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首页> 外文期刊>Jornal de Pediatria >Linear growth and bone metabolism in pediatric patients with inflammatory bowel disease ☆
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Linear growth and bone metabolism in pediatric patients with inflammatory bowel disease ☆

机译:小儿炎症性肠病患者的线性生长和骨代谢☆

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摘要

Objective: To review the pathophysiology and evaluation methods of linear growth and bone mineral density in children and adolescents diagnosed with inflammatory bowel disease. Source of data: Narrative review carried out in the PubMed and Scopus databases through an active search of the terms: inflammatory bowel disease, growth, failure to thrive, bone health, bone mineral density, and children and adolescents, related to the last ten years, searching in the title, abstract, or keyword fields. Synthesis of findings: Inflammatory bowel diseases of childhood onset may present as part of the clinical picture of delayed linear growth in addition to low bone mineral density. The presence of a chronic inflammatory process with elevated serum levels of inflammatory cytokines negatively interferes with the growth rate and bone metabolism regulation, in addition to increasing energy expenditure, compromising nutrient absorption, and favoring intestinal protein losses. Another important factor is the chronic use of glucocorticoids, which decreases the secretion of growth hormone and the gonadotrophin pulses, causing pubertal and growth spurt delay. In addition to these effects, they inhibit the replication of osteoblastic lineage cells and stimulate osteoclastogenesis. Conclusion: Insufficient growth and low bone mineral density in pediatric patients with inflammatory bowel disease are complex problems that result from multiple factors including chronic inflammation, malnutrition, decreased physical activity, late puberty, genetic susceptibility, and immunosuppressive therapies, such as glucocorticoids.
机译:目的:探讨诊断为炎性肠病的儿童和青少年的线性生长和骨矿物质密度的病理生理学和评估方法。数据来源:通过对以下术语的积极搜索,在PubMed和Scopus数据库中进行了叙述性回顾:炎症性肠病,生长,无法生长,骨骼健康,骨骼矿物质密度以及与最近十年相关的儿童和青少年,在标题,摘要或关键字字段中进行搜索。研究结果的综合:儿童期发病的炎症性肠病除了低骨密度外,还可能是线性生长延迟的临床表现之一。慢性炎症过程的存在与血清炎性细胞因子水平的升高相比,除了增加能量消耗,损害营养吸收和有利于肠蛋白质损失外,还不利于生长速率和骨代谢调节。另一个重要因素是糖皮质激素的长期使用,它会减少生长激素和促性腺激素脉冲的分泌,从而导致青春期和生长突突的延迟。除这些作用外,它们还抑制成骨细胞系细胞的复制并刺激破骨细胞生成。结论:小儿炎性肠病患者生长不足和骨矿物质密度低是复杂的问题,其由多种因素引起,包括慢性炎症,营养不良,体力活动减少,青春期晚,遗传易感性和免疫抑制疗法(如糖皮质激素)。

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