Your search keyword '"Ivarsson, S"' showing total 49 results

1. Reduced display of conformational epitopes in the N-terminal truncated GAD65 isoform : relevance for people with stiff person syndrome or DQ8/8-positive Type 1 diabetes mellitus

Author

Hampe, C. S., Radtke, J. R., Wester, A., Carlsson, A., Cedervall, E., Jönsson, B., Ivarsson, S. A., Elding Larsson, H., Larsson, K., Lindberg, B., Neiderud, J., Rolandsson, Olov, Lernmark, Å., Hampe, C. S., Radtke, J. R., Wester, A., Carlsson, A., Cedervall, E., Jönsson, B., Ivarsson, S. A., Elding Larsson, H., Larsson, K., Lindberg, B., Neiderud, J., Rolandsson, Olov, and Lernmark, Å.

Abstract

Aims: To investigate whether the N‐terminal truncated glutamic acid decarboxylase 65 (GAD65) isoform is as well recognized by people with stiff person syndrome as it is by people with Type 1 diabetes, and whether conformational GAD65 antibody epitopes are displayed properly by the isoform. Methods: GAD65 antibody‐positive healthy individuals (n=13), people with stiff‐person syndrome (n=15) and children with new‐onset Type 1 diabetes (n=654) were analysed to determine binding to full‐length GAD65 and the N‐terminal truncated GAD65 isoform in each of these settings. GAD65 autoantibody epitope specificity was correlated with binding ratios of full‐length GAD65/N‐terminal truncated GAD65. Results: The N‐terminal truncated GAD65 isoform was significantly less recognized in GAD65Ab‐positive people with stiff‐person syndrome (P=0.002) and in healthy individuals (P=0.0001) than in people with Type 1 diabetes. Moreover, at least two specific conformational GAD65Ab epitopes were not, or were only partially, presented by the N‐terminal truncated GAD65 isoform compared to full‐length GAD65. Finally, an N‐terminal conformational GAD65Ab epitope was significantly less recognized in DQ8/8 positive individuals with Type 1 diabetes (P=0.02). Conclusions: In people with stiff person syndrome preferred binding to the full‐length GAD65 isoform over the N‐terminal truncated molecule was observed. This binding characteristic is probably attributable to reduced presentation of two conformational epitopes by the N‐terminal truncated molecule. These findings support the notion of disease‐specific GAD65Ab epitope specificities and emphasize the need to evaluate the applicability of novel assays for different medical conditions.

Published

2019

2. The Better Diabetes Diagnosis (BDD) study - A review of a nationwide prospective cohort study in Sweden

Author

Persson, M., Becker, C., Larsson, H. Elding, Lernmark, A., Forsander, G., Ivarsson, S. A., Ludvigsson, Johnny, Samuelsson, Ulf, Marcus, C., Carlsson, A., Persson, M., Becker, C., Larsson, H. Elding, Lernmark, A., Forsander, G., Ivarsson, S. A., Ludvigsson, Johnny, Samuelsson, Ulf, Marcus, C., and Carlsson, A.

Abstract

The incidence of type 1 diabetes (T1D) in Sweden is one of the highest in the world. However, the possibility of other types of diabetes must also be considered. In addition, individuals with T1D constitute a heterogeneous group. A precise classification of diabetes is a prerequisite for optimal outcome. For precise classification, knowledge on the distribution of genetic factors, biochemical markers and clinical features in individuals with new onset of diabetes is needed. The Better Diabetes Diagnosis (BDD), is a nationwide study in Sweden with the primary aim to facilitate a more precise classification and diagnosis of diabetes in order to enable the most adequate treatment for each patient. Secondary aims include identification of risk factors for diabetes-related co-morbidities. Since 2005, data on almost all children and adolescents with newly diagnosed diabetes in Sweden are prospectively collected and including heredity of diabetes, clinical symptoms, levels of C peptide, genetic analyses and detection of autoantibodies. Since 2011, analyses of HLA profile, autoantibodies and C peptide levels are part of clinical routine in Sweden for all pediatric patients with suspected diagnosis of diabetes. In this review, we present the methods and main results of the BDD study so far and discuss future aspects. (C) 2018 Elsevier B.V. All rights reserved.

