ACUTE DESTRUCTION BY HUMORAL ANTIBODY OF RAT SKIN GRAFTED TO MICE: THE ROLE OF COMPLEMENT AND POLYMORPHONUCLEAR LEUKOCYTES

doi:10.1084/jem.137.4.893

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ACUTE DESTRUCTION BY HUMORAL ANTIBODY OF RAT SKIN GRAFTED TO MICE : THE ROLE OF COMPLEMENT AND POLYMORPHONUCLEAR LEUKOCYTES

Henry J. Winn ¹, Conrad A. Baldamus ¹, Somarie V. Jooste ¹, and Paul S. Russell ¹

¹ From the Transplant Unit, General Surgical Services, and the Department of Surgery, Harvard Medical School at the Massachusetts General Hospital, Boston, Massachusetts 02114

A study has been made of the roles played by complement andpolymorphonuclear leukocytes (PMN) in the acute destructionof xenografts of rat skin that follows injection of their hostswith antisera specifically reactive with graft antigens. Therat skin was grafted onto mice whose immune responses were suppressedby removal of the thymus and a brief course of treatment withrabbit antimouse lymphocyte serum. At about 2 wk after graftingthe mice were injected intravenously or intraperitoneally withmouse antirat serum (MARS). This time interval was chosen becauseit avoided the complications that might be associated with eitherthe process of healing in or with incipient rejection. Signsof graft damage were evident as early as 10 min after the injectionof MARS, and in most animals so injected the grafts were completelydestroyed within 24–48 h.

The role of complement (C) inthis acute destructive process is indicated by the results ofthree lines of experimentation. (a) Non-C-fixing antibodiesor antibody fragments failed to cause damage to the grafts.Indeed, both chicken antirat serum and F(ab')₂ fragments fromrabbit antirat serum completely protected the grafts againstthe effects of MARS that was administered 24 h later. (b) Whenmice were depleted of hemolytic C by treatment with cobra venomfactor or heat-aggregated gamma globulin, the damage causedby MARS was greatly reduced or completely inhibited. (c) Inmice with a genetically determined absence of C5 much greaterquantities of MARS were required to cause graft damage; thetempo of the destructive process was consistently slower; anda greater number of grafts recovered from the initial inflammatoryprocess than was the case for animals with an intact complementsystem.

The participation of PMN in serum-mediated destructionof grafts was initially suggested by the results of microscopeexamination of fixed tissues. The essential role of these cellsin the process is indicated by the failure of MARS to causetissue damage in mice whose circulating PMN have been reducedto very low levels by treatment with nitrogen mustard or morespecifically with an anti-PMN serum.

The absence of tissue damagewhen circulating PMN are reduced but C levels are normal suggeststhat C-mediated cytolysis is unimportant in graft destructionand that the role of C lies in its ability to generate chemotacticfactors. The latter may then attract the PMN that provide mediatorsof tissue damage.

Submitted on December 28, 1972

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