Leif Kyrre Berg scite author profile

BackgroundHepatitis C (HCV) infection causes an asymptomatic chronic hepatitis in most affected individuals, which often remains undetected until cirrhosis and cirrhosis-related complications occur. Screening of high-risk subjects in Northern Norway has revealed a relatively low prevalence in the general population (0.24%). Despite this, late complications of HCV infection are increasing. Our object was to estimate the future prevalence and complications of chronic HCV infection in the period 2013–2050 in a low-risk area.MethodsWe have entered available data into a prognostic Markov model to project future complications to HCV infection.ResultsThe model extrapolates the prevalence in the present cohort of HCV-infected individuals, and assumes a stable low incidence in the projection period. We predict an almost three-fold increase in the incidence of cirrhosis (68 per 100,000), of decompensated cirrhosis (21 per 100,000) and of hepatocellular carcinoma (4 per 100,000) by 2050, as well as a six-fold increase in the cumulated number of deaths from HCV-related liver disease (170 per 100,000 inhabitants). All estimates are made assuming an unchanged treatment coverage of approximately 15%. The estimated numbers can be reduced by approximately 50% for cirrhosis, and by approximately one third for the other endpoints if treatment coverage is raised to 50%.ConclusionThese projections from a low-prevalence area indicate a substantial rise in HCV-related morbidity and mortality in the coming years. The global HCV epidemic is of great concern and increased treatment coverage is necessary to reduce the burden of the disease.Electronic supplementary materialThe online version of this article (10.1186/s12879-017-2722-0) contains supplementary material, which is available to authorized users.

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Clinical outcomes in a prospective study of community-acquired hepatitis C virus infection in Northern Norway

Kristiansen

Gutteberg

Mortensen

et al. 2010

Scandinavian Journal of Gastroenterology

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Intestinal inflammatory profile shows increase in a diversity of biomarkers in irritable bowel syndrome

Berg

Goll

Fagerli³

et al. 2020

Scandinavian Journal of Gastroenterology

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Self-reported dietary fructose intolerance in irritable bowel syndrome: Proposed diagnostic criteria

Berg¹

2015

WJG

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AIM: To study the criteria for self-reported dietary fructose intolerance (DFI) and to evaluate subjective global assessment (SGA) as outcome measure. METHODS:Irritable bowel syndrome (IBS) patients were randomized in an open study design with a 2 wk run-in on a habitual IBS diet, followed by 12 wk with/without additional fructose-reduced diet (FRD). Daily registrations of stool frequency and consistency, and symptoms on a visual analog scale (VAS) were performed during the first 4 wk. SGA was used for weekly registrations during the whole study period. Provocation with high-fructose diet was done at the end of the registration period. Fructose breath tests (FBTs) were performed. A total of 182 subjects performed the study according to the protocol (88 FRD, 94 controls). RESULTS:We propose a new clinically feasible diagnostic standard for self-reported fructose intolerance. The instrument is based on VAS registrations of symptom relief on FRD combined with symptom aggravation upon provocation with fructose-rich diet. Using these criteria 43 of 77 patients (56%) in the present cohort of IBS patients had self-reported DFI. To improve the concept for clinical evaluation, we translated the SGA scale instrument to Norwegian and validated it in the context of the IBS diet regimen. The validation procedures showed a sensitivity, specificity and κ value for SGA detecting the self-reported DFI group by FRD response within the IBS patients of 0.79, Randomized Controlled Trial Self

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Leif Kyrre Berg

Effect of fructose-reduced diet in patients with irritable bowel syndrome, and its correlation to a standard fructose breath test

Future complications of chronic hepatitis C in a low-risk area: projections from the hepatitis c study in Northern Norway

Clinical outcomes in a prospective study of community-acquired hepatitis C virus infection in Northern Norway

Intestinal inflammatory profile shows increase in a diversity of biomarkers in irritable bowel syndrome

Self-reported dietary fructose intolerance in irritable bowel syndrome: Proposed diagnostic criteria

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