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eISSN: 2373-6372

Gastroenterology & Hepatology: Open Access

Editorial Volume 9 Issue 2

Hepatitis C (HCV) and human immunodeficiency virus (HIV) infections promote liver fibrosis development by potentiation of liver cell death

Natalia Osna, Larisa Poluektova

Research Service, Veterans Affairs Nebraska-Western Iowa, USA

Correspondence: Natalia Osna, MD, Ph.D, VA Medical Center, R151, 4101 Woolworth Ave, Omaha, NE 68105, US, Tel 1-402-995-3735, Fax 1-402-346-8800

Received: March 19, 2017 | Published: April 10, 2018

Citation: Osna N, Poluektova L. Hepatitis C (HCV) and human immunodeficiency virus (HIV) infections promote liver fibrosis development by potentiation of liver cell death. Gastroenterol Hepatol Open Access. 2018;9(2):72-73. DOI: 10.15406/ghoa.2018.09.00297

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Editorial

HIV and HCV is an often combination, with 7 million people being co-infected worldwide. This co-infection accelerates liver fibrosis even when HIV-replication is controlled by anti-retroviral therapy (ART).1 The alarming factor for co-infection is a high incidence of decompensated liver cirrhosis and HCC, which exceeds the one in mono-infections.2 In the liver, only hepatocytes are productively infected with HCV, while the productive infection of other cell types is questionable. HCV induces oxidative stress and apoptosis in hepatocytes.3 In contrast to HCV, the level of HIV infection in hepatocytes is low or this infection is even latent.4,5 While immune cells expressing CD4 receptor are HIV-permissive, liver transaminases are frequently elevated in the sera of HIV-infected patients even in the absence of accompanying viral hepatitis,6 and there is an association between HIV RNA content in the cells and liver fibrosis.5 Hepatocytes are mildly damaged by HIV-1, but the exposure of HCV-pre-sensitized hepatocytes to HIV leads to increased hepatocyte damage.7,8

The liver and activated immune cells

Due to its central anatomical position, the liver plays a significant role in the maintenance of immune responses to HIV, since it is largely responsible for the clearance of virus from the bloodstream and is supplemented by activated immune cells originated from the gut.9 The liver is considered as a graveyard of activated immune cells that are attracted to dying (apoptotic) hepatocytes and to chemoattractants released by non-parenchymal cells (NPC).10,11 In the liver, there is accumulation of HIV-activated immune cells, and these cells undergo apoptosis.12 In addition to apoptotic hepatocytes, immune cells themselves become a significant source of apoptotic bodies in this organ.

Liver fibrosis

Accompanies intensive hepatocyte death and is characterized by enhanced synthesis and secretion of extracellular matrix (ECM) proteins and its reduced degradation. The main source of ECM during fibrogenesis are hepatic stellate cells (HSC). Fibrosis occurs when ECM proteins accumulate in excessive amounts leading to scarring that increases tissue stiffness.13 To reverse fibrosis, degrading ECM matrix metalloproteinases (MMPs) must overcome the effects of tissue inhibitors of MMPs (TIMPs).14 When apoptosis is massive, apoptotic bodies are captured by liver NPC, Mph and HSC, thereby inducing inflammation and fibrosis.15–17 After massive hepatocyte death, the HSCs are activated into proliferative, fibrogenic and contractile myofibroblasts expressing prostaglandin D receptor that actively produce ECM components, such as type I collagen. Numerous cytokines (like TGFβ) activate HSC for pro-inflammatory response. HIV-1 was reported to infect HSCs in a CD4/chemokine receptor independent manner, resulting in increased expression of collagen-1 and the pro-inflammatory monocyte chemoattractant protein 1 (MCP-1).18 Inflammasome (IFS) plays a role in pro-inflammatory activation of HSC.19 Also, increased density of matrix during liver fibrosis leads to increasing liver stiffness, which is now believed to correlate and contribute to the progression of liver fibrosis.

HIV potentiates fibrosis progression un HCV-infected livers

Recently, we have shown that co-infection of hepatocytes with HIV and HCV induces prominent apoptosis in these cells, and apoptotic bodies engulfed by HSC promote the production of ECM. Interestingly, apoptotic bodies generated from hepatocytes serve as more efficient pro-fibrotic triggers than apoptotic immune cells, which induce pro-inflammatory effects. These effects are HIV-and HCV-specific since the magnitude of pro-fibrotic response is lower when apoptotic bodies were made from HIV-and HCV-negative hepatocytes. To ensure long-term persistence and efficient infection of hepatocytes in cells culture, we have used Huh7.5 cells transfected with CYP2E1 (named RLW cells) and plated on synthetic 2D gels, which makes cultured cells hepatocyte-like.20,21 The obtained data allowed hypothesizing that HIV infection of hepatocytes followed by apoptotic cell death plays a substantial role in the progression of HCV-triggered liver injury. This “second hit” system based on interaction between double-infected apoptotic liver parenchymal and non-parenchymal cells is crucial for further fibrosis development.

Taken together

Co-infection of hepatocytes with HIV and HCV induces apoptotic cell death; Internalization of these apoptotic bodies by hepatic stellate cells promotes liver fibrosis development.

Acknowledgement

None.

Conflict of interest

The author declares no conflict of interest.

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©2018 Osna, et al. This is an open access article distributed under the terms of the, which permits unrestricted use, distribution, and build upon your work non-commercially.

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