LÆKNABLAÐIÐ 1990; 76: 375 375 NÝR DOKTOR í LÆKNISFRÆÐI - HELGI JÓNSSON í september 1989 lauk Helgi Jónsson læknir doktorsprófi frá Lundarháskóla. Ritgerðin nefnist á frummáli: »ON SYSTEMIC LUPUS ERYTHEMATOSUS. Clinical studies with special reference to epidemiology, lung function and complement activation«. SLE patients from a defined population (mean population at risk 158,572) were monitored prospectively during 1981- 1986. By the end of 1986, 86 patients (72 females, 14 males, median age 48) had been included in the cohort, the point prevalence being 68 patients (42/100,000 population at risk). The annual incidence was 4,0 cases/ 100.000/adults /year. A high completeness of retrieval of patients was achieved by computerized diagnosis and ANA registers in addition to clinical case finding. Five year survival in the prospective group was 97 percent. The proportion of patients with cutaneous manifestations, antibodies to dsDNA and hypocomplementemia decreased with increasing age at diagnosis, while the proportion of patients with serositis, secondary Sjögren’s syndrome and antibodies to SSA increased. Outcome was considered favorable, as witnessed by low mortality, low frequency of organ damage, and high percentage of patients gainfully employed. Disease flares occurred at a constant frequency after the first year. Patients with neuropsychiatric disease, drug hypersensitivity, persistent hypocomplementemia, antibodies to dsDNA and cardiolipin had a high frequency of relapse. Myocardial infarctions were nine times more common than in a Swedish control population and were related to long disease duration and glucocorticoid treatment. Extensive lung function tests in twelve consecutive symptomatic patients revealed no functionally significant lung damage in the majority of the patients. Reduced working capacity was related to non-respiratory factors. Spirometry screening in the epidemiological cohort revealed only a moderate reduction of vital capacity in patients with a past history of serositis. In prospective studies of C1 dissociation, the concentration of C1 IA complexes of the tetramer C1 IA-Clr-Cls-Cl IA variety correlated with the concentrations of C2 and C3 fragments, suggesting effective activation of the classical pathway. This was a characteristic finding in active SLE nephritis. Trimer C1 IA-Clr-Cls complexes were found in low amounts in nephritis, but in high concentrations in extrarenal SLE, and probably reflected C1 activation controlled at the Clr level.

Qupperneq 1
Qupperneq 2
Qupperneq 3
Qupperneq 4
Qupperneq 5
Qupperneq 6
Qupperneq 7
Qupperneq 8
Qupperneq 9
Qupperneq 10
Qupperneq 11
Qupperneq 12
Qupperneq 13
Qupperneq 14
Qupperneq 15
Qupperneq 16
Qupperneq 17
Qupperneq 18
Qupperneq 19
Qupperneq 20
Qupperneq 21
Qupperneq 22
Qupperneq 23
Qupperneq 24
Qupperneq 25
Qupperneq 26
Qupperneq 27
Qupperneq 28
Qupperneq 29
Qupperneq 30
Qupperneq 31
Qupperneq 32
Qupperneq 33
Qupperneq 34
Qupperneq 35
Qupperneq 36
Qupperneq 37
Qupperneq 38
Qupperneq 39
Qupperneq 40
Qupperneq 41
Qupperneq 42
Qupperneq 43
Qupperneq 44
Qupperneq 45
Qupperneq 46
Qupperneq 47
Qupperneq 48
Qupperneq 49
Qupperneq 50
Qupperneq 51
Qupperneq 52
Qupperneq 53
Qupperneq 54
Qupperneq 55
Qupperneq 56
Qupperneq 57
Qupperneq 58
Qupperneq 59
Qupperneq 60