Genetic Control of the Cytotoxic T Cell Response to SV40 Tumor-Associated Specific Antigen

Genetic Control of the Cytotoxic T Cell Response to SV40 Tumor-Associated Specific Antigen

The H-2 gene complex controls the ability of mice to generate cytotoxic T cells to the SV40 tumor-associated specific antigen (TASA). Mice of six H-2 haplotypes (H-2b, d, f, k, q, and s) were challenged in vivo with syngeneic simian virus 40 (SV40)-transformed cells. By testing splenic lymphocytes i...

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Veröffentlicht in:The Journal of immunology (1950) 1979-05, Vol.122 (5), p.1798-1806
Hauptverfasser: Knowles, Barbara B, Koncar, Mirjana, Pfizenmaier, Klaus, Solter, Davor, Aden, David P, Trinchieri, Giorgio
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Antigens, Viral
Cell Differentiation
Cytotoxicity, Immunologic
Epitopes
Immunologic Memory
Male
Mice
Mice, Inbred AKR
Mice, Inbred BALB C
Mice, Inbred C3H
Mice, Inbred C57BL
Mice, Inbred CBA
Simian virus 40 - immunology
T-Lymphocytes - cytology
T-Lymphocytes - immunology
Tumor Virus Infections - immunology
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container_end_page 1806
container_issue 5
container_start_page 1798
container_title The Journal of immunology (1950)
container_volume 122
creator Knowles, Barbara B
Koncar, Mirjana
Pfizenmaier, Klaus
Solter, Davor
Aden, David P
Trinchieri, Giorgio
description The H-2 gene complex controls the ability of mice to generate cytotoxic T cells to the SV40 tumor-associated specific antigen (TASA). Mice of six H-2 haplotypes (H-2b, d, f, k, q, and s) were challenged in vivo with syngeneic simian virus 40 (SV40)-transformed cells. By testing splenic lymphocytes in a 51Cr cytotoxic test, only H-2b mice were able to generate cytotoxic T cells specific for syngeneic SV40-transformed target cells. In contrast, immune lymphocytes from both H-2b and H-2k mice assayed after secondary in vitro restimulation lysed SV40-transformed target cells of appropriate H-2 genotype. Popliteal lymph node cells from H-2b, k, and d mice, immunized by footpad injection of SV40 and then incubated for 14 days in vitro before assay, are cytotoxic for syngeneic SV40-transformed cells. With this immunization protocol, H-2b mice respond to SV40 TASA in association with both the H-2 K and D locus-coded molecules, whereas H-2k mice respond to SV40 TASA in association with the H-2 K molecule only and H-2d mice respond to SV40 TASA in association with the H-2 D gene product. SV40 TASA-immune lymphocytes from various F1 (responder × nonresponder) mice were also unable to lyse syngeneic H-2Kd or H-2Dk SV40-transformed target cells. Inhibition of the response to SV40 TASA in association with H-2Dd is found when lymphocytes from SV40 TASA-immune F1 hybrid (H-2b × H-2d) or H-2 congenic recombinant (H-2KbDd) mice are analyzed. A dominant suppression or recessive helper mechanism is hypothesized to account for these results.
doi_str_mv 10.4049/jimmunol.122.5.1798
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Mice of six H-2 haplotypes (H-2b, d, f, k, q, and s) were challenged in vivo with syngeneic simian virus 40 (SV40)-transformed cells. By testing splenic lymphocytes in a 51Cr cytotoxic test, only H-2b mice were able to generate cytotoxic T cells specific for syngeneic SV40-transformed target cells. In contrast, immune lymphocytes from both H-2b and H-2k mice assayed after secondary in vitro restimulation lysed SV40-transformed target cells of appropriate H-2 genotype. Popliteal lymph node cells from H-2b, k, and d mice, immunized by footpad injection of SV40 and then incubated for 14 days in vitro before assay, are cytotoxic for syngeneic SV40-transformed cells. With this immunization protocol, H-2b mice respond to SV40 TASA in association with both the H-2 K and D locus-coded molecules, whereas H-2k mice respond to SV40 TASA in association with the H-2 K molecule only and H-2d mice respond to SV40 TASA in association with the H-2 D gene product. SV40 TASA-immune lymphocytes from various F1 (responder × nonresponder) mice were also unable to lyse syngeneic H-2Kd or H-2Dk SV40-transformed target cells. Inhibition of the response to SV40 TASA in association with H-2Dd is found when lymphocytes from SV40 TASA-immune F1 hybrid (H-2b × H-2d) or H-2 congenic recombinant (H-2KbDd) mice are analyzed. 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Mice of six H-2 haplotypes (H-2b, d, f, k, q, and s) were challenged in vivo with syngeneic simian virus 40 (SV40)-transformed cells. By testing splenic lymphocytes in a 51Cr cytotoxic test, only H-2b mice were able to generate cytotoxic T cells specific for syngeneic SV40-transformed target cells. In contrast, immune lymphocytes from both H-2b and H-2k mice assayed after secondary in vitro restimulation lysed SV40-transformed target cells of appropriate H-2 genotype. Popliteal lymph node cells from H-2b, k, and d mice, immunized by footpad injection of SV40 and then incubated for 14 days in vitro before assay, are cytotoxic for syngeneic SV40-transformed cells. With this immunization protocol, H-2b mice respond to SV40 TASA in association with both the H-2 K and D locus-coded molecules, whereas H-2k mice respond to SV40 TASA in association with the H-2 K molecule only and H-2d mice respond to SV40 TASA in association with the H-2 D gene product. SV40 TASA-immune lymphocytes from various F1 (responder × nonresponder) mice were also unable to lyse syngeneic H-2Kd or H-2Dk SV40-transformed target cells. Inhibition of the response to SV40 TASA in association with H-2Dd is found when lymphocytes from SV40 TASA-immune F1 hybrid (H-2b × H-2d) or H-2 congenic recombinant (H-2KbDd) mice are analyzed. 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SV40 TASA-immune lymphocytes from various F1 (responder × nonresponder) mice were also unable to lyse syngeneic H-2Kd or H-2Dk SV40-transformed target cells. Inhibition of the response to SV40 TASA in association with H-2Dd is found when lymphocytes from SV40 TASA-immune F1 hybrid (H-2b × H-2d) or H-2 congenic recombinant (H-2KbDd) mice are analyzed. A dominant suppression or recessive helper mechanism is hypothesized to account for these results.</abstract><cop>United States</cop><pub>Am Assoc Immnol</pub><pmid>87443</pmid><doi>10.4049/jimmunol.122.5.1798</doi><tpages>9</tpages><oa>free_for_read</oa></addata></record>
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ispartof The Journal of immunology (1950), 1979-05, Vol.122 (5), p.1798-1806
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source MEDLINE; Alma/SFX Local Collection
subjects Animals
Antigens, Viral
Cell Differentiation
Cytotoxicity, Immunologic
Epitopes
Immunologic Memory
Male
Mice
Mice, Inbred AKR
Mice, Inbred BALB C
Mice, Inbred C3H
Mice, Inbred C57BL
Mice, Inbred CBA
Simian virus 40 - immunology
T-Lymphocytes - cytology
T-Lymphocytes - immunology
Tumor Virus Infections - immunology
title Genetic Control of the Cytotoxic T Cell Response to SV40 Tumor-Associated Specific Antigen
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