低出生体重儿肠道菌群及肠道屏障功能的研究

目的研究低出生体重儿的肠道菌群分布情况和肠道屏障功能的变化。方法以低出生体重儿(1 500g≤体重2 500g)为研究对象,采用16SrRNA荧光定量PCR技术和JY-DLT肠道屏障功能分析系统检测低出生体重儿出生后第7天粪便中双歧杆菌、乳杆菌、大肠埃希菌、肠球菌4种细菌的含量以及血清中的二胺氧化酶、D-乳酸和细菌内毒素的浓度,比较正常新生儿与低出生体重儿肠道菌群和肠道屏障功能的差异,分析不同喂养方式、并发症对低出生体重儿肠道菌群及肠道屏障功能的影响。结果 (1)低出生体重儿组粪便中大肠埃希菌、肠球菌、乳杆菌、双歧杆菌含量均明显低于健康新生儿组(P0.05),血清中二胺氧化酶、D-乳酸高于健康新生儿组(P0.05),细菌内毒素水平差异无统计学意义(P0.05)。(2)母乳喂养组低出生体重儿粪便中双歧杆菌和乳杆菌含量明显高于乳制品喂养组(P0.05),且血清中二胺氧化酶和和D-乳酸含量低于乳制品喂养组(P0.05),细菌内毒素水平差异无统计学意义(P0.05)。(3)无并发症组低出生体重儿粪便中乳杆菌和双歧杆菌含量明显高于有并发症组(P0.05),其血清中二胺氧化酶、D-乳酸和细菌内毒素水平均低于有并发症的低出生体重儿(P0.05)。结论低出生体重儿的肠道菌群和肠道屏障功能都与正常新生儿存在差异,母乳喂养有助于肠道有益菌的定植和肠道屏障功能的恢复。     

用16S rRNA荧光定量PCR技术分析低出生体重儿肠道菌群变化及影响因素

目的监测低出生体重儿肠道细菌分布情况,并分析影响低出生体重儿肠道微生态平衡的因素。方法以低出生体重儿(1 500g≤体重2 500g)为研究对象,采用16SrRNA荧光定量PCR技术检测新生儿出生后第1天、3天、7天粪便中双歧杆菌、乳杆菌、大肠埃希菌和肠球菌4种细菌的含量,比较正常新生儿与低出生体重儿肠道菌群构建的差异;分析不同胎龄、体重、喂养方式、疾病状态等因素对低出生体重儿肠道微生态平衡的影响。结果 (1)低出生体重儿组和健康新生儿组粪便中大肠埃希菌、肠球菌、乳杆菌和双歧杆菌含量与婴儿日龄呈明显正相关关系,且低出生体重儿组婴儿粪便4种细菌含量均明显低于健康对照组(P0.05)。(2)2 000g≤体重2 500g组低出生体重儿大肠埃希菌和肠球菌含量在各日龄明显高于体重2 000g组新生儿(P0.05),双歧杆菌和乳杆菌含量在3日龄和7日龄阶段明显高于体重2 000g组(P0.05),而1日龄阶段差异无统计学意义(P0.05)。(3)母乳喂养组在3日龄和7日龄阶段双歧杆菌和乳杆菌含量明显高于乳制品喂养组(P0.05)。(4)无并发症患儿组在3日龄和7日龄阶段乳杆菌和双歧杆菌含量明显高于有并发症组(P0.05)。结论低出生体重儿肠道菌群构建规律异于正常新生儿,尤其是乳杆菌和双歧杆菌的定植差异更为突出;低出生体重儿的出生体重与肠道乳杆菌和双歧杆菌的含量呈正相关;母乳喂养对低出生体重儿肠道中益生菌的定植有明显的优势;新生儿相关疾病直接影响低出生体重儿肠道微生态的构建,可导致其胃肠道生态系统的异常;16S rRNA荧光定量PCR技术适用于评价婴幼儿肠道微生态状况。     

