J. Theophilus scite author profile

SUMMARYThe distribution of phenotypes controlled by two loci on chromosome 6 has been studied in a series of 239 patients with type 1 (insulin-dependent) and 297 patients with type 2 (non-insulin-dependent) diabetes mellitus. At the properdin factor B (Bf) locus there is a significant increase in the frequency of the Bf s1 and Bf n alleles for type 1 patients, and the combined increase in frequency of Bf s^ and Bf F1 in those patients is highly significant. The relative risk for F1 is 6.2 and for F1 and S1 combined is 5.3. These results confirm the association with F1 reported recently by Raum and co-workers in Boston. The two rare alleles Bf s1 and Bf F1 are in significant negative disequilibrium with HLA B8.For the glyoxalase (GLO) locus there is a slight but nonsignificant increase in the frequency bf the GLO 2 allele, but a significant disturbance in the distribution of the GLO phenotypes for type 2 patients. These results for the GLO alleles may be due to stratification in our series of type 2 patients. Further studies are in progress to test this hypothesis. DIABETES 28:949-951, October 1979. . R enewed attention has been given recently to the role of genetic factors in susceptibility to diabetes mellitus, 1 " 4 and this has received added impetus from the studies of the distribution of human leucocyte antigens (HLA) in diabetic patients. Several surveys 5 " 9 have shown, a significant increase in some antigens, particularly HLA B8 and BW15 for Caucasian patients with type 1 (juvenile or insulin-dependent) diabetes mellitus,

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The rare factor BfSl of the properdin system strongly associated with insulin‐dependent diabetes in north India

Kirk¹,

Ranford²,

Theophilus³

et al. 1982

Tissue Antigens

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Lymphocytotoxic Antibodies and Histocompatibility Antigens in Juvenile-onset Diabetes Mellitus

Serjeantson¹,

Theophilus²,

Zimmet³

et al. 1981

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Cold-reacting serum lymphocytotoxic antibodies (LCAs) were measured in sera from 230 insulin-dependent juvenile-onset diabetes mellitus (IDDM) patients and from 116 control subjects. LCAs were present in only 4% of control sera compared with 19% in IDDM patients. The most significant determinant of LCAs was time since onset of diabetes; within the first 12 mo, 55% of IDDM sera had LCAs, compared with 25% after one year and 15% after five years of diabetes. LCAs were absent in sera from patients with IDDM for 10 yr or more. Genetic factors were also implicated in susceptibility toi occurrence of LCAs. HLA antigen B8 and B18 were associated with an increased risk for LCAs, whereas HLA-B7 was associated with a decreased risk. The relative risk for LCAs in patients positive for HLA-B8 but not B7 was 2.3, compared with 0.0 in HLA-B7/B8 heterozygotes. In contrast, B7 did not provide protection from LCAs in B18/B7 IDDM patients. Properdin factor B (Bf) alleles, which are in linkage disequilibrium with alleles of the HLA-B locus, were also associated with LCAs, IDDM patients with alleles BfS1 or BfF hd a prevalence of LCAs of 7%, significantly less than the 39% in Bf-F1S or -F1 patients. LCAs were not identical or closely correlated to pancreatic islet cell antibodies. Our findings indicate genetic heterogeneity in, yet, another autoimmune process in IDDM.

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The distribution of properdin factor B (Bf) and glyoxalase (GLO) phenotypes in diabetes

Theophilus¹,

Kirk²,

Whitehouse³

et al. 1980

Pathology

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J. Theophilus

Age Relationship Between Insulin-Dependent Diabetes and Rare Alleles of Properdin Factor B

Genetic Susceptibility to Diabetes Mellitus: the Distribution of Properdin Factor B (Bf) and Glyoxalase (GLO) Phenotypes

The rare factor BfSl of the properdin system strongly associated with insulin‐dependent diabetes in north India

Lymphocytotoxic Antibodies and Histocompatibility Antigens in Juvenile-onset Diabetes Mellitus

The distribution of properdin factor B (Bf) and glyoxalase (GLO) phenotypes in diabetes

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