Hepatitis C virus modulation of lipid and autophagy pathways


Autoria(s): Harty, Ciara
Contribuinte(s)

Fanning, Liam J.

Crosbie, Orla

Kenny-Walsh, Elizabeth

Data(s)

16/09/2016

2016

2016

Resumo

Hepatitis C virus [HCV] infects 170 million people worldwide. We investigated interactions between HCV proteins and cellular proteins involved in autophagy and lipid metabolism. We sought to develop an infection model using patient derived human serum containing HCV and human hepatocytes, Huh7 cells. Using the model, we have shown intracellular expression of incoming HCV RNA (5′ UTR region and region spanning the E1/E2 glycoproteins), expression of the HCV proteins, core and NS5B, and a cellular response to HCV infection. These data suggests this model can be used to analyse the early stage of HCV infection. HCV utilises the autophagy pathway to both establish infection and to complete its life cycle. We investigated HCV interaction with the early stage autophagy protein ATG5. We found that although ATG5 mRNA is unchanged in HCV infected cells, protein expression of ATG5 is significantly upregulated. These data indicated HCV controls the post-transcriptional regulation of ATG5. We used the upstream open reading frame (uORF) and the 5′ UTR region of ATG5 to examine the post-transcriptional regulation. Our data suggest HCV RNA replication either directly or indirectly causes post-transcriptional regulation of the early autophagy protein, ATG5 in a 5′ UTR and uORF independent manner. HCV infection leads to an increase in SREBP controlled genes e.g. HMG-CoA Reductase, cholesterol, LDL and fatty acid synthesis. We hypothesised that HCV infection causes the activation of SREBP pathway by interacting directly or indirectly with proteins involved in the initiation of the pathway. We sought to determine if HCV interacts with SCAP or INSIG. We confirmed a change in LD distribution and HMG-CoA reductase activity as a result of HCV RNA replication. Significantly, we show SCAP protein expression was also altered during HCV RNA replication and HCV core protein possibly interacts with SCAP.

Formato

application/pdf

Identificador

Harty, C. 2016. Hepatitis C virus modulation of lipid and autophagy pathways. PhD Thesis, University College Cork.

http://hdl.handle.net/10468/3095

Idioma(s)

en

Publicador

University College Cork

Direitos

© 2016, Ciara Harty.

http://creativecommons.org/licenses/by-nc-nd/3.0/

Palavras-Chave #Hepatitis C virus #Autophagy #Lipid metabolism
Tipo

Doctoral thesis

Doctoral Degree (Structured)

PhD (Medicine and Health)