布拉酵母菌散联合早期微量喂养 对早产儿喂养不耐受及肠道菌群的影响

目的探讨布拉酵母菌散联合早期微量喂养对早产儿喂养不耐受及肠道菌群的影响。方法选取2014年1月至2018年6月在我院住院治疗的喂养不耐受早产儿80例,随机分为2组,各40例。对照组早产儿生后早期间歇持续微量喂养(12～24 h内),观察组早产儿在对照组基础上加用布拉酵母菌散0.125 g/次,1次/d,通过奶瓶或鼻饲给药。两组患儿均连用3周。观察两组早产儿治疗后恢复情况、肠道菌群变化及治疗效果。结果观察组早产儿呕吐腹胀消失时间、达全胃肠喂养时间及恢复出生体重时间均明显短于对照组(均P0.05)。治疗3周后,两组早产儿肠道乳杆菌和双歧杆菌数量较治疗前明显上升(均P0.05),且观察组早产儿上升幅度较对照组更大(均P0.05)。治疗后观察组早产儿临床总有效率明显高于对照组,差异有统计学意义(95.0%vs 80.0%,χ~2=4.16,P0.05)。结论布拉酵母菌散联合早期微量喂养治疗早产儿喂养不耐受的疗效显著,能加快患儿的恢复,其作用机制可能与其能促进肠道正常菌群定植,加快肠道菌群的建立密切相关。     

双歧杆菌预防早产儿坏死性小肠结肠炎的疗效观察

目的 探讨双歧杆菌预防早产儿坏死性小肠结肠炎(NEC)的疗效.方法 随机分成试验组和对照组,对照组给予常规治疗,试验组在对照组基础上给予双歧杆菌治疗.观察两组不同胎龄和不同出生体重早产儿NEC患病率、治疗前后肠道各菌群变化的差异.结果 (1)试验组NEC总发生率显著低于对照组,差异有统计学意义(P＜0.01);(2)试验组出生体重＜1500g早产儿NEC发生率显著低于对照组,差异有统计学意义(P＜0.05);(3)治疗后试验组细菌总数、球菌总数及杆菌总数上升幅度显著大于对照组,差异均有统计学意义(P＜0.01);治疗后试验组杆球菌比值较对照组显著下降,差异有统计学意义(P＜0.01).结论 双歧杆菌可有效预防早产儿坏死性小肠结肠炎.     

低出生体重儿肠道微生态构建影响因素的 动态监测

目的动态监测低出生体重儿肠道菌群,分析不同体重、不同喂养方式及疾病状态等因素对患儿肠道微生态的影响,为规范临床低出生体重儿宫外营养支持措施及治疗手段提供依据。方法应用16SrRNA荧光定量PCR技术检测正常新生儿和低出生体重儿生后第1、3、7天粪便中大肠埃希菌、肠球菌、乳杆菌及双歧杆菌的含量。结果 (1)在生后7d内,无论正常新生儿还是低出生体重儿,其粪便中大肠埃希菌、肠球菌、乳杆菌和双歧杆菌的含量均随日龄的增加而增加,且生后7d内正常新生儿的粪便中大肠埃希菌、肠球菌、乳杆菌和双歧杆菌的含量均显著高于低出生体重儿(P0.05),正常新生儿生后7d内粪便中各细菌的增长率均高于低出生体重儿。(2)体重2 000~2 500g的低出生体重儿粪便中大肠埃希菌和肠球菌在各日龄中的含量明显高于体重2 000g的新生儿(P0.05);同时其粪便中双歧杆菌和乳杆菌含量在3日龄和7日龄阶段明显高于体重2 000g的新生儿(P0.05)。(3)3日龄和7日龄母乳喂养组的低出生体重儿粪便中双歧杆菌和乳杆菌含量明显高于乳制品喂养组(P0.05);且母乳喂养组新生儿生后7日内粪便中大肠埃希菌、乳杆菌和双歧杆菌含量的增长率均高于乳制品喂养组,尤其是双歧杆菌的增长率(126.49%vs 54.81%)。(4)合并并发症的3日龄和7日龄的低出生体重儿,粪便中乳杆菌和双歧杆菌含量均明显低于无合并症的低出生体重儿(P0.05);且无并发症组的低出生体重儿其粪便中肠球菌、乳杆菌和双歧杆菌的增长率均高于有并发症组的低出生体重儿,大肠埃希菌增长率则低于有并发症组。结论低出生体重儿肠道菌群的定植时间晚且数量少,体重、喂养方式及有无并发症是影响新生儿肠道菌群丰度的重要因素。母乳喂养可促进低出生体重儿肠道中益生菌的定植。疾病因素会导致肠道菌群丰度的降低,使肠道菌群紊乱,其程度可能与病情的严重程度相关。     

