电子结肠镜检查在儿童下消化道出血中的应用价值

目的探讨电子结肠镜检查在儿童下消化道出血(LGIB)中的临床应用价值和胃镜替代电子结肠镜检查的可行性。方法回顾性分析2017年1月-2020年3月该院消化内科收治的267例LGIB患儿的病历资料,对病因及电子结肠镜检查结果进行归纳总结。结果学龄前儿童占69.29%。儿童LGIB的常见病因为肠道息肉、结直肠炎、炎症性肠病(IBD)、过敏性结肠炎、过敏性紫癜(HSP)和梅克尔憩室。其中,肠道息肉、IBD、嗜酸细胞性胃肠炎、过敏性结肠炎和白塞病的诊断阳性率达100.00%。通过内镜直视下局部止血治疗29例,镜下高频电凝电切治疗肠道息肉100例,均安全有效。267例患儿行电子结肠镜检查268例次,完成全结肠检查234例,总体盲肠插管率为87.31%。其中,电子结肠镜检查227例(盲肠插镜率为90.31%),胃镜代电子结肠镜检查41例(盲肠插镜率为70.73%)。结论电子结肠镜检查在儿童LGIB诊疗中安全有效,不同病因导致的LGIB在电子结肠镜下表现不同,对于1岁以下或体重小于10 kg的患儿,采用胃镜替代电子结肠镜检查安全可行。

折叠式人工玻璃体球囊植入术与外伤眼睫状体功能关系的初步分析

目的:探讨折叠式人工玻璃体球囊(FCVB)植入术治疗重度眼外伤患者的有效性和安全性,初步分析睫状体功能对FCVB植入手术的影响。方法:回顾性分析。纳入2018-01/2020-07在南方医科大学附属小榄人民医院接受FCVB植入手术的重度眼外伤患者10例10眼。根据患者术前检查结果进行睫状体功能评分,评分≤5分者判定睫状体功能衰竭:其中评分>5分者8眼,评分≤5分者2眼。术后随访1~31mo,检查患者BCVA、眼压,观察前房、视网膜复位情况、球囊位置及术后不良反应。结果:纳入9眼无晶状体眼患者FCVB植入过程顺利,术中无并发症;1眼有晶状体眼患者在FCVB植入过程中出现上方部分虹膜根部离断。至末次随访,所有患者FCVB位置良好,视网膜复位率100%。无严重不良事件发生。术前和末次随访的BCVA和眼压比较均无差异(P>0.05)。术前睫状体评分>5分组(8眼)中,有2眼各补充手术1次,1眼补充手术2次。睫状体功能评分≤5分组(2眼),1眼补充手术1次,1眼补充手术5次。结论:FCVB可用于治疗重度眼外伤患者,但不能有效提高患者视力。患者术前的睫状体功能状态可能与FCVB植入术后持续性低眼压、浅前房相关。

不同时期微创玻璃体切除术治疗伴有视网膜脱离的开放性眼外伤的疗效比较

目的:研究不同手术时期行Ⅱ期微创玻璃体手术治疗伴有视网膜脱离的开放性眼外伤的临床疗效。方法:回顾性分析2013-12/2018-06中山市小榄人民医院眼科收治的合并视网膜脱离的开放性眼外伤患者共41例41眼,按照Ⅱ期玻璃体切除术时间分为:早期组(伤后≤6d)24眼,常规组(伤后7~14d)17眼。术后随访以6mo为节点,比较两组术后视网膜复位率、增殖性玻璃体视网膜病变(TPVR)发生率、视力、并发症情况。结果:早期组视网膜复位率为92%,常规组为76%,两者无差异(P=0.692)。早期组TPVR发生率低于常规组(P=0.014),术后视力提高程度好于常规组(U=119.5,P=0.0018)。两组并发症发生率无差异。结论:合并视网膜脱离的开放性眼外伤患者伤后6d内行Ⅱ期玻璃体切除术预后相对较好。

Infliximab treatment of glycogenosis Ib with Crohn's-like enterocolitis: A case report

BACKGROUND Glycogen storage disease type Ib(GSD-Ib)is a glycogen metabolism disorder that leads to the manifestations of inflammatory bowel disease(IBD),especially Crohn’s disease(CD)-like colitis.Although biological agents are effective for treating CD,their application in the treatment of GSD-Ib with CD-like colitis has been rarely reported.CASE SUMMARY A 13-year-old Han male was diagnosed with GSD-Ib with CD.The patient was treated with granulocyte colony-stimulating factor.When he had symptoms of CD-like colitis,he was continuously pumped with enteral nutrition and administered oral mesalazine for 2 wk;however,the symptoms did not improve significantly.Hence,infliximab(IFX)was administered.Hitherto,the patient has been followed up for 1 year,and no clinical manifestations have been observed.After 6 mo of treatment(fifth IFX treatment),the disease activity index and all inflammatory indexes decreased,and a review of the colonoscopy data showed that the ulcers appeared smooth.CONCLUSION In this study,the patient was successfully treated with IFX.In cases of GSD-Ib,IBD should be highly considered.

