2242. Cost-effectiveness of laparoscopic ileocaecal resection versus infliximab treatment of terminal ileitis in Crohn's disease: the LIR!C Trial.
作者: E Joline de Groof.;Toer W Stevens.;Emma J Eshuis.;Tjibbe J Gardenbroek.;Judith E Bosmans.;J M van Dongen.;Bregje Mol.;Christianne J Buskens.;Pieter C F Stokkers.;Ailsa Hart.;Geert R D'Haens.;Willem A Bemelman.;Cyriel Y Ponsioen.; .
来源: Gut. 2019年68卷10期1774-1780页
Evaluate the cost-effectiveness of laparoscopic ileocaecal resection compared with infliximab in patients with ileocaecal Crohn's disease failing conventional therapy.
2243. Duration of organ failure impacts mortality in acute pancreatitis.
作者: Na Shi.;Tingting Liu.;Daniel de la Iglesia-Garcia.;Lihui Deng.;Tao Jin.;Lan Lan.;Ping Zhu.;Weiming Hu.;Zongguang Zhou.;Vikesh Singh.;J Enrique Dominguez-Munoz.;John Windsor.;Wei Huang.;Qing Xia.;Robert Sutton.
来源: Gut. 2020年69卷3期604-605页 2244. Prevention of recurrent idiopathic gastroduodenal ulcer bleeding: a double-blind, randomised trial.
作者: Grace L H Wong.;Louis H S Lau.;Jessica Y L Ching.;Yee-Kit Tse.;Rachel H Y Ling.;Vincent W S Wong.;Philip W Y Chiu.;James Y W Lau.;Francis K L Chan.
来源: Gut. 2020年69卷4期652-657页
Patients with a history of Helicobacter pylori-negative idiopathic bleeding ulcers have a considerable risk of recurrent ulcer complications. We hypothesised that a proton pump inhibitor (lansoprazole) is superior to a histamine 2 receptor antagonist (famotidine) for the prevention of recurrent ulcer bleeding in such patients.
2245. First known case of paediatric inflammatory bowel disease in a western lowland gorilla may be linked to a familial mutation in the MEFV gene.
作者: Britt-Sabina Petersen.;Bernd Bokemeyer.;Christian Wenker.;Stefan Hoby.;Katrin Baumgartner.;Hermann Will.;Marc P Hoeppner.;Stefan Schreiber.;Ingo Mecklenburg.;Andre Franke.
来源: Gut. 2020年69卷6期1153-1154页 2246. JAK selectivity for inflammatory bowel disease treatment: does it clinically matter?
作者: Silvio Danese.;Marjorie Argollo.;Catherine Le Berre.;Laurent Peyrin-Biroulet.
来源: Gut. 2019年68卷10期1893-1899页
The two major forms of inflammatory bowel disease (IBD), encompassing Crohn's disease (CD) and ulcerative colitis (UC), are chronic immune-mediated conditions characterised by an increased production of pro-inflammatory cytokines that act as critical drivers of intestinal inflammation. Anti-cytokine therapy has been shown to improve clinical outcomes in IBD. Janus kinases (JAKs) are tyrosine kinases that bind different intracellular cytokine receptors, leading to phosphorylation of signal transducer and activation of transcription molecules implicated on targeted gene transcription. Four isoforms of JAKs have been described: JAK1, JAK2, JAK3 and TYK2. Oral JAK inhibitors (JAKi) have been developed as synergic anti-cytokine therapy in IBD, showing different selectivity towards JAK isoforms. Tofacitinib, a pan-JAK inhibitor, has been recently approved for the treatment of moderate-to-severe UC. With the aim of improving the benefit: risk ratio of this drug class, several second-generation subtype-selective JAKi are under development. However, whether selective inhibition of JAK isoforms is associated with an increased clinical efficacy and/or a better safety profile remains debatable. The aim of this review is to critically review the preclinical and clinical data for the differential selectivity of JAK inhibitors and to summarise the potential clinical implications of the selective JAK inhibitors under development for UC and CD.
2247. Integrated multiomic analysis reveals comprehensive tumour heterogeneity and novel immunophenotypic classification in hepatocellular carcinomas.
作者: Qi Zhang.;Yu Lou.;Jiaqi Yang.;Junli Wang.;Jie Feng.;Yali Zhao.;Lin Wang.;Xing Huang.;Qihan Fu.;Mao Ye.;Xiaozhen Zhang.;Yiwen Chen.;Ce Ma.;Hongbin Ge.;Jianing Wang.;Jiangchao Wu.;Tao Wei.;Qi Chen.;Junqing Wu.;Chengxuan Yu.;Yanyu Xiao.;Xinhua Feng.;Guoji Guo.;Tingbo Liang.;Xueli Bai.
来源: Gut. 2019年68卷11期2019-2031页
Hepatocellular carcinoma (HCC) is heterogeneous, especially in multifocal tumours, which decreases the efficacy of clinical treatments. Understanding tumour heterogeneity is critical when developing novel treatment strategies. However, a comprehensive investigation of tumour heterogeneity in HCC is lacking, and the available evidence regarding tumour heterogeneity has not led to improvements in clinical practice.
