A novel lymphoproliferative/autoimmune syndrome resembling murine lpr/gld disease

M C Sneller, S E Straus, E S Jaffe, J S Jaffe, T A Fleisher, M Stetler-Stevenson, W Strober, M C Sneller, S E Straus, E S Jaffe, J S Jaffe, T A Fleisher, M Stetler-Stevenson, W Strober

Abstract

In mice, the two distinct autosomal recessive genes lpr and gld can induce a syndrome characterized by autoantibody formation and the progressive accumulation of an unusual CD4-CD8- T cell population in peripheral lymphoid tissue. This phenotype does not precisely mirror any human disease. In this report we describe two patients with a progressive lymphoproliferative disorder associated with autoimmunity. The peripheral blood and lymph nodes of these patients contained large numbers of an unusual CD4-CD8- T cell population. These CD4-CD8- T cells express surface markers characteristic of mature peripheral blood T cells (CD3, CD2, CD5), express the alpha/beta form of the T cell receptor, and do not express surface markers characteristic of immature thymocytes (CD1) or NK cells (CD16, CD56). Functionally, these cells exhibited deficient proliferation and lymphokine production upon stimulation with mitogenic antibodies to CD3 or CD2. Both proliferation and lymphokine production could be augmented by co-stimulation with an antibody directed at the CD28 determinant. The clinical and immunological features of this syndrome resemble the lymphoproliferative/autoimmune disease seen in lpr and gld mice.

References

    1. J Exp Med. 1989 Mar 1;169(3):795-806
    1. Nature. 1989 Oct 5;341(6241):447-50
    1. FASEB J. 1987 Aug;1(2):103-9
    1. J Immunol. 1987 Mar 15;138(6):1660-6
    1. Nature. 1988 Jun 23;333(6175):742-6
    1. J Immunol. 1987 Jan 1;138(1):157-63
    1. J Exp Med. 1983 Jul 1;158(1):126-45
    1. Proc Natl Acad Sci U S A. 1984 Feb;81(3):881-5
    1. J Immunol. 1981 Apr;126(4):1473-7
    1. J Immunol. 1991 Feb 15;146(4):1113-7
    1. Scand J Immunol. 1991 Nov;34(5):635-45
    1. Annu Rev Immunol. 1991;9:243-69
    1. Nature. 1990 Jul 19;346(6281):271-4
    1. J Immunol. 1990 May 15;144(10):3762-9
    1. Immunol Today. 1990 Jun;11(6):211-6
    1. Adv Immunol. 1989;44:207-64
    1. Proc Natl Acad Sci U S A. 1989 Jul;86(13):5059-63
    1. J Immunol. 1989 Jul 1;143(1):103-12
    1. N Engl J Med. 1989 Oct 19;321(16):1080-5
    1. J Exp Med. 1986 Feb 1;163(2):383-99
    1. J Immunol. 1986 May 1;136(9):3282-7
    1. J Exp Med. 1988 May 1;167(5):1713-8
    1. J Immunol. 1988 Sep 15;141(6):1848-54
    1. Proc Natl Acad Sci U S A. 1985 Sep;82(18):6268-71
    1. Cell. 1981 Dec;27(3 Pt 2):583-91
    1. J Immunol. 1984 Oct;133(4):1710-5
    1. Cell. 1984 Apr;36(4):897-906
    1. J Immunol. 1984 Jul;133(1):227-33
    1. J Immunol. 1980 Aug;125(2):871-3
    1. J Exp Med. 1990 Dec 1;172(6):1805-17
    1. J Immunol. 1990 May 15;144(10):3756-61
    1. J Immunol. 1990 Jun 15;144(12):4507-12
    1. J Immunol. 1989 Jul 1;143(1):153-61

Source: PubMed

Szponzorok és közreműködők

Egészségi állapot

Kábítószer-beavatkozások

3
Iratkozz fel