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1. Prevention of rebleeding after primary haemostasis using haemostatic powder in non-variceal upper gastrointestinal bleeding: a multicentre randomised controlled trial.

作者: Jongbeom Shin.;Boram Cha.;Jitaek Hong.;Kye Sook Kwon.;Eunhye Lee.;Jin Hee Maeng.;Jun-Won Chung.;Dong Kyun Park.;Yoon Jae Kim.;Kwang An Kwon.;Jung Ho Kim.;Kwang-Suk Seo.;Su Jin Hong.;Kyoung Oh Kim.
来源: Gut. 2025年
Non-variceal upper gastrointestinal bleeding (NVUGIB) remains a major cause of morbidity and mortality. Rebleeding rates following endoscopic treatment can reach up to 25% within 72 hours in patients with high-risk lesions.

2. Activation of RAS/MEK/ERK signalling drives biliary differentiation in primary liver cancer.

作者: Thomas Rösner.;Carina Rupp.;Christian Lechler.;Ulrike Bauer.;Saumya Sukumary Manmadhan.;Sophia Bernatik.;Fabian Delugré.;Franziska Ihli.;Tanja Derowski.;Simone Jörs.;Birgit Kohnke-Ertel.;Henrik Einwächter.;Nicole Pfarr.;Katja Steiger.;Carolin Mogler.;Maximilian Reichert.;Dieter Saur.;Diana Becker.;Jens U Marquardt.;Rupert Öllinger.;Thomas Engleitner.;Roland Rad.;Roland M Schmid.;Ursula Ehmer.
来源: Gut. 2025年
RAS mutations are frequently observed in human cholangiocarcinoma (CCA), while they are relatively rare in hepatocellular carcinoma (HCC). The role of RAS-dependent signalling pathways in CCA development is currently not well understood.

3. Beneficial infections of the enterovirus genus in patients with liver cancer.

作者: Lichun Ma.;Man Hsin Hung.;Farid Rashidi Mehrabadi.;Limin Wang.;Qin Li.;Marshonna Forgues.;Kathy Cheng Wang.;Anuradha Budhu.;Julián Candia.;Jittiporn Chaisaingmongkol.;Siritida Rabibhadana.;Benjarath Pupacdi.;Mathuros Ruchirawat.;Xin Wei Wang.
来源: Gut. 2025年
Hepatocellular carcinoma (HCC) is a significant global cancer burden, with rising incidence and lacking a unified prevention strategy due to complex aetiologies. Viral exposures may shape host immunity via specific reactive viral antigens that could induce immune responses against hepatocarcinogenesis.

4. Microbiota fasting-related changes ameliorate cognitive decline in obesity and boost ex vivo microglial function through the gut-brain axis.

作者: Virginia Mela.;Violeta Heras.;Monika Iesmantaite.;María Luisa García-Martín.;Manuel Bernal.;Joel D Posligua-García.;Alba Subiri-Verdugo.;José Ignacio Martínez-Montoro.;Ana María Gómez-Pérez.;Borja Banderas.;Isabel Moreno Indias.;Francisco J Tinahones.
来源: Gut. 2025年
Obesity-related cognitive decline is linked to gut microbiota dysbiosis, with emerging evidence suggesting that dietary interventions may ameliorate cognitive impairment via gut-brain axis modulation. The role of microglial cells in this process remains underexplored.

