Proton pump inhibitors as a risk factor for recurrence of Clostridium-difficile-associated diarrhea

AIM:To investigate the risk factors for Clostridiumdifficile-associated diarrhea(CDAD)recurrence,and its relationship with proton pump inhibitors(PPIs). METHODS:Retrospective data of 125 consecutive hospitalized patients diagnosed with CDAD between January 2006 and December 2007 were collected by medical chart review.Collected data included patient characteristics at baseline,underlying medical disease, antibiotic history before receiving a diagnosis of CDAD, duration of hospital stay,severity of CDAD,concurrenttreatment with PPIs,laboratory parameters,response to CDAD therapy,and recurrence of disease within 90 d of successful treatment.Various clinical and laboratory parameters were compared in patients in whom CDAD did or did not recur. RESULTS:Of the 125 patients(mean age,67.6± 13.9 years)that developed CDAD,98(78.4%)did not experience recurrence(non-recurrent group)and 27 (21.6%)experienced one or more recurrences(recurrent group).Prior to the development of CDAD,96% of the 125 patients were prescribed antibiotics,and 56(44.8%)of the patients received PPIs.Age older than 65 years(P=0.021),feeding via nasogastric tube(NGT)(P=0.045),low serum albumin level(P =0.025),and concurrent use of PPIs(P=0.014) were found to be risk factors for CDAD recurrence by univariate analysis.However,sex,length of hospital stay,duration and type of antibiotics used,severity of disease,leukocyte count and C-reactive protein(CRP) were not associated with risk of CDAD recurrence.On multivariate analysis,the important risk factors were advanced age(>65 years,adjusted OR:1.32,95% CI:1.12-3.87,P=0.031),low serum albumin level(< 2.5 g/dL,adjusted OR:1.85,95%CI:1.35-4.91,P= 0.028),and concurrent use of PPIs(adjusted OR:3.48, 95%CI:1.64-7.69,P=0.016). CONCLUSION:Advanced age,serum albumin level< 2.5 g/dL,and concomitant use of PPIs were found to be significant risk factors for CDAD recurrence.

Clostridium diffi cile associated infection,diarrhea and colitis

A new, hypervirulent strain of Clostridium difficile, called NAP1/BI/027, has been implicated in C. difficile outbreaks associated with increased morbidity and mortality since the early 2000s. The epidemic strain is resistant to fluoroquinolones in vitro, which was infrequent prior to 2001. The name of this strain reflects its characteristics, demonstrated by different typing methods： pulsed-field gel electrophoresis （NAP1）, restriction endonuclease analysis （BI） and polymerase chain reaction （027）. In 2004 and 2005, the US Centers for Disease Control and Prevention （CDC） emphasized that the risk of C. difficile-associated diarrhea （CDAD） is increased, not only by the usual factors, including antibiotic exposure, but also gastrointestinal surgery/manipulation, prolonged length of stay in a healthcare setting, serious underlying illness, immune-compromising conditions, and aging. Patients on proton pump inhibitors （PPIs） have an elevated risk, as do peripartum women and heart transplant recipients. Before 2002, toxic megacolon in C. dif/icile-associated colitis （CDAC）, was rare, but its incidence has increased dramatically. Up to two- thirds of hospitalized patients may be infected with C. difficile. Asymptomatic carriers admitted to healthcare facilities can transmit the organism to other susceptible patients, thereby becoming vectors. Fulminant colitis is reported more frequently during outbreaks of C. difficile infection in patients with inflammatory bowel disease （IBD）. C. diff/cile infection with IBD carries a higher mortality than without underlying IBD. This article reviews the latest information on C. difficile infection, including presentation, vulnerable hosts and choice of antibiotics, alternative therapies, and probiotics and immunotherapy. We review contact precautions for patients with known or suspected C. difficile- associated disease. Healthcare institutions require accurate and rapid diagnosis for early detection of possible outbreaks, to initiate specific therapy and implement effective control measures. A comprehensive C. difficile infection control management rapid response team （RRT） is recommended for each health care facility. A communication network between RRTs is recommended, in coordination with each country＇s department of health. Our aim is to convey a comprehensive source of information and to guide healthcare professionals in the difficult decisions that they face when caring for these oftentimes very ill patients.

