队列简介:克赖斯特彻奇肠易激综合征队列,旨在研究肠道缓解和改善转运机制(COMFORT)。
Cohort Profile: The Christchurch IBS cOhort to investigate Mechanisms FOr gut Relief and improved Transit (COMFORT).
作者信息
Heenan Phoebe, Creemers Rob H, Sharma Shriya, Keenan Jacqueline, Bayer Simone, Young Wayne, Cooney Janine, Armstrong Kelly, Fraser Karl, Skidmore Paula M, Talley Nicholas J, Roy Nicole, Gearry Richard B
机构信息
Department of Medicine, University of Otago, Christchurch, New Zealand.
Department of Surgery, University of Otago, Christchurch, New Zealand.
出版信息
Inflamm Intest Dis. 2020 Aug;5(3):132-143. doi: 10.1159/000508160. Epub 2020 Jul 8.
BACKGROUND AND AIMS
This cross-sectional observational case-control study was initiated in July 2016 with the aim of increasing an understanding of the underlying disease mechanisms in functional gastrointestinal disorders (FGIDs) including irritable bowel syndrome (IBS), functional diarrhoea (FD), and functional constipation (FC). Specific areas of interest include the effect of food, microbiome, host and microbial genetics, metabolome, and psychological variables on unexplained chronic gastrointestinal (GI) symptoms.
METHODS
This study recruited consecutive patients who were attending one of two endoscopy centres in Christchurch, New Zealand, for colonoscopy and a subgroup of participants from the general public who did not undergo colonoscopy. Participants with known GI disease other than an FGID were excluded. Those with symptoms were recruited as cases, whilst those without symptoms were recruited as controls. In the days prior to preparation for colonoscopy, or an agreeable time for those not undergoing colonoscopy, demographic, symptom, psychological, dietary, and health data were collected in addition to biological samples (breath, faeces, blood, and urine). Colonic biopsies were taken at the time of colonoscopy from participants in the colonoscopy subgroup.
RESULTS
Between July 2016 and December 2018, 349 participants were recruited, 315 of whom completed the study, 220 participants were from the colonoscopy subgroup, and 95 from the non-colonoscopy subgroup. This included 129 controls and 186 cases (57 IBS-diarrhoea predominant, 30 IBS-constipation predominant, 41 IBS-mixed, 42 FC, and 16 FD). The mean age of FGID cases was 53.4 years and controls 54.4 years. Cases (149/186, 80.1%) and controls (57/72, 55.8%) were predominantly female. Education levels were similar across the cohort. Smoking and alcohol rates were also similar. Biological samples were collected as planned from participants.
CONCLUSIONS
The COMFORT cohort is a unique clinical cohort of FGID cases and controls with a wide range of demographic, dietary, clinical, psychological, and health data in addition to biological samples. Future research will aim to use a systems biology approach to establish the potential role of diet, host-microbiome interactions, and other factors in the pathogenesis of FGIDs.
背景与目的
这项横断面观察性病例对照研究于2016年7月启动,旨在加深对功能性胃肠疾病(FGID)潜在发病机制的理解,这些疾病包括肠易激综合征(IBS)、功能性腹泻(FD)和功能性便秘(FC)。具体关注领域包括食物、微生物群、宿主和微生物遗传学、代谢组以及心理变量对不明原因的慢性胃肠道(GI)症状的影响。
方法
本研究招募了在新西兰克赖斯特彻奇的两个内镜检查中心之一接受结肠镜检查的连续患者,以及未接受结肠镜检查的普通公众中的一组参与者。排除患有除FGID以外已知胃肠道疾病的参与者。有症状的参与者被招募为病例组,无症状的参与者被招募为对照组。在准备结肠镜检查的前几天,或者对于未接受结肠镜检查的人来说是合适的时间,除了生物样本(呼气、粪便、血液和尿液)外,还收集了人口统计学、症状、心理、饮食和健康数据。结肠镜检查亚组的参与者在结肠镜检查时进行结肠活检。
结果
2016年7月至2018年12月期间,共招募了349名参与者,其中315名完成了研究,220名参与者来自结肠镜检查亚组,95名来自非结肠镜检查亚组。这包括129名对照组和186名病例组(57名腹泻型IBS为主、30名便秘型IBS为主、41名混合型IBS、42名FC和16名FD)。FGID病例组的平均年龄为53.4岁,对照组为54.4岁。病例组(149/186,80.1%)和对照组(57/72,55.8%)以女性为主。整个队列的教育水平相似。吸烟和饮酒率也相似。按计划从参与者中收集了生物样本。
结论
COMFORT队列是一个独特的FGID病例和对照的临床队列,除了生物样本外,还拥有广泛的人口统计学、饮食、临床、心理和健康数据。未来的研究将旨在使用系统生物学方法来确定饮食、宿主-微生物群相互作用和其他因素在FGID发病机制中的潜在作用。
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