母乳联合鼠李糖乳杆菌预防早产儿喂养不耐受的疗效观察

目的观察母乳联合鼠李糖乳杆菌预防早产儿喂养不耐受的临床疗效。方法选取2016年2月至2017年2月武汉大学人民医院收治的80例生后24h内入住本院儿科新生儿病房的早产儿,随机分配成2组,其中研究组40例,对照组40例。研究组以新鲜母乳联合鼠李糖乳杆菌早期开奶喂养,对照组以早产儿配方奶早期开奶喂养,比较2组早产儿喂养不耐受症的发生率及其恢复出生体重时间、达全胃肠道喂养时间、体重增长速度和住院时间的差异。结果研究组患儿喂养不耐受发生率低于对照组,研究组恢复出生体重时间、达全胃肠道喂养时间及住院时间均短于对照组(P0.05),研究组患儿体重增加速度快于对照组(P0.05)。结论早产儿早期喂养母乳联合鼠李糖乳杆菌能够较早建立全胃肠道营养,减少早产儿喂养不耐受症的发生率,促进患儿体重增长,缩短恢复出生体重时间及达全胃肠道喂养时间,降低住院天数。     

酪酸梭菌活菌散在防治早产儿喂养不耐受方面的应用

目的观察和评价酪酸梭菌活菌散防治早产儿喂养不耐受的临床疗效。方法将56例早产儿随机分成观察组和对照组,观察组30例,对照组26例。对照组给予早产儿配方奶及部分肠外营养等常规治疗,观察组在常规治疗基础上同时添加酪酸梭菌活菌散。观察2组早产儿恢复出生体重、达到全胃肠喂养时间及发生喂养不耐受等情况。结果观察组早产儿恢复出生体重、达到全胃肠喂养时间明显短于对照组(P<0.01或P<0.05),喂养不耐受的发生率也显著少于对照组(P<0.05)。结论早产儿服用酪酸梭菌活菌散,对防治喂养不耐受具有积极的作用,能减少早产儿喂养过程中呕吐、胃潴留、腹胀的发生,促进患儿早期的生长发育,缩短达到全胃肠喂养的时间。     

新生儿胆汁淤积症患儿肠道菌群与分娩方式及喂养方式的关系

目的分析新生儿胆汁淤积症患儿肠道菌群特征及其与分娩方式、喂养方式的关系。方法选择2018年6月至2019年6月我院收治的40例新生儿胆汁淤积症患儿作为观察组,选择同期入院的120例健康新生儿作为对照组,比较两组对象肠道菌群分布情况。各组对象进一步按不同喂养方式分为母乳喂养组和混合喂养组,按不同分娩方式分为阴道分娩组和剖宫产组,分析各组新生儿肠道菌群与分娩方式、喂养方式的相关性。结果观察组新生儿粪便中双歧杆菌、乳杆菌数量及双歧杆菌/大肠埃希菌值[(7.53±0.57)lg copies/g、(8.12±0.71)lg copies/g、1.06±0.18]明显少于对照组[(9.58±0.64)lg copies/g、(8.64±0.75)lg copies/g、1.39±0.22],大肠埃希菌数量[(7.28±0.85)lg copies/g]明显多于对照组[(6.81±0.63)lg copies/g]。观察组中,阴道分娩与剖宫产分娩患儿粪便中双歧杆菌、乳杆菌、大肠埃希菌数量及双歧杆菌/大肠埃希菌值差异均有统计学意义(P0.05)。观察组中,母乳喂养与混合喂养新生儿粪便中双歧杆菌、乳杆菌、大肠埃希菌数量及双歧杆菌/大肠埃希菌值差异均有统计学意义(P0.05)。结论新生儿胆汁淤积症患儿肠道菌群存在异常,且受到分娩方式和喂养方式的影响。     