Published

2018

3. Origin of mutation in sporadic cases of severe haemophilia A in Sweden

Author

Mårtensson, A., Ivarsson, S., Letelier, A., Manderstedt, Eric, Halldén, Christer, Ljung, R., Mårtensson, A., Ivarsson, S., Letelier, A., Manderstedt, Eric, Halldén, Christer, and Ljung, R.

Abstract

Many newly diagnosed Swedish severe haemophilia A (HA) patients are sporadic cases. Some genotypically non-carrier mothers have gone on to have two descendants with the same mutation, presumably because of mosaicism. AIMS: To define the origin of mutation in sporadic cases of HA, reveal possible sex-specific differences in mutagenesis and identify potential mosaics among non-carrier mothers. METHOD: Sanger sequencing characterized the mutations and microsatellite haplotyping determined the origin of the X chromosome carrying the mutation in 3 generations of 45 families with sporadic severe HA. Droplet digital polymerase chain reaction (ddPCR) was used in five cases to reveal that mosaicism mutations are not found on conventional DNA sequencing. RESULTS: In 23 out of 45 families, the mother carried the mutation and in 5 out of 28 families, the grandmother was also a carrier. The X chromosome was of grandpaternal origin in 17 out of 23 cases. One of five tested mothers was a mosaic with a mutation frequency of 7%. CONCLUSION: In 40 out of 45 families, the sporadic case resulted from a mutation in the last two generations. In 82% (23/28), the carrier mothers had a de novo mutation where the X chromosome was of paternal origin in 74% (17/23). ddPCR is a potentially powerful and promising analysis for mosaicism in HA.

Published

2016

4. Serological Evaluation of Possible Exposure to Ljungan Virus and Related Parechovirus in Autoimmune (Type 1) Diabetes in Children

Author

Nilsson, A-L, Vaziri-Sani, F., Broberg, P., Elfaitouri, A., Pipkorn, R., Blomberg, Jonas, Ivarsson, S-A, Larsson, H. Elding, Lernmark, A., Nilsson, A-L, Vaziri-Sani, F., Broberg, P., Elfaitouri, A., Pipkorn, R., Blomberg, Jonas, Ivarsson, S-A, Larsson, H. Elding, and Lernmark, A.

Abstract

Exposure to Ljungan virus (LV) is implicated in the risk of autoimmune (type 1) diabetes but possible contribution by other parechoviruses is not ruled out. The aim was to compare children diagnosed with type 1 diabetes in 2005-2011 (n=69) with healthy controls (n=294), all from the Jamtland County in Sweden, using an exploratory suspension multiplex immunoassay for IgM and IgG against 26 peptides of LV, human parechoviruses (HPeV), Aichi virus and poliovirus in relation to a radiobinding assay (RBA) for antibodies against LV and InfluenzaA/H1N1pdm09. Islet autoantibodies and HLA-DQ genotypes were also determined. 1) All five LV-peptide antibodies correlated to each other (P<0.001) in the suspension multiplex IgM- and IgG-antibody assay; 2) The LV-VP1_31-60-IgG correlated with insulin autoantibodies alone (P=0.007) and in combination with HLA-DQ8 overall (P=0.022) as well as with HLA-DQ 8/8 and 8/X subjects (P=0.013); 3) RBA detected LV antibodies correlated with young age at diagnosis (P<0.001) and with insulin autoantibodies (P<0.001) especially in young HLA-DQ8 subjects (P=0.004); 4) LV-peptide-VP1_31-60-IgG correlated to RBA LV antibodies (P=0.009); 5) HPeV3-peptide-IgM and -IgG showed inter-peptide correlations (P<0.001) but only HPeV3-VP1_1-30-IgG (P<0.001) and VP1_95-124-IgG (P=0.009) were related to RBA LV antibodies without relation to insulin autoantibody positivity (P=0.072 and P=0.486, respectively). Both exploratory suspension multiplex IgG to LV-peptide VP1_31-60 and RBA detected LV antibodies correlated with insulin autoantibodies and HLA-DQ8 suggesting possible role in type 1 diabetes. It remains to be determined if cross-reactivity or concomitant exposure to LV and HPeV3 contributes to the seroprevalence. J. Med. Virol. 87:1130-1140, 2015.

