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Open AccessJournal ArticleDOI

Cellular and vascular components of the allograft reaction : evidence from returned skin allografts

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TLDR
In order to gain added insight into the mechanisms of allograft destruction, skin grafts were returned to their original donors after remaining as allografteds long enough to induce immunity in the intermediate host but not longenough to cause destruction of the graft.
Abstract
In order to gain added insight into the mechanisms of allograft destruction, skin grafts were returned to their original donors after remaining as allografts long enough to induce immunity in the intermediate host but not long enough to cause destruction of the graft. Upon their return to unmodified donors, such grafts became revascularized and remained viable. An intense cellular infiltration was incited within the graft and its draining lymph node by the interaction between immunologically competent cells, some antigenically activated, that were transferred from the intermediate host with the graft, and those of the final host, the original donor. This immune interaction excited a nonspecific granulocytic and histiocytic response, which led to the destruction of the adjacent epithelium already re-accepted within its native habitat. This mechanism of epithelial destruction required vascular connection to permit the cellular infiltration, and was unlikely to have primarily involved circulating antibody. When similar grafts were returned to donors that had been sensitized to the intermediate host, vascularization and reacceptance of the graft did not occur. No cellular infiltration took place in the graft and no lymph node response was evoked. The returned grafts were cast off as full-thickness sloughs. Here the mechanism of graft rejection was apparently an interaction between the preformed antibody of the specifically sensitized host and the allogeneic cells transferred from the intermediate host; this interaction prevented the vascularization of the graft, even though the endothelia involved were autologous. In unmodified allografts, both the character and the variability of the histologic patterns can be accounted for by the superimposition, in differing rates and degrees, of humoral vascular effects upon cellular events already in progress.

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Book ChapterDOI

In Vitro Approaches to the Mechanism of Cell-Mediated Immune Reactions

TL;DR: This chapter focusses on the study of cell-mediated immunity in vitro, principally in terms of explaining the effector process of the response, with general assumptions that all cell- mediated immune reactions have a common basis.
Book ChapterDOI

Genetics and Immunology of Sex-Linked Antigens

TL;DR: Although the Y antigen of mice is clearly a sex-limited trait, its sex-linked status remains somewhat controversial.
Journal ArticleDOI

Antigen-mediated macrophage adherence inhibition

TL;DR: Antigen-mediated macrophage adherence inhibition (MAI) was studied in inbred rats immunized with various transplantation, tumour-specific and protein antigens and seems to be due to the direct interaction of the respective antigen with a corresponding PC receptor.
Journal ArticleDOI

H‐Y Antigen: Genetics and Serology

TL;DR: H-Y antigen has been studied extensively, both as a prototypical weak transplantation antigen (in a system that may represent a simple genetic disparity between donor and host) and as a plasma membrane component concerned in the morphogenesis of the heterogametic gonad.
References
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Journal ArticleDOI

“Lymphokines”: Non-Antibody Mediators of Cellular Immunity generated by Lymphocyte Activation

TL;DR: Four principal features of cellular immunity in the guinea-pig are mediated by a group of soluble factors generated by antigen-activated lymphocytes, which are different from classical antibodies.
Journal ArticleDOI

Humoral antibodies in renal allotransplantation in man.

TL;DR: A very high correlation was found between the occurrence of antibodies reactive with graft antigens and histologic evidence of vascular lesions, particularly those of an obliterative nature, in renal-allograft recipients tested.
Journal ArticleDOI

The H-Y transplantation antigen: a Y-linked or sex-influenced factor?

TL;DR: The complete penetrance of the Y factor in C57 mice is due to the females of this strain being relatively strong reactors against male skin isografts, and is not because the antigen is strongest in this strain.
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