在 32 岁时,有出生后追赶生长的 SGA 成年人具有持续不良的代谢健康状况和肥胖增加的特征。
SGA-born adults with postnatal catch-up have a persistently unfavourable metabolic health profile and increased adiposity at age 32 years.
机构信息
Department of Paediatrics, Subdivision of Endocrinology, Erasmus University Medical Centre, Rotterdam, The Netherlands.
Dutch Growth Research Foundation, Rotterdam, The Netherlands.
出版信息
Eur J Endocrinol. 2022 May 16;187(1):15-26. doi: 10.1530/EJE-21-1130.
BACKGROUND
Catch-up in weight-for-length in the first year of life results in more insulin resistance, an adverse lipid profile and more fat mass (FM) in 21-year-old adults born small for gestational age (SGA-CU) compared to peers born SGA without catch-up and those born appropriate for gestational age (AGA). The aim of present study was to investigate if the adverse metabolic health profile in the SGA-CU group would worsen or remain stable over the years and to determine the cardiometabolic health at 32 years between the SGA and AGA groups.
METHODS
We longitudinally investigated 287 adults, 170 SGA with catch-up growth (SGA-CU) or persistent short stature (SGA-S) and 117 AGA at ages 21 and 32 years. Insulin sensitivity (Si) and β-cell function were measured by frequently sampled i.v. glucose tolerance test, body composition by dual-energy X-ray absorptiometry (DXA) scan, and abdominal adipose tissue and liver fat fraction by MRI scan. Also, fasting serum lipid levels and blood pressure were measured.
RESULTS
At age 32 years, SGA-CU had lower Si than AGA (P = 0.030), while SGA-S had similar Si than AGA. FM and trunk fat were higher in SGA-CU than AGA (P = 0.033, P = 0.024, respectively), while SGA-S had lower lean body mass than SGA-CU and AGA (P = 0.001 and P < 0.001, respectively). SGA-CU had significantly higher levels of adverse lipids than AGA. Beta-cell function, visceral fat, liver fat fraction and blood pressure were similar in all groups. Metabolic health parameters in SGA-CU and SGA-S did not worsen compared to AGA during 11 years of follow-up. Gain in weight SDS from birth to age 32 years was associated with a higher risk of developing metabolic syndrome at age 32 years.
CONCLUSION
At age 32 years, SGA-CU adults had insulin resistance, higher FM with central adiposity and an adverse lipid profile. Postnatal catch-up growth increases the cardiometabolic risk; therefore, accelerated gain in weight should be prevented in SGA-born children.
背景
与未追赶生长(SGA-S)和胎龄适当(AGA)的 SGA 相比,1 岁时体重-身长追赶生长的 SGA 成年患者表现出更高的胰岛素抵抗、不良血脂谱和更多的脂肪量(FM)。本研究旨在调查 SGA-CU 组的不良代谢健康状况是否会随着时间的推移而恶化或保持稳定,并确定 SGA 和 AGA 组在 32 岁时的心脏代谢健康状况。
方法
我们对 287 名成年人进行了纵向研究,其中 170 名是 SGA 且有追赶生长(SGA-CU)或持续矮小(SGA-S),117 名是 AGA,分别在 21 岁和 32 岁时进行研究。通过多次采样静脉葡萄糖耐量试验测量胰岛素敏感性(Si)和β细胞功能,通过双能 X 射线吸收仪(DXA)扫描测量身体成分,通过 MRI 扫描测量腹部脂肪组织和肝脂肪分数。同时,还测量了空腹血清脂质水平和血压。
结果
在 32 岁时,SGA-CU 的 Si 低于 AGA(P = 0.030),而 SGA-S 的 Si 与 AGA 相似。SGA-CU 的 FM 和躯干脂肪量高于 AGA(P = 0.033,P = 0.024),而 SGA-S 的瘦体重低于 SGA-CU 和 AGA(P = 0.001 和 P < 0.001)。SGA-CU 的不良血脂水平显著高于 AGA。所有组的β细胞功能、内脏脂肪、肝脂肪分数和血压均相似。在 11 年的随访期间,SGA-CU 和 SGA-S 的代谢健康参数与 AGA 相比没有恶化。从出生到 32 岁时体重 SDS 的增加与 32 岁时代谢综合征的发生风险增加相关。
结论
在 32 岁时,SGA-CU 成年患者表现出胰岛素抵抗、更高的 FM 伴中心性肥胖和不良血脂谱。追赶生长增加了心脏代谢风险;因此,应防止 SGA 出生的儿童体重过快增长。
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