Li Tingting, Hu Sufen, Guo Fangfang, He Youming, Cheng Haiping, Wu Mengying, Mao Yan, Zhang Kexin, Lin Juan, Li Rui, Ma Defei, Li Shiting, Chen Cheng, Hu Bing, Wang Mingbang, Xie Yingmei
Department of Neonatology, Longgang District Maternity & Child Healthcare Hospital of Shenzhen City [Affiliated Shenzhen Women and Children's Hospital (Longgang) of Shantou University Medical College], Shenzhen, Guangdong, China.
Department of Pediatric Rehabilitation, Longgang District Maternity & Child Healthcare Hospital of Shenzhen City [Affiliated Shenzhen Women and Children's Hospital (Longgang) of Shantou University Medical College], Shenzhen, Guangdong, China.
Front Pediatr. 2025 Aug 14;13:1658039. doi: 10.3389/fped.2025.1658039. eCollection 2025.
BACKGROUND/OBJECTIVES: Pregnancy complications are associated with adverse maternal-neonatal outcomes, but the underlying immune mechanisms remain unclear. Here we examined umbilical cord IL-17A levels and their link to gestational diabetes mellitus (GDM) and perinatal infections (PIs).
This two-phase study analyzed 87 pregnant women (38 in the exploratory phase and 49 in the validation phase) from Shenzhen's Premature Infants Gut Microbiota Assembly and Neurodevelopment (PIGMAN) cohort, divided into perinatal complication (PC) (45 cases) and non-perinatal complication (NPC) (42 cases) groups. Cord blood IL-17A levels were measured by ELISA and analyzed as a continuous variable by Nonparametric rank-sum test and a categorical variable using Fisher's exact test.
Nonparametric analysis revealed consistently lower IL-17A levels in the PC group across both phases. The discovery phase median in the PC group was 0.67 pg/ml lower than the 5.68 pg/ml median in the NPC group ( = 0.001); in the validation phase, the PC and NPC group levels were 0.93 and 2.05 pg/ml ( = 0.012), respectively. Low IL-17A (<1 pg/ml) prevalence was significantly higher in PC cases (discovery: 61.9% vs. 11.8%, = 0.002; validation: 50% vs. 36%, = 0.031). Rank-sum test and Fisher's exact test demonstrated concordant results, confirming a robust association between reduced IL-17A levels and perinatal complications.
Umbilical cord blood from PC pregnancies exhibited significantly lower IL-17A levels compared to that from NPC pregnancies, suggesting compromised neonatal cellular immunity. These findings implicate IL-17A deficiency in the immune dysregulation associated with GDM and PI. Conversely, the higher IL-17A levels observed in NPC pregnancies may reflect its protective role in maternal-fetal immunity during early development.
背景/目的:妊娠并发症与不良的母婴结局相关,但其潜在的免疫机制仍不清楚。在此,我们检测了脐带血白细胞介素-17A(IL-17A)水平及其与妊娠期糖尿病(GDM)和围产期感染(PI)的关联。
这项两阶段研究分析了来自深圳早产儿肠道微生物群组装与神经发育(PIGMAN)队列的87名孕妇(探索阶段38名,验证阶段49名),分为围产期并发症(PC)组(45例)和非围产期并发症(NPC)组(42例)。通过酶联免疫吸附测定法(ELISA)测量脐带血IL-17A水平,并通过非参数秩和检验作为连续变量进行分析,使用Fisher精确检验作为分类变量进行分析。
非参数分析显示,在两个阶段中,PC组的IL-17A水平始终较低。PC组在发现阶段的中位数比NPC组的中位数5.68 pg/ml低0.67 pg/ml(P = 0.001);在验证阶段,PC组和NPC组的水平分别为0.93和2.05 pg/ml(P = 0.012)。PC病例中低IL-17A(<1 pg/ml)的患病率显著更高(发现阶段:61.9%对11.8%,P = 0.002;验证阶段:50%对36%,P = 0.031)。秩和检验和Fisher精确检验结果一致,证实IL-17A水平降低与围产期并发症之间存在密切关联。
与NPC妊娠的脐带血相比,PC妊娠的脐带血IL-17A水平显著降低,提示新生儿细胞免疫受损。这些发现表明IL-17A缺乏与GDM和PI相关的免疫失调有关。相反地,在NPC妊娠中观察到的较高IL-17A水平可能反映了其在早期发育过程中对母胎免疫的保护作用。