Preventing pediatric antibiotic-associated diarrhea and Clostridium difficile infections with probiotics: A metaanalysis

AIM： To assess the effcacy and safety of probiotics for preventing pediatric： （1） antibiotic associated diarrhea and （2） Clostridium diffcile （C. diffcile） infections.METHODS： On June 3, 2013, we searched PubMed （1960-2013）, EMBASE （1974-2013）, Cochrane Da-tabase of Systematic Reviews （1990-2013）, CINAHL （1981-2013）, AMED （1985-2013）, and ISI Web of Science （2000-2013）. Additionally, we conducted an extensive grey literature search including contact with National Institutes of Health Clinical Trials Registry, abstracts from annual infectious disease and gastroen-terology meetings, experts in the feld and correspondence with authors. The primary outcomes were the incidence of antibiotic-associated diarrhea （AAD） and C. difficile infections （CDI）. Dichotomous outcomes （e.g. , incidence of AAD or CDI） were pooled using a random-effects model to calculate the relative risk and corresponding 95% confidence interval （95%CI） and weighted on study quality. To explore possible explanations for heterogeneity, a priori subgroup analysis were conducted on probiotic strain type, daily dose, quality of study and safety of probiotics. The overall quality of the evidence supporting each outcome was assessed using the grading of recommendations, assessment, development and evaluation criteria.RESULTS： A total of 1329 studies were identifed with 22 trials （23 treatment arms and 4155 participants） meeting eligibility requirements for our review of prevention of AAD and 5 trials （1211 participants） for the prevention of CDI. Trials in adult populations, trials of uncertain antibiotic exposure or studies which did not provide incidence of AAD were excluded. We found 12 trials testing a single strain of probiotic and 10 trials testing a mixture of probiotic strains. Probiotics （all strains combined） signifcantly reduced the incidence of pediatric AAD （pooled RR = 0.42, 95%CI： 0.33-0.53） and significantly reduced pediatric CDI （pooled RR = 0.35, 95%CI： 0.13-0.92）. Of the two strains with multiple trials, both signifcantly reduced pediatric AAD： Sac-charomyces boulardii lyo （pooled RR = 0.43, 95%CI： 0.32-0.60） and Lactobacillus rhamnosus GG （pooled RR = 0.36, 95%CI： 0.19-0.69）. There was no significant effect by type of antibiotic, or by duration or dose of probiotic. No adverse events associated were found in the 22 controlled trials relating to the use of probiotics.CONCLUSION： This meta-analysis found that probiotics signifcantly prevented pediatric antibiotic associated diarrhea and pediatric CDI, but the effcacy varies signifcantly by the strain of the probiotic.

Hematologic diseases: High risk of Clostridium difficile associated diarrhea

AIM: To investigate the incidence and clinical outcome of Clostridium difficile (C. difficile) associated diarrhea (CDAD) in patients with hematologic disease.

Incidence of <i>Clostridium difficile</i>-associated diarrhea in patients using proton pump inhibitors: A Japanese study

Objective: The incidence of Clostridium difficile-associated diarrhea (CDAD) has increased in many developed countries. In addition to previous use of antimicrobials, use of proton pump inhibitors (PPIs) is thought to increase the incidence of CDAD. However, most previous studies that showed a positive relationship between PPI use and CDAD were conducted retrospectively in Western countries. We investigated whether the use of PPIs increases the incidence of CDAD in Japan. Methods: The study was carried out with all the patients admitted to the department of internal medicine of Teikyo University Hospital from April 2009 to June 2009. Clinical data were obtained from medical records. CDAD was defined as detection of CD toxin from stool samples in diarrheal patients. PPI users were defined as patients that were prescribed with PPI for more than 30 days at the detection of CD toxin. The results of Clostridium difficile (CD) toxin were collected until April 2011. Results: A total of 793 patients were included, and PPIs were prescribed to 489 patients (59.8%). The average age of PPI users was higher than that of PPI nonusers (68.9 vs. 63.1 years). Among the 489 PPI users, 19 patients developed CDAD, while 4 developed CDAD among the 304 PPI nonusers. The relative risk of PPI use on the incidence of CDAD was 3.20 in univariate analysis (95% confidence interval, 1.10 to 9.32, p = 0.04), although the hazard ratio in multivariate analysis was 1.23 (95% confidence interval, 0.35 to 3.83, p = 0.82). Conclusions: There was no association between CDAD occurrence and PPI use in patients in Japan.