2249. Absence of hepatitis E virus RNA in semen samples of infertile male in China.
作者: Lin Wang.;Zhe Zhang.;Jingyi Shu.;Haitao Zhang.;Yuzhuo Yang.;Zhaochao Liang.;Qiyu He.;Weijin Huang.;Youchun Wang.;Hui Zhuang.;Hui Jiang.;Ling Wang.
来源: Gut. 2020年69卷7期1363-1364页 2250. Yogurt consumption and risk of conventional and serrated precursors of colorectal cancer.
作者: Xiaobin Zheng.;Kana Wu.;Mingyang Song.;Shuji Ogino.;Charles S Fuchs.;Andrew T Chan.;Edward L Giovannucci.;Yin Cao.;Xuehong Zhang.
来源: Gut. 2020年69卷5期970-972页 2254. β6 integrinosis: a new lethal autosomal recessive ITGB6 disorder leading to impaired conformational transitions of the αVβ6 integrin receptor.
作者: Patrick Weil.;Rhea van den Bruck.;Thomas Ziegenhals.;Stefan Juranek.;Daniel Goedde.;Valerie Orth.;Stefan Wirth.;Andreas C Jenke.;Jan Postberg.
来源: Gut. 2020年69卷7期1359-1361页 2255. Morphological classification of pancreatic ductal adenocarcinoma that predicts molecular subtypes and correlates with clinical outcome.
作者: Sangeetha N Kalimuthu.;Gavin W Wilson.;Robert C Grant.;Matthew Seto.;Grainne O'Kane.;Rajkumar Vajpeyi.;Faiyaz Notta.;Steven Gallinger.;Runjan Chetty.
来源: Gut. 2020年69卷2期317-328页
Transcriptional analyses have identified several distinct molecular subtypes in pancreatic ductal adenocarcinoma (PDAC) that have prognostic and potential therapeutic significance. However, to date, an indepth, clinicomorphological correlation of these molecular subtypes has not been performed. We sought to identify specific morphological patterns to compare with known molecular subtypes, interrogate their biological significance, and furthermore reappraise the current grading system in PDAC.
2256. Alterations of gut microbiome in autoimmune hepatitis.
作者: Yiran Wei.;Yanmei Li.;Li Yan.;Chunyan Sun.;Qi Miao.;Qixia Wang.;Xiao Xiao.;Min Lian.;Bo Li.;Yong Chen.;Jun Zhang.;You Li.;Bingyuan Huang.;Yikang Li.;Qin Cao.;Zhuping Fan.;Xiaoyu Chen.;Jing-Yuan Fang.;Merrill Eric Gershwin.;Ruqi Tang.;Xiong Ma.
来源: Gut. 2020年69卷3期569-577页
The significance of the liver-microbiome axis has been increasingly recognised as a major modulator of autoimmunity. The aim of this study was to take advantage of a large well-defined corticosteroids treatment-naïve group of patients with autoimmune hepatitis (AIH) to rigorously characterise gut dysbiosis compared with healthy controls.
2257. Introduction of anti-TNF therapy has not yielded expected declines in hospitalisation and intestinal resection rates in inflammatory bowel diseases: a population-based interrupted time series study.
作者: Sanjay K Murthy.;Jahanara Begum.;Eric I Benchimol.;Charles N Bernstein.;Gilaad G Kaplan.;Jeffrey D McCurdy.;Harminder Singh.;Laura Targownik.;Monica Taljaard.
来源: Gut. 2020年69卷2期274-282页
To better understand the real-world impact of biologic therapy in persons with Crohn's disease (CD) and ulcerative colitis (UC), we evaluated the effect of marketplace introduction of infliximab on the population rates of hospitalisations and surgeries and public payer drug costs.
2258. Milk polar lipids reduce lipid cardiovascular risk factors in overweight postmenopausal women: towards a gut sphingomyelin-cholesterol interplay.
作者: Cécile Vors.;Laurie Joumard-Cubizolles.;Manon Lecomte.;Emmanuel Combe.;Lemlih Ouchchane.;Jocelyne Drai.;Ketsia Raynal.;Florent Joffre.;Laure Meiller.;Mélanie Le Barz.;Patrice Gaborit.;Aurélie Caille.;Monique Sothier.;Carla Domingues-Faria.;Adeline Blot.;Aurélie Wauquier.;Emilie Blond.;Valérie Sauvinet.;Geneviève Gésan-Guiziou.;Jean-Pierre Bodin.;Philippe Moulin.;David Cheillan.;Hubert Vidal.;Béatrice Morio.;Eddy Cotte.;Françoise Morel-Laporte.;Martine Laville.;Annick Bernalier-Donadille.;Stéphanie Lambert-Porcheron.;Corinne Malpuech-Brugère.;Marie-Caroline Michalski.
来源: Gut. 2020年69卷3期487-501页
To investigate whether milk polar lipids (PL) impact human intestinal lipid absorption, metabolism, microbiota and associated markers of cardiometabolic health.
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