Davide Silvagni scite author profile

Davide Silvagni

5Publications

204Citation Statements Received

73Citation Statements Given

How they've been cited

282

184

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Affiliations

Azienda Ospedaliera Universitaria Integrata Verona, University of Verona, Aristotle University of Thessaloniki

Publications

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Obesity and Inflammation: Evidence for an Elementary Lesion

Sbarbati

Osculati

Silvagni³

et al. 2006

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In obesity, an inflammatory process of the adipose tissue has been hypothesized; however, direct evidence for a tissue lesion is still lacking. Macrophage infiltration in the adipose tissue of obese individuals seems to be proven, but other alterations of the tissue have not been demonstrated. Moreover, in humans it has not been clarified whether inflammation is an early characteristic of obesity, because no data from obese children are available. In the present study, we assessed the inflammatory involvement of the adipose tissue and identified the elementary "inflammatory" lesion in a group of obese children. The study of children gives us the chance to investigate adipose tissue during early phases of obesity. In all the obese subjects, ultramicroscopic analysis of the adipose tissue demonstrated inflammatory involvement, and the extent of the lesions seemed to depend on the SD score of body mass index. The elementary lesion is a microgranuloma, with fragments of adipocytes, that evolves to fibrosis. Macrophages (and less frequently, lymphocytes or granulocytes) were found in perivascular positions. The lesions were not found in nonobese children. Our study proved that an "inflammatory" process exists in the adipose tissue of obese children, confirming previous findings in animals and obese adults and demonstrating that it is an early alteration in humans. However, the accumulation of macrophages was just one of the components of the inflammatory lesion, which also involved adipocyte degeneration, fibrosis, and, to a lesser extent, granulocyte/lymphocyte accumulation. The finding of fragments of adipocytes in the elementary lesion suggests that, at the beginning of the process, adipocytes may degenerate and that the materials generated by this process can recruit macrophages and other leukocytes. These preliminary results suggest that additional studies should be designed to clarify the cause of adipocyte fragility in obese children.

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Fat Cell Size, Insulin Sensitivity, and Inflammation in Obese Children

Maffeis

Silvagni

Bonadonna

et al. 2007

The Journal of Pediatrics

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Prevalence of Overweight and Obesity in 2‐ to 6‐year‐old Italian Children

Maffeis

Consolaro

Cavarzere

et al. 2006

Obesity

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Ghrelin, insulin sensitivity and postprandial glucose disposal in overweight and obese children

et al. 2006

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Objective: To explore the changes of ghrelin circulating levels induced by a mixed meal and their relationship with postprandial substrate oxidation rates in overweight and obese children with different levels of insulin sensitivity. Methods: A group of ten boys (age 9-12 years) with different levels of overweight (standard deviation score of body mass index: 1.6-3.2) was recruited. Body composition was measured by dual-energy Xray absorptiometry. Insulin sensitivity was assessed by a frequently sampled i.v. glucose tolerance test. Pre-prandial and postprandial (3 h) substrate oxidation was measured by indirect calorimetry. The energy content of the test meal (16% protein, 36% carbohydrate and 48% fat) was 40% of pre-prandial energy expenditure (kJ/day). Results: Pre-prandial serum concentration of total ghrelin was 701.4^66.9 pg/ml (S.E.M.). The test meal induced a rapid decrease in ghrelin levels and maximal decrease was 27.3^2.7% below baseline. Meal intake induced a progressive increase of the carbohydrate oxidation rate for 45 min after food ingestion, followed by a slow decrease without returning to pre-prandial values. Postprandial cumulative carbohydrate oxidation was 16.9^0.8 g/3 h. Insulin sensitivity and postprandial maximal decrease of ghrelin concentration showed a significant correlation (r ¼ 0.803, P , 0.01). Moreover, the postprandial carbohydrate oxidation rate correlated with the area under the curve for both insulin (r ¼ 0.673, P , 0.03) and ghrelin (r ¼ 20.661, P , 0.04). Conclusions: A relevant association between postprandial insulin-mediated glucose metabolism and ghrelin secretion in children with different levels of overweight was found. It is possible that the maintenance of an adequate level of insulin sensitivity and glucose oxidation may affect appetite regulation by favoring a more efficient postprandial ghrelin reduction.European Journal of Endocrinology 154 61-68

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Acute pain management: acetaminophen and ibuprofen are often under-dosed

Milani

Benini²,

Dell’Era

et al. 2017

Eur J Pediatr

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Agenzia Italiana del Farmaco-Observational Study Register (RSO). Registration code: PIERRE/1 What is Known: • Pain is frequent in children presented to emergency department. • International recommendations on pain management are often not implemented. What is New: • Acetaminophen and ibuprofen were frequently underdosed in children prescribed for pain in the Italian emergency departments. • Under-dosage may be related to the habit of using acetaminophen and ibuprofen in the recommended range for fever treatment.

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Davide Silvagni

Obesity and Inflammation: Evidence for an Elementary Lesion

Fat Cell Size, Insulin Sensitivity, and Inflammation in Obese Children

Prevalence of Overweight and Obesity in 2‐ to 6‐year‐old Italian Children

Ghrelin, insulin sensitivity and postprandial glucose disposal in overweight and obese children

Acute pain management: acetaminophen and ibuprofen are often under-dosed

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