基于全基因组测序分析1起产气荚膜梭菌导致的腹泻暴发事件

目的对1起产气荚膜梭菌导致腹泻暴发事件进行病原学分析。方法采集病例肛拭子样本和环境涂抹样本,肛拭子样本增菌前后分别进行产气荚膜梭菌plc和cpe基因荧光PCR检测和产气荚膜梭菌分离培养,对分离菌落进行全自动生化鉴定和飞行时间质谱鉴定。对鉴定为产气荚膜梭菌的分离株进行全基因组测序,分析菌株携带毒力基因和耐药基因情况,基于全部分离株核心基因组单核苷酸多态性进行遗传聚集性分析。结果未增菌的病例肛拭子cpe和plc基因检出率分别为46.15%(6/13)和53.85%(7/13),基于BHI厌氧增菌后病例肛拭子cpe和plc基因检出率分别为38.46%(5/13)和53.85%(7/13);10名病例肛拭子分离到产气荚膜梭菌,均为F生物型(携带毒力基因分布plc+/cpb-/etx-/iA-/cpe+/cpb2+/netB-),10个分离株基于cgSNP构建的聚类树形成2个相互独立且遗传距离较远的分支,Lineage 1仅分布1株,为ST589,携带耐药基因为erm(Q),Lineage 2分布9株,为ST149,携带耐药基因为tetB(P),为一组高度克隆化的菌株。结论本次暴发事件由F型产气荚膜梭菌所导致,且多数病例感染一组cpe+高度克隆化菌株。全基因组测序技术可应用于产气荚膜梭菌暴发事件病原学分析,基于肛拭子样本的产气荚膜梭菌增菌方法和分子筛查方法有待开发和应用。

丁酸梭菌对哺乳犊牛生长性能、血清抗氧化指标及腹泻频率的影响

本试验旨在研究丁酸梭菌对哺乳犊牛生长性能、血清抗氧化指标及腹泻频率的影响。试验选用75头健康、体重[(40±3)kg]相近的1日龄荷斯坦母犊牛,随机分为5组,每组15头牛。对照组(CB0组)饲喂基础饲粮,试验组分别在基础饲粮中添加0.2(CB0.2组)、0.4(CB0.4组)、0.8(CB0.8组)、1.6 g/d(CB1.6组)丁酸梭菌(活菌数为1×1010CFU/g)。试验期60 d。结果表明:1)各组之间哺乳犊牛生长性能差异不显著(P>0.05)。2)14和42日龄时,CB0.8组的血清超氧化物歧化酶(SOD)活性极显著高于CB0组(P<0.01),显著高于CB0.4组(P<0.05)。28日龄时,CB0.8组的血清丙二醛(MDA)含量极显著低于CB0组(P<0.01),CB0.2、CB0.4和CB1.6组的血清MDA含量显著低于CB0组(P<0.05)。3)29~42日龄、43~60日龄和3~60日龄时,CB0.2、CB0.4、CB0.8和CB1.6组的腹泻频率显著或极显著低于CB0组(P<0.05或P<0.01)。综上所述,丁酸梭菌对哺乳犊牛的生长性能无显著影响,可提高14和42日龄哺乳犊牛血清SOD活性,降低28日龄血清MDA含量,降低腹泻频率。本试验条件下,0.8 g/d丁酸梭菌降低犊牛腹泻频率效果最好。