Published

2015

5. Serological evaluation of possible exposure to Ljungan virus and related parechovirus in autoimmune (type 1) diabetes in children

Author

Nilsson, A-L, Vaziri-Sani, Fariba, Broberg, P, Elfaitouri, A, Pipkorn, R, Blomberg, J, Ivarsson, S-A, Elding Larsson, H, Lernmark, Å, Nilsson, A-L, Vaziri-Sani, Fariba, Broberg, P, Elfaitouri, A, Pipkorn, R, Blomberg, J, Ivarsson, S-A, Elding Larsson, H, and Lernmark, Å

Abstract

Exposure to Ljungan virus (LV) is implicated in the risk of autoimmune (type 1) diabetes but possible contribution by other parechoviruses is not ruled out. The aim was to compare children diagnosed with type 1 diabetes in 2005-2011 (n = 69) with healthy controls (n = 294), all from the Jämtland County in Sweden, using an exploratory suspension multiplex immunoassay for IgM and IgG against 26 peptides of LV, human parechoviruses (HPeV), Aichi virus and poliovirus in relation to a radiobinding assay (RBA) for antibodies against LV and InfluenzaA/H1N1pdm09. Islet autoantibodies and HLA-DQ genotypes were also determined. 1) All five LV-peptide antibodies correlated to each other (P < 0.001) in the suspension multiplex IgM- and IgG-antibody assay; 2) The LV-VP1_31-60-IgG correlated with insulin autoantibodies alone (P = 0.007) and in combination with HLA-DQ8 overall (P = 0.022) as well as with HLA-DQ 8/8 and 8/X subjects (P = 0.013); 3) RBA detected LV antibodies correlated with young age at diagnosis (P < 0.001) and with insulin autoantibodies (P < 0.001) especially in young HLA-DQ8 subjects (P = 0.004); 4) LV-peptide-VP1_31-60-IgG correlated to RBA LV antibodies (P = 0.009); 5) HPeV3-peptide-IgM and -IgG showed inter-peptide correlations (P < 0.001) but only HPeV3-VP1_1-30-IgG (P < 0.001) and VP1_95-124-IgG (P = 0.009) were related to RBA LV antibodies without relation to insulin autoantibody positivity (P = 0.072 and P = 0.486, respectively). Both exploratory suspension multiplex IgG to LV-peptide VP1_31-60 and RBA detected LV antibodies correlated with insulin autoantibodies and HLA-DQ8 suggesting possible role in type 1 diabetes. It remains to be determined if cross-reactivity or concomitant exposure to LV and HPeV3 contributes to the seroprevalence.

Published

2015

6. Doubly reactive INS-IGF2 autoantibodies in children with newly diagnosed autoimmune (type 1) diabetes

Author

Kanatsuna, N, Delli, A, Andersson, C, Nilsson, A-L, Vaziri-Sani, Fariba, Larsson, K, Carlsson, A, Cedervall, E, Jönsson, B, Neiderud, J, Elding Larsson, H, Ivarsson, S-A, Törn, C, Fex, M, Lernmark, Å, Kanatsuna, N, Delli, A, Andersson, C, Nilsson, A-L, Vaziri-Sani, Fariba, Larsson, K, Carlsson, A, Cedervall, E, Jönsson, B, Neiderud, J, Elding Larsson, H, Ivarsson, S-A, Törn, C, Fex, M, and Lernmark, Å

