106 HBV DNA levels too are lower in HD patients than in patients

106 HBV DNA levels too are lower in HD patients than in patients with normal renal function and hepatitis B infection.107 The explanation for these findings is not certain, but it seems that the altered inflammatory response in ESRD and removal of HBV DNA by dialysis are contributory.108 Regardless, the consequence is that selecting those dialysis patients most likely to develop fibrotic liver changes is not possible with conventional assessment of ALT levels and HBV DNA quantification.109 mTOR inhibitor Ideally, treatment of chronic hepatitis B infection would result in HBsAg seroconversion and clearance of HBV DNA. This is uncommon with current

therapy. A more pragmatic ambition is to suppress viral replication and thereby prevent, or ameliorate, cirrhosis. It is generally agreed that patients with HBsAg positivity, but undetectable viral replication (from HBeAg and HBV DNA levels) do not warrant antiviral treatment if they are to remain on dialysis, although monitoring for complications such as hepatocellular carcinoma LY2835219 mouse should be undertaken.110

In those who are HBsAg-positive and have evidence of viral replication, liver biopsy should be considered, even in the presence of ‘normal’ ALT levels.19,110 Controversy reigns with regard to subsequent initiation of treatment, but those dialysis patients with high HBV DNA levels, or evidence of active inflammation on biopsy are candidates for antiviral therapy. With regard to renal transplant candidates, it is recommended that any patient who is HBsAg positive undergo histological liver evaluation.110 Established cirrhosis before transplantation confers an increased risk of mortality and thus is a contraindication to engraftment of a kidney alone.111 Initiation of antiviral therapy before transplantation should be considered where there is evidence of viral replication on blood very testing. Hepatitis B remains a major health issue in dialysis

patients. Despite the introduction of effective infection control measures to minimize patient-to-patient transmission, occasional outbreaks occur in dialysis units, usually because of lapses in practice. In many parts of the world hepatitis B is endemic and the high background prevalence of the virus is reflected in the dialysis population. An effective vaccine has made a notable contribution to the protection of dialysis patients from the virus, although this is tempered by reduced potency and durability of the anti-HBs response in those with ESRD. The course of hepatitis B infection is different in patients with dialysis-dependent renal failure. Choosing which patients to treat with antiviral therapy, when, and with which drugs, is a subject of uncertainty at present. “
“Aim:  Anaemia management with erythropoiesis-stimulating agents (ESA) and i.v.

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