目的 探讨围生期高危因素对早产儿早期外周血γδ-T等淋巴细胞亚群水平的影响,明确γδ-T细胞对早产儿结局的预测价值。方法 选取112例胎龄28~37周的早产儿(包括早期早产儿88例、中晚期早产儿24例)为研究对象,选取同期15例胎龄37~42周的足月儿为对照组,采用流式细胞术检测其生后24 h内外周血γδ-T、CD4+、CD8+、CD3+及总淋巴细胞的比例,分析胎龄及早产高危因素对早期淋巴细胞亚群水平的影响,研究早产儿近期结局与γδ-T等淋巴细胞亚群的关系。结果 1)早期早产儿、中晚期早产儿和足月儿外周血γδ-T细胞水平比较,差异有统计学意义(F=8.855,P<0.001),且早期早产儿显著低于其他两组(P<0.05);2) 不同早产原因组间各淋巴细胞亚群差异无统计学意义(P>0.05);3)不同医源性早产原因的4个亚组间γδ-T细胞水平差异有统计学意义(F=3.595,P<0.05),且胎儿生长受限组患儿γδ-T细胞比例降低(P<0.05);4)γδ-T等淋巴细胞亚群分布在早发型感染组与无早发型感染组间差异无统计学意义(P>0.05);5)矫正胎龄6月龄和12月龄时,早产儿发育正常组、脑瘫/发育落后组和死亡组外周血中γδ-T等淋巴细胞亚群水平差异无统计学意义(P>0.05)。结论 早产儿早期外周血γδ-T细胞主要受胎龄影响,并对胎儿生长受限敏感,与早产儿近期发育水平无显著相关性。
Abstract
Objective To investigate the influence of perinatal risk factors on γδ-T lymphocyte subsets in peripheral blood of preterm infants, and to determine the prognostic value of γδ-T cells for outcomes of premature infants. Methods A total of 112 preterm infants with gestational age from 28 to 37 weeks were enrolled in this study (including 88 cases of early preterm infants, 24 cases of middle to late preterm infants). Meanwhile 15 infants with gestational age of 37 to 42 weeks were selected into the control group. The levels of γδ-T, CD4+, CD8+, CD3+ and total lymphocytes in peripheral blood within 24 hours after birth were tested by flow cytometry. The influence of gestational age and risk factors of preterm birth on the lymphocyte subsets levels, as well as the relationship between outcomes of premature infants and γδ-T cells were analyzed. Results 1)There was significantly difference in the level of γδ-T cell in peripheral blood among the early preterm infants,middle to late preterm infants and term infants(F=8.855,P<0.001),and the proportion of γδ-T cells in early preterm infants was significantly lower than that in the other two groups(P<0.05). 2) There was no significant difference in lymphocyte subsets among different causes of preterm birth groups (P>0.05). 3)The levels of γδ-T cells in the four different iatrogenic preterm delivery subgroups were significantly different(F=3.595,P<0.05), andthe proportion of γδ-T cells in the fetal growth restriction group was significantly decreased (P<0.05). 4) There was no significant difference in the proportion of lymphocyte subsets between early-onset infection group and non-early-onset infection group (P>0.05). 5) No significant difference in γδ-T lymphocyte subsets was found among the normal group, the cerebral palsy/developmental delays group and the death group with 6 and 12 months of corrected age (P>0.05). Conclusion γδ-T cells in early peripheral blood of preterm infants are mainly affected by gestational age and are sensitive to fetal growth restriction, but have no correlation with the short-term development level of preterm infants.
关键词
早产儿 /
胎龄 /
淋巴细胞亚群 /
γδ-T细胞 /
围生期因素
Key words
preterm infants /
gestational age /
lymphocyte subsets /
γδ-T cell /
perinatal factors
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参考文献
[1] WHO. MCEE-WHO methods and data sources for childcauses of death 2000-2017[EB/OL].(2018-12).http://www.who.int/healthinfo/global_burden_disease/en.
[2] 董慧芳,王银娟,范旭方,等. 双胎发育不均衡早产儿早期并发症及纠正年龄12月内神经系统预后分析[J].中国儿童保健杂志,2020,28(3):308-311.