深度水解蛋白配方奶在不同体重早产儿喂养中的临床效果观察

目的:评估深度水解配方奶(eHPF)在不同体重早产儿早期喂养中临床应用效果。方法:选取2017年9月至2018年12月出生的早产儿,分为极低出生体重儿组(体重1000-1500g之间)62例和低出生体重儿(体重1500-2000g之间)100例,每组再随机分为两组,分别予以深度水解蛋白奶(eHPF)和早产儿配方奶(SPF)喂养。极低出生体重儿组于12小时后开始微量喂养,低出生体重儿12小时内适量喂养;极低出生体重儿组深度水解蛋白奶喂养2周后改早产儿奶喂养,低出生体重儿组深度水解蛋白奶1周后改早产儿奶喂养。比较深度水解蛋白奶在不同体重早产儿早期喂养中的临床应用效果,不同体重早产儿恢复出生体重时间、每日体重增长速度、胃管留置时间、完全肠内喂养天数、住院天数、喂养不耐受发生率、宫外发育迟缓发生率及尿素氮、碱性磷酸酶指标。结果:深度水解蛋白喂养组极低出生体重儿/低出生体重儿恢复出生体重天数、完全肠道喂养天数、胃管留置时间、住院天数较早产儿奶喂养组明显缩短(P0.05),每天体重增长优于早产儿组,喂养不耐受、宫外发育迟缓发生率明显低于早产儿组(P0.05),尿素氮、碱性磷酸酶无统计学差异(P0.05)。结论:深度水解蛋白奶用于不同体重早产儿早期喂养效果明显优于早产儿配方奶,其更有助于早产儿的生长发育。     

实时荧光定量聚合酶链反应在快速诊断急性单纯性膀胱炎中的应用

目的采用实时荧光定量聚合酶链反应(real-time PCR)技术从微生态学角度研究急性单纯性膀胱炎的微生物学特征。方法收集中段尿液,处理后进行real-time PCR表达谱分析,比较健康人和急性单纯性膀胱炎两组人群菌群的差异。结果 real-time PCR表达谱分析结果显示,患者尿液中大肠埃希菌、腐生葡萄球菌和肺炎克雷伯菌的数量要明显高于健康人群。结论菌群变化可能与急性单纯性膀胱炎的发生密切相关,该研究结果从微生物学角度为临床治疗急性单纯性膀胱炎的合理用药提供辅助意见。     

脑脊液检查在早产儿及足月儿细菌性脑膜炎的诊断价值

目的:评价脑脊液检查在早产儿及足月儿细菌性脑膜炎诊断中的价值。方法:选取2014年6月1日至2016年12月31日上海市儿童医院新生儿科收治的行腰椎穿刺检查的447例新生儿,回顾性分析新生儿的一般资料、脑脊液常规生化、培养等指标,根据胎龄将患儿分为早产儿167例与足月儿280例,再根据有无患发细菌性脑膜炎分为早产儿细菌性脑膜炎27例(早产儿观察组)、早产儿非细菌性脑膜炎140例(早产儿对照组)、足月儿细菌性脑膜炎38例(足月儿观察组)、足月儿非细菌性脑膜炎242例(足月儿对照组),采用受试者工作特征(ROC)曲线评估蛋白定量、白细胞计数、葡萄糖对早产儿及足月儿细菌性脑膜炎的诊断价值。结果:与同组对照组相比,足月儿观察组和早产儿观察组蛋白定量和白细胞计数均明显升高,而葡萄糖含量显著下降,且差异均具有统计学意义(P0.05);本研究65例细菌性脑膜炎患儿脑脊液培养分离出11株细菌(16.9%)。足月儿脑脊液白细胞计数、蛋白定量以及葡萄糖诊断细菌性脑膜炎的ROC曲线下面积分别为0.995、0.846、0.703。早产儿脑脊液白细胞计数、蛋白定量以及葡萄糖诊断细菌性脑膜炎ROC曲线下面积分别为0.970、0.711、0.705。结论:脑脊液白细胞计数、蛋白定量在足月儿和早产儿细菌性脑膜炎中具有较高的诊断价值。     

