Short-chain fatty acids and polyamines in the pathogenesis of necrotizing enterocolitis: Kinetics aspects in gnotobiotic quails

Despite years of investigation, pathogenesis of necrotizing enterocolitis (NEC) remains elusive. Bacterial metabolites were implicated by several authors but their roles remain controversial. The aim of our study was to investigate the role of SCFAs and polyamines through a kinetic study of histological and macroscopical digestive lesions in monobiotic quails. Germ-free quails, inoculated with a Clostridium butyricum strain involved in a NEC case, were fed or not with a diet including lactose (7%). Quails were sacrificed at various times between D7 and D24 after bacterial inoculation. NEC-like lesions, i.e. thickening, pneumatosis, and hemorrhages, occurred only in lactose-fed quails and increased with time. The main histological characteristics were infiltrates of mononuclear cells, then heterophilic cells, then gas cyst and necrosis. The first event observed, before histological and macroscopical lesions, is a high production of butyric acid, which precedes an increase of iNOS gene expression. No difference in polyamines contents depending on the diet was observed. These results show the major role of butyric acid produced by commensal bacteria in the onset of the digestive lesions.     

Serotypes and antibiotic resistance of Verotoxigenic (VTEC) and Necrotizing (NTEC) Escherichia coli strains isolated from calves with diarrhoea

Serotypes and antibiotic resistance of 51 Verotoxigenic (VTEC) and 33 Necrotizing (NTEC) bovine Escherichia coli strains were determined and compared with those shown by 205 non-VTEC non-NTEC strains isolated from the same batch of calves. E. coli untypable for O-antigen represented 47% of the VTEC, 12% of the NTEC and 8.8% of the non-VTEC non-NTEC. Typable VTEC belonged to serotypes 02:K?, 0103:K-, 0104:K?, 0128:K?, 0153:K- and O157:K-:H7, whereas typable NTEC were of serotypes 08:K87, 015:K14, 015:K-, 054:K?, 076:K-, 078:K(80), 088:K?, 0123:K-, 0139:K- and 0153:K-. Non-VTEC non-NTEC showed a wide variety of serotypes which were generally unrelated to those found in VTEC and NTEC. VTEC were resistant to antibiotics at higher rates than NTEC and non-VTEC non-NTEC, and showed also the highest multidrug-resistant pattern. Our results show that bovine VTEC strains belonged to O-groups usually found in human VTEC causing sporadic diarrhoea, haemorrhagic colitis and/or haemolytic uraemic syndrome, such as 02, 0103, 0104, 0153 and especially 0128 and O157. In contrast, bovine NTEC strains belonged to serotypes different from those previously found in necrotizing E. coli strains of human origin.     

Toll-like Receptor 4 Is Expressed on Intestinal Stem Cells and Regulates Their Proliferation and Apoptosis via the p53 Up-regulated Modulator of Apoptosis

Factors regulating the proliferation and apoptosis of intestinal stem cells (ISCs) remain incompletely understood. Because ISCs exist among microbial ligands, immune receptors such as toll-like receptor 4 (TLR4) could play a role. We now hypothesize that ISCs express TLR4 and that the activation of TLR4 directly on the intestinal stem cells regulates their ability to proliferate or to undergo apoptosis. Using flow cytometry and fluorescent in situ hybridization for the intestinal stem cell marker Lgr5, we demonstrate that TLR4 is expressed on the Lgr5-positive intestinal stem cells. TLR4 activation reduced proliferation and increased apoptosis in ISCs both in vivo and in ISC organoids, a finding not observed in mice lacking TLR4 in the Lgr5-positive ISCs, confirming the in vivo significance of this effect. To define molecular mechanisms involved, TLR4 inhibited ISC proliferation and increased apoptosis via the p53-up-regulated modulator of apoptosis (PUMA), as TLR4 did not affect crypt proliferation or apoptosis in organoids or mice lacking PUMA. In vivo effects of TLR4 on ISCs required TIR-domain-containing adapter-inducing interferon-β (TRIF) but were independent of myeloid-differentiation primary response-gene 88 (MYD88) and TNFα. Physiological relevance was suggested, as TLR4 activation in necrotizing enterocolitis led to reduced proliferation and increased apoptosis of the intestinal crypts in a manner that could be reversed by inhibition of PUMA, both globally or restricted to the intestinal epithelium. These findings illustrate that TLR4 is expressed on ISCs where it regulates their proliferation and apoptosis through activation of PUMA and that TLR4 regulation of ISCs contributes to the pathogenesis of necrotizing enterocolitis.     