北京地区抗生素相关性腹泻住院患者发生艰难梭菌相关性腹泻的影响因素分析

目的探讨北京地区抗生素相关性腹泻(antibiotic-associated diarrhea,AAD)住院患者艰难梭菌相关性腹泻(clostridium difficile associated diarrhea,CDAD)的现状及其影响因素。方法选取2022年7月至2023年7月北京9家医院近1年内就诊的AAD住院患者157例,将患者分为CDAD组(34例)和非CDAD组(123例)。采用多因素logistic回归方程分析北京AAD住院患者发生CDAD的影响因素。结果157患者中男79例,女78例,年龄18~94岁,平均(72.8±14.7)岁。CDAD发生率为21.7%(34/157),13例谷氨酸脱氢酶抗原检测结果阳性,毒素检测阴性,进一步行PCR检测和肠镜检查诊断CDAD,漏诊率为38.2%(13/34)。多因素logistic分析结果显示,BMI越小(OR=0.833,95%CI:0.733~0.947,P=0.005)、腹泻前抗生素使用天数越长(OR=1.065,95%CI:1.016~1.115,P=0.008)的患者更容易发生CDAD。结论北京地区AAD住院患者CDAD发生率为21.7%,单独依靠毒素检测漏诊率高达38.2%。BMI和腹泻前抗生素使用天数为AAD住院患者发生CDAD的独立风险因素,CDAD的临床表现更重。

4例抗生素相关性腹泻的病例分析及治疗建议

目的:抗生素相关性腹泻不良后果严重,艰难梭菌是抗生素相关性腹泻的最常见病原体,通过分析抗生素相关性腹泻病例,为临床治疗提供建议和参考。方法:对北京医院4例抗生素相关性腹泻病例的危险因素、治疗方案、预防措施进行分析。结果:病例存在的危险因素包括高龄、抗生素治疗、长期住院、使用质子泵抑制剂等,抗菌药物治疗是发生抗生素相关性腹泻的重要危险因素。4个案例属于艰难梭菌轻中度至重度感染,口服万古霉素进行治疗后好转。病例存在用药疗程不足、未及时停用止泻药及质子泵抑制剂等问题。结论:以往甲硝唑是轻度至中度艰难梭菌的首选药物,现已被万古霉素取代。由于万古霉素口服生物利用度低,在粪便中浓度高,可口服治疗艰难梭菌感染,治疗标准疗程应为10~14 d或抗生素治疗结束后1周。同时应注意避免使用止泻剂及不必要的质子泵抑制剂,尽量使用风险较低的抗生素,减少患病风险。

新型冠状病毒感染抗生素治疗后艰难梭菌感染一例

艰难梭菌是一种能形成孢子的厌氧革兰阳性杆菌。近10年来,艰难梭菌感染率和严重程度在全球范围内不断增加,并已成为最常见的医院获得性感染之一。其临床表现多种多样,从无症状携带者状态到不同程度的腹泻,再到最严重的危及生命的结肠炎。现报告1例新型冠状病毒感染抗生素治疗后的老年患者,短期内出现艰难梭菌感染的诊治。结合对新型冠状病毒感染、艰难梭菌感染腹泻的认识,对该患者发病原因及诊治进行了探讨。

山东省潍坊市犊牛腹泻病原检测与分析

为调查潍坊市规模化奶牛场导致犊牛腹泻的主要病原,采集部分地区23个规模化奶牛场共计246份犊牛腹泻粪便样品,分别进行轮状病毒(BRV)、牛冠状病毒(BCoV)、牛病毒性腹泻病毒(BVDV)、产气荚膜梭菌、大肠杆菌和沙门氏菌检测。结果显示:产气荚膜梭菌、大肠杆菌、沙门氏菌、BRV、BCoV、BVDV的个体检出率分别为45.53%、21.95%、3.25%、24.80%、3.66%、13.01%,群体检出率分别为60.87%、34.78%、8.70%、34.78%、13.04%、26.09%;二重感染率为65.22%,三重感染率为8.70%,未见三重以上感染;时间分布分析发现,产气荚膜梭菌、大肠杆菌和BVDV在第二季度感染率最高,BRV在第三季度感染率最高;不同地区分析发现,昌邑市、寒亭区、临朐县、寿光市产气荚膜梭菌检出率最高,而诸城市大肠杆菌检出率最高。结果说明:产气荚膜梭菌、大肠杆菌及BRV是导致潍坊市犊牛腹泻的主要病原,且混合感染情况较普遍;不同季节、不同地区的病原流行情况存在差异。建议潍坊市加强产气荚膜梭菌、大肠杆菌以及BRV的检测与控制,各县(市、区)根据当地病原流行情况采取针对性防控措施。