Abstract

The splice variant INS-IGF2 entails the preproinsulin signal peptide, the insulin B-chain, eight amino acids of the C-peptide and 138 unique amino acids from an ORF in the IGF2 gene. The aim of this study was to determine whether levels of specific INS-IGF2 autoantibodies (INS-IGF2A) were related to age at diagnosis, islet autoantibodies, HLA-DQ or both, in patients and controls with newly diagnosed type 1 diabetes. Patients (n = 676), 0-18 years of age, diagnosed with type 1 diabetes in 1996-2005 and controls (n = 363) were analysed for specific INS-IGF2A after displacement with both cold insulin and INS-IGF2 to correct for non-specific binding and identify double reactive sera. GADA, IA-2A, IAA, ICA, ZnT8RA, ZnT8WA, ZnT8QA and HLA-DQ genotypes were also determined. The median level of specific INS-IGF2A was higher in patients than in controls (P < 0.001). Irrespective of age at diagnosis, 19% (126/676) of the patients had INS-IGF2A when the cut-off was the 95th percentile of the controls (P < 0.001). The risk of INS-IGF2A was increased among HLA-DQ2/8 (OR = 1.509; 95th CI 1.011, 2.252; P = 0.045) but not in 2/2, 2/X, 8/8, 8/X or X/X (X is neither 2 nor 8) patients. The association with HLA-DQ2/8 suggests that this autoantigen may be presented on HLA-DQ trans-heterodimers, rather than cis-heterodimers. Autoantibodies reactive with both insulin and INS-IGF2A at diagnosis support the notion that INS-IGF2 autoimmunity contributes to type 1 diabetes.

Published

2015

7. Thyroid autoimmunity in relation to islet autoantibodies and HLA-DQ genotype in newly diagnosed type 1 diabetes in children and adolescents

Author

Jonsdottir, B, Andersson, C, Carlsson, A, Delli, A, Forsander, G, Ludvigsson, J, Marcus, C, Samuelsson, U, Ortqvist, E, Lernmark, A, Ivarsson, S-A, Larsson, H Elding, Jonsdottir, B, Andersson, C, Carlsson, A, Delli, A, Forsander, G, Ludvigsson, J, Marcus, C, Samuelsson, U, Ortqvist, E, Lernmark, A, Ivarsson, S-A, and Larsson, H Elding

Abstract

AIMS/HYPOTHESIS: The aim of this work was to investigate, in children newly diagnosed with type 1 diabetes: (1) the prevalence of autoantibodies against thyroid peroxidase (TPOAb) and thyroglobulin (TGAb); and (2) the association between TPOAb, TGAb or both, with either islet autoantibodies or HLA-DQ genes. METHODS: Blood samples from 2,433 children newly diagnosed with type 1 diabetes were analysed for TPOAb and TGAb in addition to autoantibodies against arginine zinc transporter 8 (ZnT8RA), tryptophan zinc transporter 8 (ZnT8WA), glutamine zinc transporter 8 (ZnT8QA), glutamic acid decarboxylase (GADA), insulin (IAA), insulinoma-associated protein-2 (IA-2A), HLA-DQA-B1 genotypes, thyroid-stimulating hormone (TSH) and free thyroxine (T4). RESULTS: At type 1 diabetes diagnosis, 12% of the children had thyroid autoantibodies (60% were girls; p < 0.0001). GADA was positively associated with TPOAb (p < 0.001) and with TGAb (p < 0.001). In addition, ZnT8A was associated with both TPOAb (p = 0.039) and TGAb (p = 0.015). DQB1*05:01 in any genotype was negatively associated with TPOAb (OR 0.55, 95% CI 0.37, 0.83, p value corrected for multiple comparisons (p c) = 0.012) and possibly with TGAb (OR 0.55, 95% CI 0.35, 0.87, p c = 0.07). Thyroid autoimmunity in children newly diagnosed with type 1 diabetes was rarely (0.45%) associated with onset of clinical thyroid disease based on TSH and free T4. CONCLUSIONS/INTERPRETATION: GADA and ZnT8A increased the risk for thyroid autoimmunity at the time of clinical diagnosis of type 1 diabetes, while HLA-DQB1*05:01 reduced the risk. However, the associations between thyroid autoimmunity and HLA-DQ genotype were weak and did not fully explain the co-occurrence of islet and thyroid autoimmunity.