Intestinal Microbiota is Different in Women with Preterm Birth: Results from Terminal Restriction Fragment Length Polymorphism Analysis

Preterm birth is a leading cause of perinatal morbidity and mortality. Studies using a cultivation method or molecular identification have shown that bacterial vaginosis is one of the risk factors for preterm birth. However, an association between preterm birth and intestinal microbiota has not been reported using molecular techniques, although the vaginal microbiota changes during pregnancy. Our aim here was to clarify the difference in intestinal and vaginal microbiota between women with preterm birth and women without preterm labor. 16S ribosomal ribonucleic acid genes were amplified from fecal and vaginal DNA by polymerase chain reaction. Using terminal restriction fragment length polymorphism (T-RFLP), we compared the levels of operational taxonomic units of both intestinal and vaginal flora among three groups: pregnant women who delivered term babies without preterm labor (non-PTL group) (n = 20), those who had preterm labor but delivered term babies (PTL group) (n = 11), and those who had preterm birth (PTB group) (n = 10). Significantly low levels of Clostridium subcluster XVIII, Clostridium cluster IV, Clostridium subcluster XIVa, and Bacteroides, and a significantly high level of Lactobacillales were observed in the intestinal microbiota in the PTB group compared with those in the non-PTL group. The levels of Clostridium subcluster XVIII and Clostridium subcluster XIVa in the PTB group were significantly lower than those in the PTL group, and these levels in the PTL group were significantly lower than those in non-PTL group. However, there were no significant differences in vaginal microbiota among the three groups. Intestinal microbiota in the PTB group was found to differ from that in the non-PTL group using the T-RFLP method.     

Platelet Parameters and (1, 3)-β-D-Glucan as a Diagnostic and Prognostic Marker of Invasive Fungal Disease in Preterm Infants

The diagnosis of neonatal invasive fungal disease (IFD) is difficult and often delayed. The platelet parameters and (1, 3)-β-D-Glucan (BG) may be useful for diagnosing IFD, but their diagnostic performance are not well characterized in neonates. We studied 63 preterm infants with IFD, 160 preterm infants without sepsis (preterm control), and 41 preterm infants with bacterial sepsis. Platelet parameters at the first day of onset of IFD and at the fourteenth day after antifungal treatment were evaluated. Serum BG was measured. Platelet count (PC), plateletcrit (PCT), and platelet distribution width (PDW) values were significantly lower, and mean platelet volume (MPV) values significantly higher in the IFD versus preterm control infants. PC and PCT values were much lower in infants with IFD versus bacterial sepsis, and there were significant differences in BG value between the two groups. After 14 days of antifungal treatment, significant elevations in PC, PCT, PDW and reductions in MPV levels in IFD group were observed. Receiver operating characteristic (ROC) curves showed that PC and PCT were strong predictors of IFD. The PC and PCT cut-offs for predicting IFD were 119.5 (sensitivity 78%, specificity 95%) and 0.21 (sensitivity 83%, specificity 85%), respectively. There were significant differences in PC and PCT levels between deceased and survived patients. The PC and PCT cut-offs for predicting deceased IFD were 39 (sensitivity 62%, specificity 86%) and 0.04 (sensitivity 50%, specificity 95%), respectively. The sensitivity in diagnosing IFD by a BG cutoff of ≥10pg/ml was 68.3% and specificity was 75.6%. PC and PCT levels in the BG ≥400 pg/ml group were significantly lower compared to the BG<400 pg/ml group. Platelet parameters and BG could be useful biomarkers for the diagnosis and prognosis of neonatal IFD.     