酪酸梭菌活菌散与醒脾养儿颗粒联合治疗小儿消化不良性腹泻的效果

目的探讨在酪酸梭菌活菌散的基础上联合醒脾养儿颗粒治疗小儿消化不良性腹泻(ID)取得的效果。方法选取2021年9月至2023年8月于本院接受治疗的98例ID患儿,按照随机数字表分组。两组患儿均接受常规对症治疗,对照组49例患儿采用酪酸梭菌活菌散治疗,研究组49例患儿在对照组的基础上使用醒脾养儿颗粒治疗。针对两组患儿的疗效、大便次数与症状好转时间、胃肠激素指标、免疫功能指标[T淋巴细胞分化簇4^(+)(CD4^(+))、分化簇8^(+)(CD8^(+))、CD4^(+)/CD8^(+)]、不良反应(ADR)情况进行比较。结果两组患儿总有效率评价显示,研究组结果较对照组高(P<0.05)。治疗后研究组大便次数较对照组少(P<0.05)。研究组腹胀、大便性状、腹泻症状好转时间较对照组短(P<0.05)。治疗后研究组胃动素、胃泌素指标较对照组低(P<0.05),生长抑素指标较对照组高(P<0.05),CD4^(+)/CD8^(+)、CD4^(+)水平较对照组高(P<0.05),CD8^(+)水平较对照组低(P<0.05)。ADR评价显示中,两组未见差异(P>0.05)。结论在酪酸梭菌活菌散的基础上联合应用醒脾养儿颗粒治疗小儿ID效果较佳,可以快速改善相关症状,调节胃肠激素指标,增强机体免疫功能,安全可靠。

广州腹泻与健康非腹泻人群产气荚膜梭菌检出率及MLST分型

目的比较广州地区腹泻和健康非腹泻人群粪便中产气荚膜梭菌的检出率和序列分型的差异。方法此项前瞻性研究共收集了广州医科大学附属妇女儿童医疗中心2021年10—12月诊断为腹泻和健康非腹泻人群的粪便标本和腹泻患者大便肛管保存液标本296例,按照标本类型与人群的不同,分为腹泻儿童粪便组(104例)、腹泻儿童肛管组(68例)、非腹泻儿童粪便组(30例)和非腹泻成人粪便组(94例)。采用疱肉培养基增菌并转血平板厌氧培养,分离并鉴定产气荚膜梭菌。从各组中随机选取部分产气荚膜梭菌进行多位点序列分型(MLST)。结果腹泻儿童粪便组产气荚膜梭菌检出率为36.5%(38/104);腹泻儿童肛管组产气荚膜梭菌检出率为16.2%(11/68);非腹泻儿童粪便组产气荚膜梭菌检出率为46.7%(14/30);非腹泻成人粪便组产气荚膜梭菌检出率为53.2%(50/94)。非腹泻人群(包括成人和儿童)产气荚膜梭菌检出率[51.6%(64/124)]比腹泻人群高[23.8%(41/172)],差异有统计学意义(P=0.02)。34株产气荚膜梭菌共分为31种序列(ST)型,以ST210最多,占8.82%,共发现18种新ST型,占52.92%。结论广州地区产气荚膜梭菌在腹泻和非腹泻人群粪便的检出率较高,且检测出不溶血型菌株。MLST分型为产气荚膜梭菌病原学溯源提供可靠依据。