肛周坏死性筋膜炎抗感染治疗12例报告

目的探讨坏死性筋膜炎诊断及有效治疗方法。方法回顾性分析总结12例坏死性筋膜炎的临床表现及治疗过程（包括彻底扩创引流,全身抗感染治疗及营养支持治疗）。结果12例患者痊愈。结论早期明确诊断,尽早切开引流,抗感染及营养支持的方法,是治疗坏死性筋膜炎的有效方法。     

酪酸梭菌预防早产儿坏死性小肠结肠炎的疗效观察

目的探讨宝乐安（酪酸梭菌CGMCC0313．1散剂）预防早产儿坏死性小肠结肠炎（NEC）的疗效。方法将胎龄在28—35周的早产几90例,随机分为预防组和对照组,预防组在原发病治疗的基础上出生后即喂服宝乐安,500mg／次,2次／d;对照组仅予原发病治疗。全部早产儿观察NEC的发病率及轻重程度、病程时间、NEC并发肺部感染及早产儿体重增长情况,予大便培养进行病原菌的检测。结果预防组的早产儿在NEC的发病率及轻重程度、病程时间、NEC并发肺部感染、体重增长、病原菌克雷伯菌及大肠埃希菌检出情况等方面与对照组的早产儿比较,差异均具有显著性（P〈0．05）。结论早期服用宝乐安可以降低早产儿坏死性小肠结肠炎的发病率,并能缩短NEC的病程,减轻NEC病情,降低NEC并发肺部感染的发病率,有助于早产儿体重的恢复增长。     

GM2 activator protein inhibits platelet activating factor signaling in rats

Platelet activating factor (PAF), an endogenous bioactive phospholipid, has been documented as a pivotal mediator in the inflammatory cascade underlying the pathogenesis of many diseases including necrotizing enterocolitis. Much effort has been directed towards finding an effective in vivo inhibitor of PAF signaling. Here, we report that a small, highly stable, lysosomal lipid transport protein, the GM2 activator protein (GM2AP) is able to inhibit the inflammatory processes otherwise initiated by PAF in a rat model of necrotizing enterocolitis. Based on behavioral observations, gross anatomical observations at necropsy, histopathology and immunocytochemistry, the administration of recombinant GM2AP inhibits the devastating gastrointestinal necrosis resulting from the injection of rats with LPS and PAF. Recombinant GM2AP treatment not only markedly decrease tissue destruction, but also helped to maintain tight junction integrity at the gastrointestinal level as judged by contiguous Zonula Occludens-1 staining of the epithelial layer lining the crypts.     

Focus: Rare Disease: Necrotizing Fasciitis: Association with Pregnancy-related Risk Factors Early in Life

Background: Pregnancy-related risk factors for necrotizing fasciitis are poorly understood. We investigated pregnancy-related characteristics associated with the long-term risk of developing necrotizing fasciitis, a rare life-threatening infectious disease. Methods: We analyzed a longitudinal cohort of 1,344,996 parous women in Quebec, Canada between 1989 and 2020. The main exposure measures included complications of pregnancy such as gestational diabetes, preterm delivery, metabolic disorder, and other maternal characteristics. We followed the women over time to identify future hospitalizations for necrotizing fasciitis up to three decades after delivery. We estimated adjusted hazard ratios (HR) and 95% confidence intervals (CI) for the association of pregnancy characteristics with risk of necrotizing fasciitis in time-varying Cox proportional hazards regression models. Results: A total of 420 women were hospitalized for necrotizing fasciitis during follow-up, including 83 (19.8%) with diabetes-related necrotizing fasciitis. The incidence of necrotizing fasciitis was elevated for women with gestational diabetes (2.9 per 100,000 person-years), preterm delivery (3.2 per 100,000 person-years), and metabolic disorders (5.4 per 100,000 person-years), compared with no pregnancy complication (1.1 per 100,000 person-years). Compared with no pregnancy complication, gestational diabetes was associated with 1.87 times the risk (95% CI 1.38-2.53), preterm delivery with 2.10 times the risk (95% CI 1.65-2.66), and metabolic disorder with 3.72 times the risk (95% CI 2.92-4.74) of developing necrotizing fasciitis over time. Pregnancy complications were more strongly associated with the risk of necrotizing fasciitis 5 years or more after delivery. Conclusions: Complications of pregnancy may be associated with the long-term risk of necrotizing fasciitis in women.     