5. British Society of Gastroenterology guidelines on colorectal surveillance in inflammatory bowel disease.

作者: James Edward East.;Morris Gordon.;Gaurav Bhaskar Nigam.;Vassiliki Sinopoulou.;Adrian C Bateman.;Shahida Din.;Marietta Iacucci.;Misha Kabir.;Christopher Andrew Lamb.;Ana Wilson.;Ibrahim Al Bakir.;Anjan Dhar.;Sunil Dolwani.;Omar Faiz.;Ailsa Hart.;Bu'Hussain Hayee.;Chris Healey.;Simon John Leedham.;Marco R Novelli.;Tim Raine.;Matthew D Rutter.;Neil A Shepherd.;Venkataraman Subramanian.;Margaret Vance.;Ruth Wakeman.;Lydia White.;Nigel J Trudgill.;A John Morris.
来源: Gut. 2025年
Patients with inflammatory bowel disease (IBD) remain at increased risk for colorectal cancer and death from colorectal cancer compared with the general population despite improvements in inflammation control with advanced therapies, colonoscopic surveillance and reductions in environmental risk factors. This guideline update from 2010 for colorectal surveillance of patients over 16 years with colonic inflammatory bowel disease was developed by stakeholders representing UK physicians, endoscopists, surgeons, specialist nurses and patients with GRADE (Grading of Recommendations Assessment, Development and Evaluation) methodological support.An a priori protocol was published describing the approach to three levels of statement: GRADE recommendations, good practice statements or expert opinion statements. A systematic review of 7599 publications, with appraisal and GRADE analysis of trials and network meta-analysis, where appropriate, was performed. Risk thresholding guided GRADE judgements.We made 73 statements for the delivery of an IBD colorectal surveillance service, including outcome standards for service and endoscopist audit, and the importance of shared decision-making with patients.Core areas include: risk of colorectal cancer, IBD-related post-colonoscopy colorectal cancer; service organisation and supporting patient concordance; starting and stopping surveillance, who should or should not receive surveillance; risk stratification, including web-based multivariate risk calculation of surveillance intervals; colonoscopic modalities, bowel preparation, biomarkers and artificial intelligence aided detection; chemoprevention; the role of non-conventional dysplasia, serrated lesions and non-targeted biopsies; management of dysplasia, both endoscopic and surgical, and the structure and role of the multidisciplinary team in IBD dysplasia management; training in IBD colonoscopic surveillance, sustainability (green endoscopy), cost-effectiveness and patient experience. Sixteen research priorities are suggested.

6. BSG/ACPGBI guidance on the management of colorectal polyps in patients with limited life expectancy.

作者: Matthew D Rutter.;Ravi Ranjan.;Clare Westwood.;Jamie Barbour.;Adam Biran.;Helen Blackett.;Nicholas Ewin Burr.;John Carlisle.;Barry Clare.;Neil Cripps.;Peter Coyne.;Sunil Dolwani.;Rachel Hodson.;Stephen Holtham.;Noor Mohammed.;Eva J A Morris.;Laura Neilson.;Raymond Oliphant.;John Painter.;Anand Prakash.;Rupert Pullan.;Sanchoy Sarkar.;Marion Sloan.;Michael Swart.;Siwan Thomas-Gibson.;Nigel J Trudgill.;Margaret Vance.;Katie Yeadon.;Linda Sharp.
来源: Gut. 2025年
Determining optimal management of colorectal polyps in patients with limited life expectancy of under 10 years can be difficult, due to challenges balancing an uncertain natural history of polyp progression to symptomatic malignancy versus the increased risk and consequences of polypectomy complications.

7. Systemic treatment in patients with hepatocellular carcinoma and advanced liver dysfunction.

作者: Matthias Pinter.;Claudia A M Fulgenzi.;David J Pinato.;Bernhard Scheiner.
来源: Gut. 2025年
Systemic therapy represents the standard of care treatment for patients with advanced hepatocellular carcinoma (HCC). Given the increased risk of death from cirrhosis-related complications in patients with advanced liver dysfunction, pivotal phase III trials traditionally limited inclusion to patients with Child-Pugh class A, where death is more likely to be attributed to HCC progression. Therefore, Western guidelines recommend the use of systemic therapies primarily in patients with preserved liver function. However, patients with HCC and Child-Pugh class B are commonly encountered in clinical practice, but due to limited prospective evidence, there is no clear guidance on their optimal management.In this recent advances article, we discuss how the clinical course of cirrhosis can affect eligibility to treatment in the modern era of systemic therapy for HCC, elaborate on strategies to improve liver function in HCC patients by targeting cirrhosis-related and tumour-related factors and summarise the current literature on systemic therapy in HCC patients with Child-Pugh class B. Based on this information, we finally propose a clinical algorithm on how to systematically approach patients with HCC and advanced liver dysfunction in clinical practice.

8. Parecoxib sequential with imrecoxib for occurrence and remission of severe acute pancreatitis: a multicentre, double-blind, randomised, placebo-controlled trial.

作者: Luming Huang.;Zhe Feng.;Wenjuan Yang.;Yin Zhu.;Jing Li.;Libin Huang.;Rui Wang.;Lan Peng.;Mingshun He.;Yingmei Tang.;Ping Chen.;Cheng Lan.;Xiaoqing Zhou.;Lin Zhou.;Cheng Ye.;Linhao Zhang.;Jingsun Jiang.;Yanting Ye.;Rui Wang.;Yan He.;Yan Liu.;Hui Gong.;Huifang Xiong.;Liang Xia.;Haiyan Xu.;Bin Zhang.;Rongfang Tu.;Chun Du.;Lujia Cui.;Jinhang Gao.;Zhiyin Huang.;Chengwei Tang.
来源: Gut. 2025年
There is no effective drug treatment for the organ failure (OF) caused by severe acute pancreatitis (SAP).

