Strikingly, some of the HCV-mediated mitochondrial dysfunctions c

Strikingly, some of the HCV-mediated mitochondrial dysfunctions could even be rescued by alisporivir. Conclusion:

These observations provide new insights into the pathogenesis of HCV-related liver disease and reveal an additional mechanism of action of alisporivir that is likely beneficial in the treatment of chronic hepatitis C. (HEPATOLOGY 2012) Hepatitis C virus (HCV)-related liver disease represents a major health burden worldwide.1 Treatment with pegylated interferon-α and ribavirin has limited efficacy and numerous adverse effects.2 While a first generation of directly acting antivirals have entered clinical application, targeting host factors essential for the HCV life cycle represents an attractive alternative therapeutic approach. In this context, non-immunosuppressive analogues of the cyclophilin (Cyp) inhibitor cyclosporine A (CsA) represent a new class Selleck Talazoparib of potent anti-HCV agents,3 with efficacy both in vitro as well as in clinical studies in patients with chronic hepatitis C.4-6 Alisporivir (also known as Debio-025 or DEB025) is the prototype and most advanced molecule in this novel class of antivirals. It efficiently inhibits Cyps but, unlike CsA, does selleck chemical not interact with calcineurin, explaining the lack of immunosuppressive effect.7 At least 16 Cyp isoforms are expressed in

human cells, and these are involved in diverse cellular processes and pathways, many of which may influence the HCV life cycle.8 The respective roles of Cyp isoforms in the HCV life cycle remains controversial. However, the peptidyl-prolyl cis-trans isomerase activity of cyclophilin A (CypA)

is crucial for HCV replication, and its inhibition mediates the antiviral activity of alisporivir.9, 10 CypA may interact with different viral proteins and favor a particular conformation that is required for efficient viral replication medchemexpress and/or could have a role in facilitating the processing of the HCV polyprotein.3 Cyclophilin D (CypD) is a member of the family that has been receiving growing attention because of its role in controlling cell fate.11 It is localized within the mitochondrial matrix and interacts with the mitochondrial permeability transition pore (MPTP), sensitizing its opening by physiological inducers.12, 13 Activation of the MPTP allows the rapid passage of low molecular weight molecules and ions (up to 1.5 kDa) and, when persistent, the release of proapoptotic mitochondrial intermembrane proteins, i.e., proteins located between the outer and inner mitochondrial membranes.12 This last event, whose mechanism has not yet been completely clarified, induces adaptive cellular responses that can lead to mitophagy, apoptosis, or necrotic cell death.

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