The lymphoreticular system in triggering virus plus self-specific cytotoxic T cells: evidence for T help.

Rm, Zinkernagel; Callahan, Gerald N.; Althage, Alana; Cooper, Sheila; Streilein, J. Wayne; Klein, Jan

doi:10.1084/jem.147.3.897

Cited by 256 publications

(129 citation statements)

References 34 publications

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“…This does not mean that help would be required in CTL responses to all other antigens as well. We found that in completely allogeneic chimeras excellent CTL responses to H-2 antigens were obtained which, according to the suggestion of Zinkernagel et al (8), would be independent of T-cell help. …”

Section: Involvement Of Helper Cells In Thementioning

confidence: 64%

Distinct Ir genes for helper and killer cells in the cytotoxic response to H-Y antigen.

Boehmer¹,

Haas²

1979

The Journal of Experimental Medicine

113

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The H-Y-specific cytotoxic T-cell response requires helper cells: cells from bone marrow chimeras B6 X CBA leads to B6, B6 X CBA leads to B10.A (5R), or B6 X CBA leads to CBA are each unable to respond to H-2k male cells. If, however, cells from B6 X CBA leads to B6 or B6 X CBA leads to B10.A (5R) chimeras are adoptively transferred together with cells from B6 X CBA leads to CBA chimeras, H-Y-specific CTL restricted to H-2k can be obtained. Thus, cells from B6 X CBA leads to B6 or B6 X CBA leads to B10.,A (5R) chimeras (restricted to the left end of the H-2b haplotype) can help CTL precursors from B6 X CBA leads to CBA chimeras (restricted to H-2k). The two classes of T cells required for the CTL response to H-Y antigen are controlled by different IR genes. All H-Y-specific CTL obtained from chimeras B6 + CBA leads to B6 X CBA were found to be of B6 origin. This suggests that CTL or their precursors must express antigens encoded in the left end of the H-2b haplotype for interaction with helper cells.

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Section: Involvement Of Helper Cells In Thementioning

confidence: 64%

Distinct Ir genes for helper and killer cells in the cytotoxic response to H-Y antigen.

Boehmer¹,

Haas²

1979

The Journal of Experimental Medicine

113

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mentioning

confidence: 99%

“…Nonetheless, on the basis of mostly indirect results from a variety of experimental approaches, the most prevalent model of CTL activation is one that closely parallels models of B cell activation, i.e., that I regionrestricted helper T cells activated by interaction with antigen in the context of I region determinants deliver inducing signals to antigen-activated precursor CTL (1)(2)(3)(4)(5). In some models, the helper T cell interacts with CTL precursors via the restricted recognition of I region determinants expressed by the CTL precursor (1,2). Experiments interpreted as supporting the role of I region-recognition events during the process of CTL induction include (a) studies demonstrating the augmentation of CTL responses to foreign H-2K and D antigens by I region-reactive T cells (5,6), (b) studies of CTL responses to viral (2) or non-H-2 cell surface antigens (7) or hapten (8), demonstrating an influence of I region genes expressed by cells of the thymus on the response phenotype of T cells that mature therein, (c) a study demonstrating the apparent depletion, by in vivo negative selection procedures, of I region-restricted helper cells required for an in vitro secondary CTL response specific for minor histocompatibility antigens (9), and (d) the finding that Ia + non-T accessory cells are required for in vitro CTL responses (4, 10, 1 1).…”

mentioning

confidence: 99%

“…In some models, the helper T cell interacts with CTL precursors via the restricted recognition of I region determinants expressed by the CTL precursor (1,2). Experiments interpreted as supporting the role of I region-recognition events during the process of CTL induction include (a) studies demonstrating the augmentation of CTL responses to foreign H-2K and D antigens by I region-reactive T cells (5,6), (b) studies of CTL responses to viral (2) or non-H-2 cell surface antigens (7) or hapten (8), demonstrating an influence of I region genes expressed by cells of the thymus on the response phenotype of T cells that mature therein, (c) a study demonstrating the apparent depletion, by in vivo negative selection procedures, of I region-restricted helper cells required for an in vitro secondary CTL response specific for minor histocompatibility antigens (9), and (d) the finding that Ia + non-T accessory cells are required for in vitro CTL responses (4, 10, 1 1). In addition, studies of the Ir gene defect ofnonresponder strains in the CTL response of female mice to the male antigen, H-Y, have been interpreted in terms of I region-restricted helper T cells (1,7,(12)(13)(14)(15).…”

mentioning

confidence: 99%

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Helper T cells for cytotoxic T lymphocytes need not be I region restricted