Plasma concentration of intestinal- and liver-FABP in neonates suffering from necrotizing enterocolitis and in healthy preterm neonates

Both early diagnostic and prognostic assessment of the acute abdomen in preterm infants are hampered by the lack of a sensitive and specific parameter for intestinal injury. In this prospective clinical study we wanted to estimate the value of intestinal (I-) and liver (L-) fatty acid binding protein (FABP) in diagnosing necrotizing enterocolitis (NEC). Using highly sensitive and specific sandwich ELISAs which employ recombinant human I- and L-FABP as standard proteins (limit of detection 0.1 ng/ml plasma), the L-FABP concentration (median 7.6 ng/ml) was determined to be about 3 fold that of I-FABP (median 2.52 ng/ml) in plasma of healthy preterm infants. I- and L-FABP concentrations significantly increased with birth weight (1.6 and 5.0 ng/ml per kg, respectively). At onset of symptoms, I-FABP concentration was significantly higher in infants who later developed severe NEC compared to healthy infants and those, whose illness remained confined to stage I or II. L-FABP was significantly elevated compared to the control group at onset of symptoms regardless of the further course of NEC. In conclusion, I-FABP appears to be a specific parameter for early detection of intestinal injury leading to severe NEC stage III. L-FABP, however, is a promising sensitive marker even for stage I of NEC.     

婴幼儿腹泻患者肠道菌群分布特点研究

目的研究不同年龄段腹泻患儿肠道菌群分布特点,探讨不同年龄腹泻患儿肠道菌群与疾病的关联。方法选取9例符合临床诊断标准的0~1岁婴儿腹泻患者和8例符合临床诊断标准的1~3岁幼儿腹泻患者的粪便样本,同时于健康儿童中随机选取6例粪便样本作为对照,提取各组对象粪便总DNA,采用PCR-DGGE进行菌群多样性与差异性分析。结果 0~1岁腹泻患儿肠道菌群与健康对照组相比,肠道菌群构成差异显著,条件致病菌巴黎链球菌数量显著增加。1~3岁腹泻患儿肠道菌群与健康对照组相比,条件致病菌解没食子酸链球菌、屎肠球菌数量显著增加,长双歧杆菌数量下降。结论婴幼儿腹泻患者肠道菌群的构成与健康对照组相比差异显著,该特点可作为婴幼儿腹泻早期诊断的实验依据。     

ERIC-PCR指纹图谱技术分析糖尿病小鼠肠道细菌群落变化

目的通过比较1型糖尿病模型组和空白对照组雄性小鼠肠道菌群结构的变化,探索糖尿病造模与肠道菌群的关系。方法收集造模2周后空白对照组(n=5)、STZ造模成功组(n=5)和造模不成功组(n=3)ICR小鼠的新鲜粪便样品,提取粪便样品的总DNA,ERIC-PCR扩增形成DNA指纹图谱,借助多变量统计分析方法研究各组样品肠道菌群结构上的异同。结果ERIC-PCR指纹图谱结合偏最小二乘法(PLS-DA)分析表明造模成功组和造模不成功组小鼠的肠道菌群结构显著区别于空白对照组,而造模不成功组小鼠的肠道菌群结构与造模成功组仍有一定的区别。结论STZ诱导的1型糖尿病会造成小鼠的肠道菌群结构的变化,而部分小鼠造模失败可能与这些小鼠的肠道菌群结构有关。     

Antimicrobial Protein and Peptide Concentrations and Activity in Human Breast Milk Consumed by Preterm Infants at Risk of Late-Onset Neonatal Sepsis

ObjectiveWe investigated the levels and antimicrobial activity of antimicrobial proteins and peptides (AMPs) in breast milk consumed by preterm infants, and whether deficiencies of these factors were associated with late-onset neonatal sepsis (LOS), a bacterial infection that frequently occurs in preterm infants in the neonatal period.ResultsLevels of most AMPs and antibacterial activity in preterm breast milk were higher at day 7 than at day 21. Lactoferrin was the only AMP that limited pathogen growth >50% when added to formula at a concentration equivalent to that present in breast milk. Levels of AMPs were similar in the breast milk fed to infants with and without LOS, however, infants who developed LOS consumed significantly less breast milk and lower doses of milk AMPs than those who were free from LOS.ConclusionsThe concentrations of lactoferrin and defensins in preterm breast milk have antimicrobial activity against common neonatal pathogens.     