9. Translational strategies for oral delivery of faecal microbiota transplantation.

作者: Srinivas Kamath.;Robert V Bryant.;Samuel P Costello.;Alice S Day.;Ben Forbes.;Craig Haifer.;Georgina Hold.;Colleen R Kelly.;Anna Li.;Evance Pakuwal.;Andrea Stringer.;Emily C Tucker.;Hannah Rose Wardill.;Paul Joyce.
来源: Gut. 2025年
Faecal microbiota transplantation (FMT) has emerged as a transformative therapy for Clostridioides difficile infections and shows promise for various GI and systemic diseases. However, the poor patient acceptability and accessibility of 'conventional' FMT, typically administered via colonoscopies or enemas, hinders its widespread clinical adoption, particularly for chronic conditions. Oral administration of FMT (OralFMT) overcomes these limitations, yet faces distinct challenges, including a significant capsule burden, palatability concerns and poor microbial viability during gastric transit. This review provides a comprehensive analysis of emerging strategies that aim to advance OralFMT by: (1) refining processing technologies (eg, lyophilisation) that enable manufacturing of low-volume FMT formulations for reducing capsule burden and (2) developing delivery technologies that improve organoleptic acceptability and safeguard the microbiota for targeted colonic release. These advancements present opportunities for OralFMT to expand its therapeutic scope, beyond C. difficile infections, towards chronic GI conditions requiring frequent dosing regimens. While this review primarily focuses on optimising OralFMT delivery, it is important to contextualise these advancements within the broader shift towards defined microbial consortia. Live biotherapeutic products (LBPs) offer an alternative approach, yet the interplay between OralFMT and LBPs in clinical practice remains unresolved. We postulate that continued innovation in OralFMT and LBPs via a multidisciplinary approach can further increase therapeutic efficacy and scalability by enabling disease site targeting, co-delivery of therapeutic compounds and overcoming colonisation resistance. Realising these goals positions OralFMT as a cornerstone of personalised care across a range of diseases rooted in microbiome health.

10. DUOX2 activation drives bacterial translocation and subclinical inflammation in IBD-associated dysbiosis.

作者: Hajar Hazime.;Gloria Michelle Ducasa.;Ana M Santander.;Nivis Brito.;Eddy Ernesto Gonzalez-Horta.;Maria A Quintero.;Stephen Barnes.;Landon Wilson.;Yanping Zhang.;Fahong Yu.;Raad Z Gharaibeh.;Christian Jobin.;Katerina M Faust.;Oriana M Damas.;Amar Deshpande.;David H Kerman.;Siobhan Proksell.;Judith Pignac-Kobinger.;Irina Fernández.;Juan F Burgueño.;Maria T Abreu.
来源: Gut. 2025年
Inflammatory bowel diseases (IBDs) are characterised by dysbiosis and a leaky gut. The NADPH oxidase dual oxidase 2 (DUOX2) is upregulated in patients with IBD, yet its role in driving the disease remains unclear.

11. Integrated multimodel analysis of intestinal inflammation exposes key molecular features of preclinical and clinical IBD.

作者: Miguel Gonzalez-Acera.;Jay V Patankar.;Lena Erkert.;Roodline Cineus.;Reyes Gamez-Belmonte.;Tamara Leupold.;Marvin Bubeck.;Li-Li Bao.;Martin Dinkel.;Ru Wang.;Laura Schickedanz.;Heidi Limberger.;Iris Stolzer.;Katharina Gerlach.;Leonard Diemand.;Fabrizio Mascia.;Pooja Gupta.;Elisabeth Naschberger.;Kristina Koop.;Christina Plattner.;Gregor Sturm.;Benno Weigmann.;Claudia Günther.;Stefan Wirtz.;Michael Stürzl.;Kai Hildner.;Anja A Kühl.;Britta Siegmund.;Andreas Gießl.;Raja Atreya.; .;Ahmed N Hegazy.;Zlatko Trajanoski.;Markus F Neurath.;Christoph Becker.
来源: Gut. 2025年
IBD is a chronic inflammatory condition driven by complex genetic and immune interactions, yet preclinical models often fail to fully recapitulate all aspects of the human disease. A systematic comparison of commonly used IBD models is essential to identify conserved molecular mechanisms and improve translational relevance.