Raulet¹,

Bevan²

1982

The Journal of Experimental Medicine

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The development of procedures for the physical or functional separation of B cells and helper T cells permitted extensive studies to be performed that have elucidated the nature of cell-cell interactions that occur during the antibody response. Current models of B cell activation state that antigen-specific helper T cells are activated by recognition of antigen in the context of H-2 I region-encoded determinants on specialized antigen-presenting cells (APC) 1 and then deliver inducing signals to antigen-activated B cells via recognition of antigen plus I region determinants on the B Cell.In contrast, studies of cellular interactions in the cytotoxic T lymphocyte (CTL) response have been hampered by the inability to cleanly separate CTL precursors from their helper T cells (see Discussion). Nonetheless, on the basis of mostly indirect results from a variety of experimental approaches, the most prevalent model of CTL activation is one that closely parallels models of B cell activation, i.e., that I regionrestricted helper T cells activated by interaction with antigen in the context of I region determinants deliver inducing signals to antigen-activated precursor CTL (1-5). In some models, the helper T cell interacts with CTL precursors via the restricted recognition of I region determinants expressed by the CTL precursor (1, 2). Experiments interpreted as supporting the role of I region-recognition events during the process of CTL induction include (a) studies demonstrating the augmentation of CTL responses to foreign H-2K and D antigens by I region-reactive T cells (5, 6), (b) studies of CTL responses to viral (2) or non-H-2 cell surface antigens (7) or hapten (8), demonstrating an influence of I region genes expressed by cells of the thymus on the response phenotype of T cells that mature therein, (c) a study demonstrating the apparent depletion, by in vivo negative selection procedures, of I region-restricted helper cells required for an in vitro secondary CTL response specific for minor histocompatibility antigens (9), and (d) the finding that Ia + non-T accessory cells are required for in vitro CTL responses (4, 10, 1 1). In addition, studies of the Ir gene defect ofnonresponder strains in the CTL response of female mice to the male antigen, H-Y, have been interpreted in terms of I region-restricted helper T cells (1,7,(12)(13)(14)(15).

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“…A gene regulating testosterone metabolism is linked to the major histocompatibility complex (H-2) of the mouse (72). Finally, during differentiation of T cells, the ability to recognize "self" versus "'nonself" with respect to the ability to respond normally to virus infections is determined by the thymic epithelial cells and not other cells of the body (73). These epithelial cells are the source of the thymic hormones.…”

Section: Endocrine Status With Respect To Age and Immunitymentioning

confidence: 99%

Effect of Age on Immune Function in Terms of Chemically Induced Cancers

Bennett¹

1979

Environmental Health Perspectives

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Neonatal, fetal, and very old animals are particularly sensitive to chemical carcinogenesis. Reasons for this increased sensitivity could be due to increased susceptibility of "target" organs or cells, peculiar hormonal levels at these age groups, relatively deficient immune functions, or combinations of these and/or other factors. During the late fetal and first three weeks of neonatal life, the immune system is rapidly maturing, is relatively incompetent, and its diverse components are developing at different rates. Gonadotrophic hormones of the pituitary or placenta are high during pregnancy, the early neonatal period, after the menopause, and in a large fraction of men over 60 years of age. These and other hormones are immunosuppressive and could theoretically facilitate carcinogenesis. The particular immune cell type, if any, responsible for resistance to chemically induced tumors has not been determined. One can only state that susceptibility to chemical carcinogenesis is associated with a relative dysfunction of the immune system and that age is an important factor.

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The lymphoreticular system in triggering virus plus self-specific cytotoxic T cells: evidence for T help.

Cited by 256 publications

References 34 publications

Distinct Ir genes for helper and killer cells in the cytotoxic response to H-Y antigen.

Distinct Ir genes for helper and killer cells in the cytotoxic response to H-Y antigen.

Helper T cells for cytotoxic T lymphocytes need not be I region restricted

Effect of Age on Immune Function in Terms of Chemically Induced Cancers

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