Published

2013

8. Triple specificity of ZnT8 autoantibodies in relation to HLA and other islet autoantibodies in childhood and adolescent type 1 diabetes

Author

Andersson, C, Vaziri-Sani, F, Delli, A J., Lindblad, B, Carlsson, A, Forsander, G, Ludvigsson, Johnny, Marcus, C, Samuelsson, Ulf, Ivarsson, S A., Lernmark, A, Elding Larsson, H, Andersson, C, Vaziri-Sani, F, Delli, A J., Lindblad, B, Carlsson, A, Forsander, G, Ludvigsson, Johnny, Marcus, C, Samuelsson, Ulf, Ivarsson, S A., Lernmark, A, and Elding Larsson, H

Abstract

Andersson C, Vaziri-Sani F, Delli AJ, Lindblad B, Carlsson A, Forsander G, Ludvigsson J, Marcus C, Samuelsson U, Ivarsson SA, Lernmark A, Elding Larsson H, the BDD Study group. Triple specificity of ZnT8 autoantibodies in relation to HLA and other islet autoantibodies in childhood and adolescent type 1 diabetes. Pediatric Diabetes 2013: 14: 97-105. Objective To establish the diagnostic sensitivity of and the relationships between autoantibodies to all three Zinc transporter 8 (Zinc transporter 8 autoantibody to either one, two, or all three amino acid variants at position 325, ZnT8A) variants to human leukocyte antigen (HLA)-DQ and to autoantibodies to glutamic acid decarboxylase (GADA), insulinoma-associated protein 2 (IA-2A), and insulin (IAA). Methods We analyzed 3165 patients with type 1 diabetes (T1D) in the Better Diabetes Diagnosis study for HLA-DQ genotypes and all six autoantibodies (ZnT8RA, arginine 325 Zinc transporter 8 autoantibody; ZnT8WA, tryptophan 325 Zinc transporter 8 autoantibody; ZnT8QA, glutamine 325 Zinc transporter 8 autoantibody; GADA, IA-2A, and IAA). Results ZnT8A was found in 65% of the patients and as many as 108 of 3165 (3.4%) had 13 ZnT8A alone. None had ZnT8QA alone. Together with GADA (56%), IA-2A (73%), and IAA (33%), 93% of the T1D patients were autoantibody positive. All three ZnT8A were less frequent in children below 2 yr of age (pandlt;0.0001). All three ZnT8A were associated with DQA1-B1*X-0604 (DQ6.4) and DQA1-B1*03-0302 (DQ8). ZnT8WA and ZnT8QA were negatively associated with DQA1-B1*05-02 (DQ2). Conclusions Analysis of ZnT8A increased the diagnostic sensitivity of islet autoantibodies for T1D as only 7% remained islet autoantibody negative. The association between DQ6.4 and all three ZnT8A may be related to ZnT8 antigen presentation by the DQ6.4 heterodimer., Funding Agencies|Swedish Research Council|14064|Swedish Child Diabetes Foundation||Swedish Diabetes Association||National Institutes of Health|DK26190|UMAS Fund||Knut and Alice Wallenberg Foundation||Skane County Council for Research and Development

Published

2013

9. Residual beta cell function at diagnosis of type 1 diabetes in children and adolescents varies with gender and season

Author

Samuelsson, Ulf, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S, Kockum, I, Lernmark, A, Marcus, C, Ludvigsson, Johnny, Samuelsson, Ulf, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S, Kockum, I, Lernmark, A, Marcus, C, and Ludvigsson, Johnny