非闭塞性肠系膜缺血致肠坏死的临床分析(附11例报道)

目的:探讨非闭塞性肠系膜缺血所致肠坏死的临床表现和结局。方法:回顾性总结青岛大学附属医院11例非闭塞性肠系膜缺血所致肠坏死的病例,评估分析其临床表现、实验室检查、腹部CT影像和手术过程。结果:所有病人均在全麻下行剖腹探查术,实施肠管切除术并一期吻合术或肠造口术,7例病人恢复良好,2例住院期间死亡,2例放弃治疗回家后死亡。结论:非闭塞性肠系膜缺血临床罕见,术前难以诊断,具有较高的病死率,血管造影可以作为NOMI早期诊断及治疗的有效手段,对于怀疑有肠坏死发生的患者需及早行手术治疗。     

南京地区早产儿坏死性小肠结肠炎病原体特点和益生菌干预效果及预后影响因素分析

目的探究南京地区早产儿坏死性小肠结肠炎(NEC)的病原体特点,并观察益生菌辅助治疗对患儿血清炎症因子水平的影响,分析影响NEC早产儿预后的因素。方法将2014年5月至2018年12月于东南大学附属中大医院就诊的87例NEC早产儿选为研究对象,分析其病原体特点,观察不同治疗方法对患儿血清炎症因子的影响,并通过Logistic回归分析影响NEC患儿预后的危险因素。结果革兰阴性菌是NEC早产儿的主要致病菌,主要包括肺炎克雷伯菌(25株,27.78%)和大肠埃希菌(21株,23.33%)。肺炎克雷伯菌和大肠埃希菌对美罗培南、亚胺培南/西司他丁、哌拉西林/他唑巴坦、多粘菌素和阿米卡星敏感。益生菌干预后的NEC早产儿血清IL-1β、IL-10、TNF-α水平及TLR4的表达均显著低于常规治疗患儿(均P0.05)。发病前3 d内输血、新生儿窒息、益生菌干预、非营养性吮吸、腹膜炎、败血症、加奶速度、PDA均是影响NEC早产儿预后的相关因素(均P0.05),其中发病前3 d内输血、新生儿窒息、加奶速度、PDA是影响NEC早产儿预后的独立危险因素(均P0.05)。结论革兰阴性菌是NEC早产儿的主要致病菌,益生菌干预可有效降低NEC早产儿血清炎症因子水平。对于NEC早产儿的治疗可选用碳青霉烯类、氨基糖苷类等抗生素,同时需关注影响NEC早产儿预后的独立危险因素。     

Tight junctions as targets of infectious agents

The epithelial barrier is a critical border that segregates luminal material from entering tissues. Essential components of this epithelial fence are physical intercellular structures termed tight junctions. These junctions use a variety of transmembrane proteins coupled with cytoplasmic adaptors, and the actin cytoskeleton, to attach adjacent cells together thereby forming intercellular seals. Breaching of this barrier has profound effects on human health and disease, as barrier deficiencies have been linked with the onset of inflammation, diarrhea generation and pathogenic effects. Although tight junctions efficiently restrict most microbes from penetrating into deeper tissues and contain the microbiota, some pathogens have developed specific strategies to alter or disrupt these structures as part of their pathogenesis, resulting in either pathogen penetration, or other consequences such as diarrhea. Understanding the strategies that microorganisms use to commandeer the functions of tight junctions is an active area of research in microbial pathogenesis. In this review we highlight and overview the tactics bacteria and viruses use to alter tight junctions during disease. Additionally, these studies have identified novel tight junction protein functions by using pathogens and their virulence factors as tools to study the cell biology of junctional structures.