Impairment of left ventricular function in combined immune deficiency mice after transfer of peripheral blood leukocytes from patients with myocarditis

doi:10.1093/eurheartj/16.suppl_O.59

European Heart Journal 1995 16(Supplement O):59-63; doi:10.1093/eurheartj/16.suppl_O.59
Copyright © 1995 by the European Society of Cardiology.

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Impairment of left ventricular function in combined immune deficiency mice after transfer of peripheral blood leukocytes from patients with myocarditis

P. L. Schwimmbeck, C. Badorff, G. Rohn, K. Schulze and H. P. Schultheiss

Department of Internal Medicine/Cardiology, Benjamin Franklin Hospital, Free University Berlin Berlin, Germany

Peter L. Schwimmbeck. MD, Department of Internal Aedicine/Cariology. Benjamin Franklin Hospital. Free University Berlin, Hindenburgdamn 30, 12200 Berlin, Germany.

Autoimmune mechanisms are suspected to play an important rolein the pathogenesis of human myocarditis. In order to evaluatethe significance of autoimmune leukocytes for the developmentof human myocarditis (MC) and subsequent heart failure, we transferred15 x 10⁶ or 50 x 10⁶ peripheral blood leukocytes (PBLs) frompatients with immunohistologically proven MC and impaired leftventricular function into severe combined immune deficiency(SCID) mice that possess neither B nor T lymphocytes. PBLs fromseven patients and five healthy controls were transferred intothree SCID mice each by intraperitoneal injection. After 60days human PBLs could be demonstrated in the peripheral bloodof SCID mice, representing up to 10% of peripheral blood mononuclearcells. Likewise, human immunoglobulins were present in all transfusedSCID mice (up to 3 mg.ml^-1 IgG and IgM); however, autoantibodiesagainst the adenine nucleotide translocator, a myocardial autoantigen,were only present in the mice receiving PBLs from patients withMC. Infiltrating human lymphocytes were also only found in thehearts of SCID mice having received PBLs from MC patients, butnot in those receiving PBLs from normal controls. When we measuredthe slope of the left ventricular pressure pulse by direct punctureunder ether anaesthesia, we found it to be decreased (dp/dl=1750 ± 194 mmHg.s^-1) in mice receiving PBLs from MCpatients, compared with mice receiving PBLs from controls (dp/dl= 2456 ± 92 mmHg.s^-1) or receiving no transfusion (dp/dt= 2576 ± 142 mmHg.s^-1). These results demonstrate thatthe impairment of the ventricular function seen in patientswith MC can be transferred to SCID mice by transfer of PBLs.This proves the significance of autoimmune mechanisms for thepathogenesis of MC.

Key Words: Transfer of myocarditis • peripheral blood leukocytes • severe combined immune deficiency (SCID) mice • cellular infiltrates • autoantibodies

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