60 research outputs found
A micro-elimination approach to addressing hepatitis C in Turkey
Background: In 2016, WHO passed the Global Health Sector Strategy on Viral Hepatitis (GHSS), calling for its elimination by 2030. Two years later, Turkey approved a strategy to reach the WHO targets. This study reports new national prevalence data, breaks it down by subpopulation, and models scenarios to reach HCV elimination.
Methods: Literature was reviewed for estimates of HCV disease burden in Turkey. They were discussed with stakeholders and used as inputs to develop a disease burden model. The infected population was estimated by sequelae for the years 2015–2030. Three scenarios were developed to evaluate the disease burden in Turkey: a Base 2017 scenario, representing the current standard of care in Turkey; an increased treatment scenario, representing the impact of improved access to DAAs; and a WHO targets scenario, which meet the WHO GHSS viral hepatitis targets of a 65% reduction in mortality and 90% diagnosis rate of the infected population by 2030.
Results: At the beginning of 2017, 271,000 viremic infections were estimated. Of these, 58,400 were diagnosed and 10,200 treated. Modelling results showed that, with the current treatment paradigm in Turkey, by 2030 the total number of viremic HCV infections would decline by 35%, while liver-related deaths, hepatocellular carcinoma (HCC), and decompensated cirrhosis would decrease by 10–25%. In the increased treatment scenario, by 2030 viremic HCV infections would decrease by 50%; liver-related deaths, HCC and decompensated cirrhosis would decrease by 45–70%. In the WHO targets scenario, HCV infections would decrease by 80%; sequelae would decrease by 80–85%. Data on disease burden in micro-elimination target subpopulations are largely unavailable.
Conclusions: To meet the WHO Global Health Sector Strategy targets for the elimination of HCV, Turkey needs to increase treatment. Better data are needed as well as countrywide access to DAAs
Multiplex-PCR-based screening and computational modeling of virulence factors and t-cell mediated immunity in helicobacter pylori infections for accurate clinical diagnosis
The outcome of H. pylori infection is closely related with bacteria's virulence factors and host immune response. The association between T cells and H. pylori infection has been identified, but the effects of the nine major H. pylori specific virulence factors; cagA, vacA, oipA, babA, hpaA, napA, dupA, ureA, ureB on T cell response in H. pylori infected patients have not been fully elucidated. We developed a multiplex- PCR assay to detect nine H. pylori virulence genes with in a three PCR reactions. Also, the expression levels of Th1, Th17 and Treg cell specific cytokines and transcription factors were detected by using qRT-PCR assays. Furthermore, a novel expert derived model is developed to identify set of factors and rules that can distinguish the ulcer patients from gastritis patients. Within all virulence factors that we tested, we identified a correlation between the presence of napA virulence gene and ulcer disease as a first data. Additionally, a positive correlation between the H. pylori dupA virulence factor and IFN-γ, and H. pylori babA virulence factor and IL-17 was detected in gastritis and ulcer patients respectively. By using computer-based models, clinical outcomes of a patients infected with H. pylori can be predicted by screening the patient's H. pylori vacA m1/m2, ureA and cagA status and IFN-γ (Th1), IL-17 (Th17), and FOXP3 (Treg) expression levels. Herein, we report, for the first time, the relationship between H. pylori virulence factors and host immune responses for diagnostic prediction of gastric diseases using computer—based models
Securing sustainable funding for viral hepatitis elimination plans
The majority of people infected with chronic hepatitis C
virus (HCV) in the European Union (EU) remain undiagnosed and
untreated. During recent years, immigration to EU has further
increased HCV prevalence. It has been estimated that, out of the
4.2 million adults affected by HCV infection in the 31 EU/
European Economic Area (EEA) countries, as many as
580\xC2\xA0000 are migrants. Additionally, HCV is highly
prevalent and under addressed in Eastern Europe. In 2013, the
introduction of highly effective treatments for HCV with
direct-acting antivirals created an unprecedented opportunity to
cure almost all patients, reduce HCV transmission and eliminate
the disease. However, in many settings, HCV elimination poses a
serious challenge for countries' health spending. On 6 June
2018, the Hepatitis B and C Public Policy Association held the
2nd EU HCV Policy summit. It was emphasized that key
stakeholders should work collaboratively since only a few
countries in the EU are on track to achieve HCV elimination by
2030. In particular, more effort is needed for universal
screening. The micro-elimination approach in specific
populations is less complex and less costly than country-wide
elimination programmes and is an important first step in many
settings. Preliminary data suggest that implementation of the
World Health Organization (WHO) Global Health Sector Strategy on
Viral Hepatitis can be cost saving. However, innovative
financing mechanisms are needed to raise funds upfront for
scaling up screening, treatment and harm reduction interventions
that can lead to HCV elimination by 2030, the stated goal of the
WHO
Epidemiology and viral risk factors for hepatocellular carcinoma in the Eastern Mediterranean countries
Given the high prevalence of viral hepatitis in the Eastern Mediterranean countries, hepatitis B and C infections are the major causes of hepatocellular carcinoma (HCC) in the region. Most cases are associated with cirrhosis related to hepatitis B or C infection. Environmental, host genetic and viral factors can affect the risk of HCC in patients with hepatitis B and C infection. Understanding the epidemiology and viral risk factors in the region provides the implementation of strategies for prevention and treatment of viral hepatitis. Herein, we reviewed the epidemiology, burden of disease and viral risk factors for HCC
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