Jiashun Li scite author profile

These studies show that both CD4+ and CD8+ T cells (but not host NTC) can independently initiate the rejection of allogeneic hepatocytes. While hepatocyte rejection by isolated CD4+ T cells is not surprising, rejection by CD8+ T cells (in the absence of CD4+ T cells) was unusual, and may explain the failure of "standard" immunosuppressive regimens to suppress acute rejection of allogeneic hepatocytes, as noted in prior studies. Furthermore, NK cells do not appear to be required for either CD4+ T cell or CD8+ T cell initiated hepatocyte rejection.

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Proton Channel Activity of Influenza A Virus Matrix Protein 2 Contributes to Autophagy Arrest

Ren

Feng

et al. 2016

J Virol

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cInfluenza A virus infection can arrest autophagy, as evidenced by autophagosome accumulation in infected cells. Here, we report that this autophagosome accumulation can be inhibited by amantadine, an antiviral proton channel inhibitor, in amantadinesensitive virus infected cells or cells expressing influenza A virus matrix protein 2 (M2). Thus, M2 proton channel activity plays a role in blocking the fusion of autophagosomes with lysosomes, which might be a key mechanism for arresting autophagy.

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In Vivo Immunogenicity of Purified Allogeneic Hepatocytes in a Murine Hepatocyte Transplant Model1,2

Bumgardner

Li²,

Heininger³

et al. 1998

Transplantation

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Jiashun Li

A Functional Model of Hepatocyte Transplantation for in Vivo Immunologic Studies1,2

Rejection Responses to Allogeneic Hepatocytes by Reconstituted Scid Mice, Cd4 Ko, and Cd8 Ko Mice1,2

Proton Channel Activity of Influenza A Virus Matrix Protein 2 Contributes to Autophagy Arrest

In Vivo Immunogenicity of Purified Allogeneic Hepatocytes in a Murine Hepatocyte Transplant Model1,2

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