酪酸梭菌二联活菌散联合头孢唑肟钠治疗抗生素相关性腹泻患儿的效果

目的:观察酪酸梭菌二联活菌散联合头孢唑肟钠治疗抗生素相关性腹泻(AAD)患儿的效果。方法:选取2022年3月至2023年5月该院收治的74例AAD患儿进行前瞻性研究,按照随机数字表法将其分为对照组和研究组各37例。两组均予以常规治疗,在此基础上,对照组予以头孢唑肟钠治疗,研究组在对照组基础上联合酪酸梭菌二联活菌散治疗,两组均治疗3 d。比较两组临床疗效,临床相关指标(止泻时间、大便性状恢复正常时间和住院时间)水平,治疗前后肠道菌群(双歧杆菌、乳杆菌、大肠埃希菌、真杆菌)数量、炎性因子[C反应蛋白(CRP)、白细胞介素(IL)-2、IL-6、肿瘤坏死因子-α(TNF-α)、降钙素原(PCT)]水平,以及不良反应发生率。结果:研究组治疗总有效率为97.30%(36/37),高于对照组的78.38%(29/37),差异有统计学意义(P<0.05);研究组止泻时间、大便性状恢复正常时间、住院时间均短于对照组,差异有统计学意义(P<0.05);治疗后,研究组乳杆菌、双歧杆菌、真杆菌数量多于对照组,大肠埃希菌数量少于对照组,差异均有统计学意义(P<0.05);治疗后,研究组TNF-α、CRP、IL-6、PCT、IL-2水平均低于对照组,差异有统计学意义(P<0.05);两组治疗期间均未出现明显不良反应。结论:酪酸梭菌二联活菌散联合头孢唑肟钠治疗AAD患儿可提高治疗总有效率,改善临床指标水平,调节肠道菌群数量,降低炎性因子水平,效果优于单纯头孢唑肟钠治疗。

Clostridium difficile and inflammatory bowel disease: Role in pathogenesis and implications in treatment

Clostridium difficile(C.difficile)is the leading cause of antibiotic associated colitis and nosocomial diarrhea.Patients with inflammatory bowel disease(IBD)are at increased risk of developing C.difficile infection(CDI),have worse outcomes of CDI-including higher rates of colectomy and death,and experience higher rates of recurrence.However,it is still not clear whether C.difficile is a cause of IBD or a consequence of the inflammatory state in the intestinal environment.The burden of CDI has increased dramatically over the past decade,with severe outbreaks described in many countries,which have been attributed to a new and more virulent strain.A parallel rise in the incidence of CDI has been noted in patients with IBD.IBD patients with CDI tend be younger,have less prior antibiotic exposure,and most cases of CDI in these patients represent outpatient acquired infections.The clinical presentation of CDI in these patients can be unique-including diversion colitis,enteritis and pouchitis,and typical findings on colonoscopy are often absent.Due to the high prevalence of CDI in patients hospitalized with an IBD exacerbation,and the prognostic implications of CDI in these patients,it is recommended to test all IBD patients hospitalized with a disease flare for C.difficile.Treatment includes general measures such as supportive care and infection control measures.Antibiotic therapy with either oral metronidazole,vancomycin,or the novel antibiotic-fidaxomicin,should be initiated as soon as possible.Fecal macrobiota transplantation constitutes another optional treatment for severe/recurrent CDI.The aim of this paper is to review recent data on CDI in IBD:role in pathogenesis,diagnostic methods,optional treatments,and outcomes of these patients.

Probiotics for antibiotic-associated diarrhea:Do we have a verdict?

Probiotics use has increased tremendously over the past ten years.This was coupled with a surge of data relating their importance in clinical practice.Antibioticassociated diarrhea,whose frequency has risen recently,was one of the earliest targets with data published more than ten years ago.Unfortunately,available trials suffer from severe discrepancies associated with variability and heterogeneity of several factors.Most published randomized controlled trials and subsequent meta-analyses suggest benefit for probiotics in the prevention of antibiotic-associated diarrhea.The same seems to also apply when the data is examined for Clostridium difficile-associated colitis.However,the largest randomized double-blind placebo-controlled trial to date examining the use of a certain preparation of probiotics in antibiotic-associated diarrhea showed disappointing results,but it was flawed with several drawbacks.The commonest species of probiotics studied across most trials is Lactobacillus;however,other types have also shown similar benefit.Probiotics have enjoyed an impeccable safety reputation.Despite a few reports of severe infections sometimes leading to septicemia,most of the available trials confirm their harmless behavior and show similaradverse events compared to placebo.Since a consensus dictating its use is still lacking,it would be advisable at this point to suggest prophylactic use of probiotics to certain patients at risk for antibiotic-associated diarrhea or to those who suffered previous episodes.