胎膜早破早产的临床分析

目的:探讨胎膜早破早产的临床处理方法及其对新生儿的影响.方法:以2009年3月至2012年1月在我院产科住院的妊娠满28～36+6周的205例胎膜早破早产患者为研究对象,针对不同孕周,采用相应的治疗方法,并对其妊娠结局和早产儿的状况进行观察和分析.结果:胎龄28～34+6周的早产儿并发症的发生率和死亡率分别为52.2％和10％,胎龄35～35+6周的早产儿并发症的发生率和死亡率分别为32.3％和4.8％,分别明显高于胎龄＞36周出生的早产儿(1.6％和0),差异具有统计学意义(P＜0.05);但孕周在36周以上出生的新生儿的并发症的发生率和死亡率与足月出生的新生儿相比无明显差异(P＞0.05).结论:胎膜早破早产是新生儿患病和死亡的主要原因,胎龄越小新生儿的患病率和死亡率越高,对于胎膜早破早产的孕妇,应针对不同孕周采用不同的治疗方法,以延长孕周以降低早产儿的患病率和死亡率.     

胎盘组织学绒毛膜羊膜炎与未足月胎膜早破后早产儿脑损伤关系

目的:研究胎盘组织学绒毛膜羊膜炎与未足月胎膜早破后早产儿出现脑损伤的相关性。方法:选取我院妇产科2017年1月至2019年12月收治的因胎膜早破生产的未足月早产儿80例,根据是否存在绒毛膜羊膜炎分为观察组(绒毛膜羊膜炎)和对照组(无绒毛膜羊膜炎),每组40例,患儿于胎龄40 w时行颅脑核磁共振检查(Magnetic Resonance Examination,MRI),对比两组脑室周围白质软化(periventricular leukomalacia,PVL)阳性率,且采用新生儿20项行为神经评分量表(neonatal behavior neurological assessment,NBNA)评价两组患儿神经行为,然后在纠正胎龄3、6个月时对两组患儿进行智能发育指数(mental developmentalindex,MDI)及心理运动发育指数(psychomotor development index,PDI)测定并对比。结果:观察组PVL阳性率为27.5%,高于对照组的10.0%(P<0.05);观察组纠正胎龄40 w NBNA得分为(31.02±3.51)分,对照组为(35.21±4.02)分,差异具有统计学意义(P<0.05);胎龄3个月,MDI得分在观察组与对照组间差异无具有统计学意义(P>0.05),但其PDI得分低于对照组(P<0.05);胎龄6个月,观察组MDI及PDI得分均低于对照组(P<0.05)。结论:绒毛膜羊膜炎与未足月胎膜早破后早产儿的脑部损伤情况具有一定相关性,可以作为预测早产儿脑损伤程度的一项指标。     

Hypothesis: inappropriate colonization of the premature intestine can cause neonatal necrotizing enterocolitis.

Neonatal necrotizing enterocolitis (NEC) is a major cause of morbidity in preterm infants. We hypothesize that the intestinal injury in this disease is a consequence of synergy among three of the major risk factors for NEC: prematurity, enteral feeding, and bacterial colonization. Together these factors result in an exaggerated inflammatory response, leading to ischemic bowel necrosis. Human milk may decrease the incidence of NEC by decreasing pathogenic bacterial colonization, promoting growth of nonpathogenic flora, promoting maturation of the intestinal barrier, and ameliorating the proinflammatory response.