Apoptosis of the Teratocarcinoma Cell Line Tera-1 Leads to the Cleavage of HERV-K10 super(gag) Proteins by Caspases and/or Granzyme B

Apoptosis of the Teratocarcinoma Cell Line Tera-1 Leads to the Cleavage of HERV-K10 super(gag) Proteins by Caspases and/or Granzyme B

Redistribution, post-translational modifications and coclustering with viral antigens contribute to the immunogenicity of apoptotic cell-derived autoantigens. Almost all known targets of the humoral autoimmune response in systemic lupus erythematosus (SLE) are cleaved by caspases or granzyme B durin...

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Veröffentlicht in:Scandinavian journal of immunology 2002-09, Vol.56 (3), p.303-309
Hauptverfasser: Beyer, T D, Kolowos, W, Dumitriu, I E, Voll, R E, Heyder, P, Gaipl, U S, Kalden, J R, Herrmann, M
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container_issue 3
container_start_page 303
container_title Scandinavian journal of immunology
container_volume 56
creator Beyer, T D
Kolowos, W
Dumitriu, I E
Voll, R E
Heyder, P
Gaipl, U S
Kalden, J R
Herrmann, M
description Redistribution, post-translational modifications and coclustering with viral antigens contribute to the immunogenicity of apoptotic cell-derived autoantigens. Almost all known targets of the humoral autoimmune response in systemic lupus erythematosus (SLE) are cleaved by caspases or granzyme B during apoptosis. Antibodies against retroviral proteins can frequently be detected in the sera of SLE patients without overt retroviral infections. These antibodies may represent cross-reactive antibodies or may have been induced by proteins encoded by endogenous retroviral sequences. We used Tera-1 cells that abundantly express a group-specific antigen of human endogenous retroviruses, HERV-K10 super(gag) polyprotein, to investigate its processing during apoptosis. Tera-1 cells induced to undergo apoptosis showed an altered HERV-K10 super(gag) processing compared with viable cells. In addition, granzyme B was able to cleave HERV-K10 super(gag) isolated from viable Tera-1 cells. Similar to nuclear autoantigens, endogenous retroviral proteins are cleaved during the execution phase of apoptosis. These post-translational modifications may result in the generation of T-cell neoepitopes or a changed epitope hierarchy of retroviral proteins. Therefore, immunogenicity of retroviral antigens in SLE patients may result from a similar mechanism as described for nuclear autoantigens.
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Almost all known targets of the humoral autoimmune response in systemic lupus erythematosus (SLE) are cleaved by caspases or granzyme B during apoptosis. Antibodies against retroviral proteins can frequently be detected in the sera of SLE patients without overt retroviral infections. These antibodies may represent cross-reactive antibodies or may have been induced by proteins encoded by endogenous retroviral sequences. We used Tera-1 cells that abundantly express a group-specific antigen of human endogenous retroviruses, HERV-K10 super(gag) polyprotein, to investigate its processing during apoptosis. Tera-1 cells induced to undergo apoptosis showed an altered HERV-K10 super(gag) processing compared with viable cells. In addition, granzyme B was able to cleave HERV-K10 super(gag) isolated from viable Tera-1 cells. Similar to nuclear autoantigens, endogenous retroviral proteins are cleaved during the execution phase of apoptosis. 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title Apoptosis of the Teratocarcinoma Cell Line Tera-1 Leads to the Cleavage of HERV-K10 super(gag) Proteins by Caspases and/or Granzyme B
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