Numerous studies have shown the etiology of Systemic Lupus Erythematosus (SLE) to be multifactorial though most investigations have shown an altered immune system to be the final pathway in expression of the autoimmune disease. Some lines of evidence have found a defect in cell mediated immunity and a specific defect of T-suppressor cells has been demonstrated. Familial studies, especially twin studies, have shown a high incidence of altered immune status in family members, an increased incidence of SLE among family members and a greater than 50% incidence of SLE among monozygotic twins. Other studies have suggested an environmental influence with the presence of lymphocytotoxic antibodies in SLE family members as well as close household contacts. If immunologic abnormalities can be demonstrated in SLE family members, specifically a suppressor T cell defect, this, in conjunction with the presence of anti-lymphocyte antibodies, would support the hypothesis that SLE manifests itself in those persons with a genetic predisposition given the appropriate environmental stimulus. It is the objective of this proposal to demonstrate such a defect. The research plan will select 50 family members of SLE patients and a control group of 50 non-family close contacts matched for age, race, and sex. All subjects will be screened for serologic abnormalities seen in SLE and have delayed hypersensitivity skin tests performed. Lymphocytotoxic antibodies will be tested for in all groups and identification of any T cell function aberration. In the final phase of the study, those subjects in whom T cell abnormalities have been identified will have an in-depth study of T suppressor-helper cell defects.

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
General Clinical Research Centers Program (M01)
Project #
5M01RR000068-26
Application #
3089575
Study Section
General Clinical Research Centers Committee (CLR)
Project Start
1975-10-01
Project End
1989-11-30
Budget Start
1987-12-01
Budget End
1988-11-30
Support Year
26
Fiscal Year
1988
Total Cost
Indirect Cost
Name
University of Cincinnati
Department
Type
Schools of Medicine
DUNS #
City
Cincinnati
State
OH
Country
United States
Zip Code
45221
Feghali, Maisa; Khoury, Jane C; Shveiky, David et al. (2012) Association of vaginal delivery efforts with retinal disease in women with type I diabetes. J Matern Fetal Neonatal Med 25:27-31
Luggen, M; Belhorn, L; Evans, T et al. (1995) The evolution of Raynaud's phenomenon: a longterm prospective study. J Rheumatol 22:2226-32
Mimouni, F; Mughal, Z; Tsang, R C et al. (1995) Effect of maternal oxygen therapy on placental calcium transport in intrauterine growth retarded rats. J Am Coll Nutr 14:165-8
Samaratunga, R C; Thomas, S R; Hinnefeld, J D et al. (1995) A Monte Carlo simulation model for radiation dose to metastatic skeletal tumor from rhenium-186(Sn)-HEDP. J Nucl Med 36:336-50
Nordlund, J J; Csato, M; Babcock, G et al. (1995) Low ICAM-1 expression in the epidermis of depigmenting C57BL/6J-mivit/mivit mice: a possible cause of muted contact sensitization. Exp Dermatol 4:20-9
Green, D W; Mimouni, F; Khoury, J (1995) Decreased platelet counts in infants of diabetic mothers. Am J Perinatol 12:102-5
Cruz, M L; Wong, W W; Mimouni, F et al. (1994) Effects of infant nutrition on cholesterol synthesis rates. Pediatr Res 35:135-40
Cruz, M L; Bhadra, S; Subbiah, M T et al. (1994) Serum lipid peroxidation potential in infants. Arch Pediatr Adolesc Med 148:1212-5
Wones, R G; Deck, C C; Stadler, B et al. (1993) Lack of effect of drinking water chlorine on lipid and thyroid metabolism in healthy humans. Environ Health Perspect 99:375-81
Mimouni, F; Campaigne, B; Neylan, M et al. (1993) Bone mineralization in the first year of life in infants fed human milk, cow-milk formula, or soy-based formula. J Pediatr 122:348-54

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