12. DNAJ-PKAc fusion heightens PLK1 inhibitor sensitivity in fibrolamellar carcinoma.

作者: Marina Chan.;Songli Zhu.;Manabu Nukaya.;Luisa T Ferreira.;Sean M Ronnekleiv-Kelly.;Kimberly J Riehle.;John D Scott.;Raymond S Yeung.;Taranjit S Gujral.
来源: Gut. 2025年
Fibrolamellar carcinoma (FLC), a rare and fatal liver cancer lacking effective drug therapy, is driven by the DNAJ-PKAc fusion oncoprotein. However, the underlying mechanism of DNAJ-PKAc's role in FLC tumour growth remains enigmatic.

13. Long-chain sulfatide enrichment is an actionable metabolic vulnerability in intraductal papillary mucinous neoplasm (IPMN)-associated pancreatic cancers.

作者: Yihui Chen.;Riccardo Ballarò.;Marta Sans.;Fredrik Ivar Thege.;Mingxin Zuo.;Rongzhang Dou.;Jimin Min.;Michele Yip-Schneider.;J Zhang.;Ranran Wu.;Ehsan Irajizad.;Yuki Makino.;Kimal I Rajapakshe.;Hamid K Rudsari.;Mark W Hurd.;Ricardo A León-Letelier.;Hiroyuki Katayama.;Edwin Ostrin.;Jody Vykoukal.;Jennifer B Dennison.;Kim-Anh Do.;Samir M Hanash.;Robert A Wolff.;Paolo A Guerrero.;Michael Kim.;C Max Schmidt.;Anirban Maitra.;Johannes F Fahrmann.
来源: Gut. 2025年
We conducted an integrated cross-species spatial assessment of transcriptomic and metabolomic alterations associated with progression of intraductal papillary mucinous neoplasms (IPMNs), which are bona fide cystic precursors of pancreatic ductal adenocarcinoma (PDAC).

14. A Common CTRB misfolding variant associated with pancreatic cancer risk causes ER stress and inflammation in mice.

作者: Cristina Bodas.;Irene Felipe.;Brice Chanez.;Miguel Lafarga.;Evangelina Lopez de Maturana.;Jaime Martinez de Villarreal.;Natalia Del Pozo.;Marina Malumbres.;Pierfrancesco Vargiu.;Ana Cayuela.;Isabel Peset.;Katelyn Connelly.;Jason Hoskins.;Raúl Méndez.;Laufey Amundadottir.;Núria Malats.;Sagrario Ortega.;Francisco X Real.
来源: Gut. 2025年
Genome-wide association studies have identified an exon 6 CTRB2 deletion variant proposed to increase pancreatic cancer risk.

15. Precision risk stratification of primary gastric cancer after eradication of H. pylori by a DNA methylation marker: a multicentre prospective study.

作者: Harumi Yamada.;Seiichiro Abe.;Hadrien Charvat.;Takayuki Ando.;Masahiro Maeda.;Kazunari Murakami.;Shiro Oka.;Takao Maekita.;Mitsushige Sugimoto.;Takahisa Furuta.;Mitsuru Kaise.;Nobutake Yamamichi.;Hiroyuki Takamaru.;Akiko Sasaki.;Ichiro Oda.;Sohachi Nanjo.;Nobuhiro Suzuki.;Toshiro Sugiyama.;Masaaki Kodama.;Kazuhiro Mizukami.;Masanori Ito.;Takahiro Kotachi.;Taichi Shimazu.;Seiichiro Yamamoto.;Toshikazu Ushijima.
来源: Gut. 2025年
Precision cancer risk stratification for gastric cancer is urgently needed for the growing number of healthy people after Helicobacter pylori eradication. The epimutation burden in non-malignant tissues has been associated with cancer risk in multiple cross-sectional studies.

