desenvolvimento de complicações futuras, como obesidade, hipertensão arterial sistêmica e resistência insulínica, condições relacionadas à doença cardiovascular aterosclerótica, principal causa de morbimortalidade no mundo. O objetivo desta pesquisa foi estudar o perfil clínico, metabólico, hormonal e inflamatório relacionado à doença cardiovascular em crianças pré-púberes de BPN, bem como avaliar a influência do BPN, prematuridade e restrição do crescimento intrauterino nas variáveis de interesse. Realizou-se estudo transversal com 58 crianças de dois a sete anos de BPN, sendo 32 prematuros adequados para idade gestacional (AIG), 17 prematuros pequenos para idade gestacional (PIG), 9 a termo PIG e 38 crianças de peso ao nascer adequado, nascidas no Hospital Universitário Pedro Ernesto da Universidade do Estado do Rio de janeiro, oriundas do Ambulatório de Pediatria Geral deste mesmo hospital. Frequências de perfil lipídico alterado, assim como medianas das variações no Z escore de peso e estatura do nascimento até o momento do estudo, do Z escore de índice de massa corporal (ZIMC), da circunferência da cintura, da pressão arterial sistólica e diastólica, do colesterol total, da lipoproteína de baixa densidade, da lipoproteína de baixa densidade, do triglicerídeo, da glicose, insulina, do Homeostasis Assessment for Insulin Resistance (HOMA-IR), da leptina, da adiponectina, da interleucina 6 e da proteína C reativa foram comparadas entre os dois grupos. No grupo de BPN, avaliou-se a correlação entre estas mesmas variáveis e peso de nascimento, idade gestacional, Z escores de peso e comprimento de nascimento e variações no Z escore de peso e comprimento até o primeiro ano, e até o momento do estudo, com ajuste para idade e sexo. O grupo de BPN apresentou maiores variações nos Z escore de peso (p-valor 0,0002) e estatura (p-valor 0,003) até o momento do estudo e menores níveis de adiponectina (p-valor 0,027). Não houve correlação entre as variáveis associadas ao risco cardiovascular e o grau de baixo peso, prematuridade ou crescimento intrauterino retardado. Os níveis de ZIMC (p-valor 0,0001), circunferência da cintura (p-valor 0,0008), pressão arterial diastólica (p-valor 0,046), insulina (p-valor 0,02), HOMA-IR (p-valor 0,016) e leptina (p-valor= 0,0008) se correlacionaram com a variação no Z escore de peso no primeiro ano. O ZIMC (p-valor 0,042) também se correlacionou com a variação do Z escore de comprimento no primeiro ano. Houve ainda correlação entre o ZIMC (p-valor 0,0001), circunferência da cintura (p-valor 0,0001), pressão arterial sistólica (p-valor 0,022), pressão arterial diastólica (p-valor 0,003), insulina (p-valor 0,007), HOMA-IR (p-valor 0,005) e leptina (p-valor 0,0001) com a variação no Z escore de peso até o momento do estudo. Os achados mostram que este grupo de crianças pré-púberes com BPN ainda não diferem do grupo de crianças nascidas com peso adequado exceto pelos níveis de adiponectina, sabidamente um protetor cardiovascular. Em relação às análises de correlação, nem o peso ao nascer, tampouco a prematuridade ou CIUR, influenciaram as variáveis de interesse. No entanto, fatores pós-natais como o ganho pondero-estatural se correlacionaram com o ZIMC, circunferência da cintura, pressão arterial sistólica e diastólica, insulina, HOMA-IR e leptina. Mais estudos são necessários para avaliar se os achados configuram risco cardiovascular aumentado neste grupo de pacientes. / Low birth weight (LBW) has been associated with increased neonatal mortality and long-term risks for central obesity, hypertension, insulin resistance, conditions related to cardiovascular disease, the leading cause of morbidity and mortality worldwide. The objective of this study was to evaluate clinical, metabolic, hormonal and inflammatory profile associated with cardiovascular risk in prepubertal LBW and to determine the influence of birth weight, prematurity and fetal growth restriction on this variables of interest. A cross-sectional study of 58 LBW children, between 2-7 years, including 32 preterm appropriate for gestational age (AGA), 17 preterm small for gestational age (SGA), 9 term SGA and 38 term AGA children born at the Pedro Ernesto University Hospital of the State University of Rio de Janeiro, derived from pediatric outpatient clinics of the same hospital. Frequency of altered lipid profile, as well as the median of change in weight and height SD score (SDS) between birth and the time of the study, body mass index SDS (BMI SDS), waist circumference, systolic and diastolic blood pressure, total cholesterol, low density lipoprotein, low density lipoprotein, triglyceride, glucose, insulin, Homeostasis Model Assessment for Insulin Resistance (HOMA-IR), leptin, adiponectin, interleukin-6 and C-reactive protein were compared between these two groups. In the LBW group, the correlation between these same variables and birth weight, gestational age, birth weight and length SDS and change in weight and length SDS between birth and the first year, and up to the time of the study, were evaluated after adjustment for age and sex. The LBW group showed greater variation in weight (p-value = 0.0002) and height SDS (p = 0.003) up to the time of the study and lower levels of adiponectin (p-value = 0.027). There were no correlation between the variables associated with cardiovascular risk and the degree of LBW, prematurity or fetal growth restriction. BMI SDS levels (p-value = 0.0001), waist circumference (p-value = 0.0008), diastolic blood pressure (p = 0.046), insulin (p = 0.02), HOMA -IR (p = 0.016) and leptin (p-value = 0.0008) correlated with the change in weight SDS in the first year. The BMI SDS (p-value = 0.042) also correlated with the change in length SDS in the first year. There was correlation between BMI SDS (p-value = 0.0001), waist circumference (p-value = 0.0001), systolic blood pressure (p = 0.022), diastolic blood pressure (p = 0.003), insulin (p = 0.007), HOMA-IR (p = 0.005) and leptin (p-value = 0.0001) with the change in weight SDS until the time of the study. These findings shows that prepubertal LBW children, do not differ from the group of children born with adequate weight, except for the levels of adiponectin, a known cardiovascular protective adipocitocin. Regarding the correlation analysis, neither birth weight, prematurity or fetal growth restriction influenced the variables of interest. However, postnatal factors, such as weight and height gain correlated with variables related to cardiovascular risk. Further studies are necessary to assess whether these findings constitute increased cardiovascular risk in this group of patients.

Baixo peso ao nascer

Prematuro

Resistência à insulina

Adipocinas

Low birth weight

Preterm birth

Insulin resistance

Adipokine

PEDIATRIA