Associations of Polymorphism of rs9944155, rs1051052, and rs1243166 Locus Allele in Alpha-1-antitrypsin with Chronic Obstructive Pulmonary Disease in Uygur Population of Kashgar Region

Background： Previous studies conducted in various geographical and ethnical populations have shown that Alpha-1 -antitrypsin （Alpha-1-AT） expression affects the occurrence and progression of chronic obstructive puh-nonary disease （COPD）. We aimed to explore the associations of rs9944155AG, rsl051052AG, and rs1243166AG polymorphisms in the A lpha-1-A T gene with the risk of COPD in Uygur population in the Kashgar region. Methods： From March 2013 to December 2015. a total of 225 Uygur COPD patients and 198 healthy people were recruited as cases and controls, respectively, in Kashgar region. DNA was extracted according to the protocol of the DNA genome kit, and Sequenom MassARRAY single-nucleotide polymorphism technology was used for genotype determination. Serum concentration of Alpha-1-AT was detected by enzyme-linked immunosorbent assay. A logistic regression model was used to estimate the associations of polymorphisms with COPD. Results： The rs1243166-G allele was associated with a higher risk of COPD （odds ratio [OR] = 2.039, 95% confidence interval [CI]： 1.116-3.725, P = 0.019）. In cases, Alpha-1-AT levels were the highest among participants can-yiug rs1243166 AG genotype, followed by AA and GG genotype （χ2 = 11.89, P = 0.003）. Similarly, the rs1051052-G allele was associated with a higher risk of COPD （OR = 19.433, 95% CI： 8.783-43.00, P 〈 0.001）. The highest Alpha-1-ATlevels were observed in cases carrying rs1051052 AA genotype, followed by cases with AG and GG genotypes （χ2= 122.45, P 〈 0.001）. However, individuals with rs9944155-G allele exhibited a lower risk of COPD than those carrying the rs9944155-A allele （OR = 0.121, 95% CI： 0.070-0.209, P 〈 0.001 ）. in both cases and controls, no significant difference in Alpha-l-AT levels was observed among various rs9944115 genotypes. Conclusions： rs 1243166, rs9944155, and rs 1051052 sites of Alpha- I-A Tmay be associated with the COPD morbidity in Uygur population. While rs 1243166-G allele and rs1051052-G allele are associated with an increased risk of developing COPD, rs9944155-G allele is a protect locus in Uygur population. Alpha1-AT levels in Uygur COPD patients were lower than those in healthy people and differed among patients with different rs 1051052 AG and rs 1243166 AG genotypes.

Two unrelated patients with rare Crigler-Najjar syndrome type I:two novel mutations and a patient with loss of heterozygosity of UGT1A1 gene

Cdgler-Najjar syndrome type Ⅰ （CN-I） is the most severe type of hereditary unconjugated hyperbilirubinemia. It is caused by homozygous or compound heterozygous mutations of the UDP-glycuronosyltransferase gene （UGT1A1） on chromosome 2q37. Two patients clinically diagnosed with CN-I were examined in this paper. We sequenced five exons and their flanking sequences, specifically the promoter region of UGT1A 1, of the two patients and their parents. Quantitative real-time polymerase chain reaction （qRT-PCR） was used to determine the UGT1A1 gene copy number of one patient. In patient A, two mutations, c.239_245delCTGTGCC （p.Pro80HisfsX6; had not been reported previously） and c.1156G〉T （p.Va1386Phe）, were identified. In patient B, we found that this patient had lost heterozygosity of the UGTIA1 gene by inheriting a deletion of one allele, and had a novel mutation c.1253delT （p.Met418ArgfsX5） in the other allele. In summary, we detected three UGTIA 1 mutations in two CN-I patients： c.239_ 245delCTGTGCC （p.Pro80HisfsX6）, c.1253delT （p.MeH18ArgfsX5）, and c.1156G〉T （p.Va1386Phe）. The former two mutations are pathogenic; however, the pathogenic mechanism of c.1156G〉T （p.Va1386Phe） is unknown.

Consensus for criteria of running a pediatric inflammatory bowel disease center using a modified Delphi approach

Background Good quality of care for inflammatory bowel disease(IBD)depends on high-standard management and facility in the IBD center.Yet,there are no clear measures or criteria for evaluating pediatric IBD(PIBD)center in China.The aim of this study was to develop a comprehensive set of quality indicators(QIs)for evaluating PIBD center in China.Methods A modified Delphi consensus-based approach was used to identify a set of QIs of structure,process,and outcomes for defining the criteria.The process included an exhaustive search using complementary approaches to identify potential QIs,and two web-based voting rounds to select the QIs defining the criteria for PIBD center.Results A total of 101 QIs(35 structures,48 processes and 18 outcomes)were included in this consensus.Structure QIs focused on the composition of multidisciplinary team,facilities and services that PIBD center should provide.Process QIs highlight core requirements in diagnosing,evaluating,treating PIBD,and disease follow-up.Outcome QIs mainly included criteria evaluating effectiveness of various interventions in PIBD centers.Conclusion The present Delphi consensus developed a set of main QIs that may be useful for managing a PIBD center.