Abstract

Background There are seasonal variations and gender differences in incidence of type 1 diabetes (T1D), metabolic control and responses to immune interventions at onset of the disease. We hypothesized that there are seasonal and gender differences in residual insulin secretion already at diagnosis of T1D. Methods In 2005, a national study, the Better Diabetes Diagnosis, was started to classify all newly diagnosed children and adolescents with diabetes. About 95% (3824/4017) of the patients were classified as T1D, and our analyses are based on the patients with T1D. Results C-peptide was lower in younger children, 0–10 years of age (0.23 ± 0.20 nmol/L) than in older children, 11–18 years of age (0.34 ± 0.28 nmol/L) (p < 0.000 ). There was a seasonal variation in non-fasting serum C-peptide, significantly correlated to the seasonal variation of diagnosis (p < 0.01). Most children were diagnosed in January, February and March as well as in October when C-peptide was highest, whereas fewer patients were diagnosed in April and May when serum C-peptide was significantly lower (p < 0.01). The seasonal variation of C-peptide was more pronounced in boys than in girls (p < 0.000 and p < 0.01, respectively). Girls had higher C-peptide than boys (p < 0.05), especially in early puberty. Conclusions Both seasonal and gender differences in residual beta cell function exist already at diagnosis of T1D. These observations have consequences for treatment and for randomizing patients in immune intervention clinical trials., Funding Agencies|Swedish Child Diabetes Foundation (Barndiabetesfonden)

Published

2013

10. Residual beta cell function at diagnosis of type 1 diabetes in children and adolescents varies with gender and season

Author

Samuelsson, Ulf, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S, Kockum, I, Lernmark, A, Marcus, C, Ludvigsson, Johnny, Samuelsson, Ulf, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S, Kockum, I, Lernmark, A, Marcus, C, and Ludvigsson, Johnny

Abstract

Background There are seasonal variations and gender differences in incidence of type 1 diabetes (T1D), metabolic control and responses to immune interventions at onset of the disease. We hypothesized that there are seasonal and gender differences in residual insulin secretion already at diagnosis of T1D. Methods In 2005, a national study, the Better Diabetes Diagnosis, was started to classify all newly diagnosed children and adolescents with diabetes. About 95% (3824/4017) of the patients were classified as T1D, and our analyses are based on the patients with T1D. Results C-peptide was lower in younger children, 0–10 years of age (0.23 ± 0.20 nmol/L) than in older children, 11–18 years of age (0.34 ± 0.28 nmol/L) (p < 0.000 ). There was a seasonal variation in non-fasting serum C-peptide, significantly correlated to the seasonal variation of diagnosis (p < 0.01). Most children were diagnosed in January, February and March as well as in October when C-peptide was highest, whereas fewer patients were diagnosed in April and May when serum C-peptide was significantly lower (p < 0.01). The seasonal variation of C-peptide was more pronounced in boys than in girls (p < 0.000 and p < 0.01, respectively). Girls had higher C-peptide than boys (p < 0.05), especially in early puberty. Conclusions Both seasonal and gender differences in residual beta cell function exist already at diagnosis of T1D. These observations have consequences for treatment and for randomizing patients in immune intervention clinical trials., Funding Agencies|Swedish Child Diabetes Foundation (Barndiabetesfonden)

Published

2013

11. Residual beta cell function at diagnosis of type 1 diabetes in children and adolescents varies with gender and season

Author

Samuelsson, Ulf, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S, Kockum, I, Lernmark, A, Marcus, C, Ludvigsson, Johnny, Samuelsson, Ulf, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S, Kockum, I, Lernmark, A, Marcus, C, and Ludvigsson, Johnny

Abstract

Background There are seasonal variations and gender differences in incidence of type 1 diabetes (T1D), metabolic control and responses to immune interventions at onset of the disease. We hypothesized that there are seasonal and gender differences in residual insulin secretion already at diagnosis of T1D. Methods In 2005, a national study, the Better Diabetes Diagnosis, was started to classify all newly diagnosed children and adolescents with diabetes. About 95% (3824/4017) of the patients were classified as T1D, and our analyses are based on the patients with T1D. Results C-peptide was lower in younger children, 0–10 years of age (0.23 ± 0.20 nmol/L) than in older children, 11–18 years of age (0.34 ± 0.28 nmol/L) (p < 0.000 ). There was a seasonal variation in non-fasting serum C-peptide, significantly correlated to the seasonal variation of diagnosis (p < 0.01). Most children were diagnosed in January, February and March as well as in October when C-peptide was highest, whereas fewer patients were diagnosed in April and May when serum C-peptide was significantly lower (p < 0.01). The seasonal variation of C-peptide was more pronounced in boys than in girls (p < 0.000 and p < 0.01, respectively). Girls had higher C-peptide than boys (p < 0.05), especially in early puberty. Conclusions Both seasonal and gender differences in residual beta cell function exist already at diagnosis of T1D. These observations have consequences for treatment and for randomizing patients in immune intervention clinical trials., Funding Agencies|Swedish Child Diabetes Foundation (Barndiabetesfonden)