Clinical update for the diagnosis and treatment of Clostridium difficile infection

Clostridium difficile infection(CDI)presents a rapidly evolving challenge in the battle against hospitalacquired infections.Recent advances in CDI diagnosis and management include rapid changes in diagnostic approach with the introduction of newer tests,such as detection of glutamate dehydrogenase in stool and polymerase chain reaction to detect the gene for toxin production,which will soon revolutionize the diagnostic approach to CDI.New medications and multiple medical society guidelines have introduced changing concepts in the definitions of severity of CDI and the choice of therapeutic agents,while rapid expansion of data on the efficacy of fecal microbiota transplantation heralds a revolutionary change in the management of patients suffering multiple relapses of CDI.Through a comprehensive review of current medical literature,this article aims to offer an intensive review of the current state of CDI diagnosis,discuss the strengths and limitations of available laboratory tests,compare both current and future treatments options and offer recommendations for best practice strategies.

Clostridium difficile causing acute renal failure: Case presentation and review

AIM: Clostridium difficile infection is primarily a nosocomial infection but asymptomatic carriers of Clostridium difficile can be found in up to 5% of the general population. Ampicillin, cephalosporins and clindamycin are the antibiotics that are most frequently associated with Clostridium difficile-associated diarrhea or colitis. Little is known about acute renal failure as a consequence of Clostridium difficile-associated diarrhea. METHODS: In this case report, we describe the course of Clostridium difficile-associated diarrhea in an 82-year-old patient developing acute renal failure. Stopping the offending agent and symptomatic therapy brought a rapid improvement of diarrhea and acute renal failure, full recovery was gained 18 d after admission. In a systematic review we looked for links between the two conditions. RESULTS: The link between Clostridium difficile-assoaated diarrhea and acute renal failure in our patient was most likely volume depletion. However, in experimental studies a direct influence of Clostridium difficile toxins on renal duct cells could be shown. CONCLUSION: Rapid diagnosis, nonspecific supportive treatment and specific antibiotic treatment, especially in the elderly, may lower excess mortality Clostridium difficile-associated diarrhea and renal failure being possible complications.

Toxic megacolon associated Clostridium difficile colitis

Toxic megacolon is a severe complication of Clostridium difficile (C.difficile) colitis.As the prevalence of C. difficile colitis increases and treatments become more refractory, clinicians will encounter more patients with C. difficile associated toxic megacolon in the future. Here, we review a case of toxic megacolon secondary to C. difficile colitis and review the current literature on diagnosis and management. We identify both clinical and radiologic criteria for diagnosis and discuss both medical and surgical options for management. Ultimately, we recommend using the Jalen criteria in conjunction with daily abdominal radiographs to help establish the diagnosis of toxic megacolon and to make appropriate treatment recommendations. Aggressive medical management using supportive measures and antibiotics should remain the mainstay of treatment. Surgical intervention should be considered if the patient does not clinically improve within 2-3 d of initial treatment.

Co-morbidity,not age predicts adverse outcome in clostridium difficile colitis

AIM To examine whether age alone or co-morbidity is a risk factor for death in olderadults who developed Clostridium difficile(Cd)colitis during hospitalization.METHODS A retrospective,observationalstudy design was performed in our Lady ofMercy Medical Center,a 650-bed,urban,community-based,university-affiliated teachinghospital.121 patients with a positive diagnosisof Cd colitis Caged 23-97 years)were studied,and data pertinent to demographic variables,medical history,co-morbidity,physicalexamination,and laboratory results werecollected.Age was examined as a continuousvariable and stratified into Age1(【80 vs 80+);Age2(【60,60-69,70-79 and 80+);or Age3(【60,60-69,70-79,80-89,90+).RESULTS Cd colitis occurs more frequentlywith advancing age(55% of cases 】80 years).However,age,per se,had no effect onmortality.A history of cardiac disease(P=0.036),recurrent or refractory infection】4weeks(P=0.007),low serum total protein(P=0.034),low serum albumin(P=0.001),antibiotic use 】4 weeks(P【0.010),use of over 4 antibiotics(P=0.026),and use of certainclasses of antibiotics(P=0.035-0.004)werepredictive of death.Death was stronglypredicted by the use of penicillin-like antibioticsplus clindamycin,in the presence ofhypoalbuminemia,refractory sepsis,andcardiac disease(P=0.00005).CONCLUSION Cd colitis is common in the veryold.However,unlike co-morbidity,age alonedoes not affect the clinical outcome(survival vsdeath).