[3] 董会敏,宋娟,王永,等. 极早早产儿坏死性小肠结肠炎的临床特征与危险因素分析[J].中国儿童保健杂志,2021,29(9):1012-1016.
[4] 虞嘉碧,李娟.重度支气管肺发育不良的管理现状[J].中国小儿急救医学,2021,28(1):55-58.
[5] 陆澄秋,林洁,黄金华,等. 不同妊娠期并发症/合并症对胎龄小于34周早产儿结局的影响[J].复旦学报(医学版),2020,47(2):251-256.
[6] Idzikowski E, Connors TJ. Impact andclinical implications of prematurity on adaptive immune development[J]. Curr Pediatr Rep, 2020,8(4):194-201.
[7] 徐玲,朱莉莉,叶黎离,等. 人巨细胞病毒感染婴儿γδT、Treg细胞和相关细胞因子的表达及临床意义[J].中国当代儿科杂志,2018,20(3):204-208.
[8] 冯帼,何柳芳,刘素丽,等. 双歧杆菌对坏死性小肠结肠炎新生大鼠肠上皮γδT淋巴细胞的影响[J].广东医学,2016,37(21):3177-3180.
[9] 刘位位,李超乾.γδT细胞、IL-17与支气管哮喘关系研究进展[J].实用医学杂志,2018,34(7):1207-1209.
[10] Zhang XL, Rocha-Ferreira E, Li T, et al. γδT cells but not αβT cells contribute to sepsis-induced white matter injury and motor abnormalities in mice [J]. J Neuroinflammation, 2017,14(1):255.
[11] 邵肖梅,叶鸿瑁,丘小汕.实用新生儿学[M].5版.北京:人民卫生出版社,2018:57-236.
[12] 谢幸,孔北华,段涛.妇产科学[M].9版.北京:人民卫生出版社,2018:138-140.
[13] 中华医学会儿科学分会新生儿学组,中国医师协会新生儿科医师分会感染专业委员会,余加林,等.新生儿败血症诊断及治疗专家共识(2019年版)[J].中华儿科杂志,2019,4(4):252-257.
[14] Dimova T,Brouwer M,Gosselin F,et al.Effector vgamma9Vdelta2 T cells dominate the human fetal gammadelta T-cell repertoire [J]. Proc Natl Acad Sci U S A, 2015,112(6):556-565.
[15] Li JR, Li H, Mao H, et al. Vγ9Vδ2-T lymphocytes have impaired antiviral function in small-for-gestational-age and preterm neonates [J]. Cell Mol Immunol,2013,10(3):253-260.
[16] Correa-Rocha R,Pérez A, Lorente R, et al. Preterm neonates show marked leukopenia and lymphopenia that are associated with increased regulatory T-cell values and diminished IL-7 [J]. Pediatr Res, 2012,71(5):590-597.
[17] Gupta S,Malik S,Gupta S, et al. Neonatal complications in women with premature rupture of membranes (PROM) at term and near term and its correlation with time lapsed since PROM to delivery [J]. Trop Doct, 2019, 50(1):8-11.
[18] 吴甜,石晶,鲍珊,等. 胎膜早破对孕母感染及早产儿结局的影响[J].中国当代儿科杂志,2017,19(8):861-865.
[19] Sava F,Toldi G, Treszl A, et al. Immune cell subsets, cytokine and cortisol levels during the first week of life in neonates born to pre-eclamptic mothers [J]. Am J Reprod Immunol, 2017,77(6):10.
[20] Garcia-Flores V, Romero R, Miller D, et al. Inflammation-induced adverse pregnancy and neonatal outcomes can be improved by the immunomodulatory peptide exendin-4 [J]. Front Immunol,2018,9:1291-1291.
[21] Ismail IH, Boyle RJ, Mah LJ, et al. Reduced neonatal regulatory T cell response to microbial stimuli associates with subsequent eczema in high-risk infants [J]. Pediatr Allergy Immunol, 2014, 25(7):674-684.
基金
国家自然科学基金面上项目( 81771418);河南省科技厅科技攻关项目(172102310497)
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