16. Cellular and molecular mechanisms in the pathogenesis of pouchitis: more than just the microbiota.

作者: Manuel B Braga-Neto.;Taha Qazi.;Clifton Fulmer.;Stefan D Holubar.;Claudio Fiocchi.;Andrei I Ivanov.;Florian Rieder.
来源: Gut. 2025年
Pouchitis, defined as inflammation of the ileal pouch, is the most common complication following restorative proctocolectomy for refractory ulcerative colitis. Antibiotics remain the first line of therapy for pouchitis, but the majority of patients develop subsequent episodes and some are refractory to antibiotic therapy. This highlights the need for more effective treatment options and points to a more complex pathophysiology beyond the role of th pouch microbiome, similar to what is seen in inflammatory bowel disease. In this review, we outline the putative mechanisms of pouchitis, including genetic predisposition, microbiome alterations, dysfunction of the intestinal barrier and the immune system and review the available animal models of pouchitis. In addition, we introduce the concept of pouchitis as a possible transmural disease and discuss the potential role of non-immune cells, including stromal cells, in perpetuating inflammation and intestinal barrier dysfunction. We discuss future directions, implications for novel therapies and propose novel multicellular disease models that can better capture the complexity of pouchitis pathogenesis.

17. Choice of colon capsule or colonoscopy versus default colonoscopy in FIT positive patients in the Danish screening programme: a parallel group randomised controlled trial.

作者: Gunnar Baatrup.;Thomas Bjørsum-Meyer.;Lasse Kaalby.;Benedicte Schelde-Olesen.;Morten Kobaek-Larsen.;Anastasios Koulaouzidis.;Rasmus Kroijer.;Issam Al-Najami.;Niels Buch.;Anders Høgh.;Niels Qvist.;Marianne Kirstine Thygesen.;Ulrik Deding.; .
来源: Gut. 2025年
Colonoscopy is among the standard tests for colorectal cancer (CRC) screening. However, uptake varies, and alternatives such as colon capsule endoscopy (CCE) are available. The uptake and detection rate of clinically significant neoplasia with CCE, compared with colonoscopy, remain unclear in this setting.

18. Opposite regulation of intestinal and intrahepatic CD8+ T cells controls alcohol-associated liver disease progression.

作者: Luca Maccioni.;Yukun Guan.;Mariia Kim.;Maria A Parra.;Brandon Peiffer.;Yaojie Fu.;Yang Wang.;Yu-Hong Lin.;Bryan Mackowiak.;Dechun Feng.;Andrew Cameron.;Zhaoli Sun.;George Kunos.;Peter Stärkel.;Bin Gao.
来源: Gut. 2025年
Gut-liver crosstalk plays an important role in alcohol-associated liver disease (ALD) pathogenesis; but underlying mechanisms remain obscure.

19. Reactive cholangiocyte-derived ORM2 drives a pathogenic modulation of the injured biliary niche through macrophage reprogramming.

作者: Hanyang Liu.;Guo Yin.;Bianca Franco Leonardi.;Tian Lan.;Yeni Ait Ahmed.;Hilmar Berger.;Marlene Sophia Kohlhepp.;Natalja Amiridze.;Natalia Martagón Calderón.;Carla Frau.;Ludovic Vallier.;Milad Rezvani.;Frank Tacke.;Adrien Guillot.
来源: Gut. 2025年
Injured or reactive biliary epithelial cells participate in most chronic liver injuries in a process referred to as ductular reaction, which involves multicellular interactions with marked local infiltration of macrophages and fibrogenic cell activation. The direct roles of biliary epithelial cells in shaping their cellular niche remain unknown.

20. Characteristic immune cell interactions in livers of children with acute hepatitis revealed by spatial single-cell analysis identify a possible postacute sequel of COVID-19.

作者: Felix Röttele.;Andreas Zollner.;Carolin Mogler.;Muhammed Yuksel.;Cigdem Arikan.;Vivien Karl.;Judith Helene Aberle.;Stephan W Aberle.;Hubert Kogler.;Andreas Vécsei.;Julia Vodopiutz.;Henrike Salié.;Anne Gräser.;Laurenz Krimmel.;Pius Martin.;Eberhard Lurz.;Felix Immanuel Maier.;Lena Woelfle.;Susana Nobre.;Isabel Goncalves.;Lisa Kern.;Martin Schwemmle.;Tobias Boettler.;Maike Hofmann.;Peter Hasselblatt.;Robert Thimme.;Herbert Tilg.;Thomas Müller.;Georg Friedrich Vogel.;Bertram Bengsch.
来源: Gut. 2025年
A rise in paediatric cases of acute hepatitis of unknown origin (AHUO) was observed in 2022, some requiring liver transplantation. A link to adeno-associated virus 2 infection and CD4+T-cell mediated disease was reported in cohorts in the UK and USA but does not explain all cases.
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