Hepatitis C virus infection in kidney transplantation-changing paradigms with novel agents.
Yuvaram N V ReddyDavid NunesVipul ChitaliaCraig E GordonJean M FrancisPublished in: Hemodialysis international. International Symposium on Home Hemodialysis (2019)
Hepatitis C virus (HCV) is a common cause of increased morbidity and mortality in kidney transplant patients. It is associated with posttransplant glomerulonephritis, chronic allograft nephropathy, and New Onset Diabetes after Transplant (NODAT). In the past, HCV was difficult to treat due to the presence of interferon alpha-based therapies that were difficult to tolerate and were associated with adverse side-effects, such as the risk of rejection. With the advent of oral directly acting antiviral therapies, the landscape for HCV and transplantation has changed. These agents are highly effective and well tolerated with minimal side-effects. Sustained viral response rates in excess of 90% are achieved with most current treatment regimens active against all HCV genotypes. These new agents may show an improvement in graft and patient survival while essentially eliminating the risk of acute rejection from the use of prior interferon-based HCV therapies. These agents may also result in an improvement in organ allocation for HCV donor/HCV recipient transplantation. This review is meant to discuss the epidemiology of HCV, the new oral direct-acting antiviral agents (DAAs) and future opportunities for research in the field of HCV related transplantation.
Keyphrases
- hepatitis c virus
- human immunodeficiency virus
- kidney transplantation
- cardiovascular disease
- ejection fraction
- immune response
- liver failure
- dendritic cells
- risk factors
- hepatitis c virus infection
- bone marrow
- newly diagnosed
- intensive care unit
- case report
- skeletal muscle
- hepatitis b virus
- current status
- hiv infected
- single cell
- acute respiratory distress syndrome
- extracorporeal membrane oxygenation
- aortic dissection
- replacement therapy
- free survival