Published

2013

12. Triple specificity of ZnT8 autoantibodies in relation to HLA and other islet autoantibodies in childhood and adolescent type 1 diabetes

Author

Andersson, C, Vaziri-Sani, F, Delli, A J., Lindblad, B, Carlsson, A, Forsander, G, Ludvigsson, Johnny, Marcus, C, Samuelsson, Ulf, Ivarsson, S A., Lernmark, A, Elding Larsson, H, Andersson, C, Vaziri-Sani, F, Delli, A J., Lindblad, B, Carlsson, A, Forsander, G, Ludvigsson, Johnny, Marcus, C, Samuelsson, Ulf, Ivarsson, S A., Lernmark, A, and Elding Larsson, H

Abstract

Andersson C, Vaziri-Sani F, Delli AJ, Lindblad B, Carlsson A, Forsander G, Ludvigsson J, Marcus C, Samuelsson U, Ivarsson SA, Lernmark A, Elding Larsson H, the BDD Study group. Triple specificity of ZnT8 autoantibodies in relation to HLA and other islet autoantibodies in childhood and adolescent type 1 diabetes. Pediatric Diabetes 2013: 14: 97-105. Objective To establish the diagnostic sensitivity of and the relationships between autoantibodies to all three Zinc transporter 8 (Zinc transporter 8 autoantibody to either one, two, or all three amino acid variants at position 325, ZnT8A) variants to human leukocyte antigen (HLA)-DQ and to autoantibodies to glutamic acid decarboxylase (GADA), insulinoma-associated protein 2 (IA-2A), and insulin (IAA). Methods We analyzed 3165 patients with type 1 diabetes (T1D) in the Better Diabetes Diagnosis study for HLA-DQ genotypes and all six autoantibodies (ZnT8RA, arginine 325 Zinc transporter 8 autoantibody; ZnT8WA, tryptophan 325 Zinc transporter 8 autoantibody; ZnT8QA, glutamine 325 Zinc transporter 8 autoantibody; GADA, IA-2A, and IAA). Results ZnT8A was found in 65% of the patients and as many as 108 of 3165 (3.4%) had 13 ZnT8A alone. None had ZnT8QA alone. Together with GADA (56%), IA-2A (73%), and IAA (33%), 93% of the T1D patients were autoantibody positive. All three ZnT8A were less frequent in children below 2 yr of age (pandlt;0.0001). All three ZnT8A were associated with DQA1-B1*X-0604 (DQ6.4) and DQA1-B1*03-0302 (DQ8). ZnT8WA and ZnT8QA were negatively associated with DQA1-B1*05-02 (DQ2). Conclusions Analysis of ZnT8A increased the diagnostic sensitivity of islet autoantibodies for T1D as only 7% remained islet autoantibody negative. The association between DQ6.4 and all three ZnT8A may be related to ZnT8 antigen presentation by the DQ6.4 heterodimer., Funding Agencies|Swedish Research Council|14064|Swedish Child Diabetes Foundation||Swedish Diabetes Association||National Institutes of Health|DK26190|UMAS Fund||Knut and Alice Wallenberg Foundation||Skane County Council for Research and Development

Published

2013

13. Residual beta cell function at diagnosis of type 1 diabetes in children and adolescents varies with gender and season

Author

Samuelsson, Ulf, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S, Kockum, I, Lernmark, A, Marcus, C, Ludvigsson, Johnny, Samuelsson, Ulf, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S, Kockum, I, Lernmark, A, Marcus, C, and Ludvigsson, Johnny

Abstract

Background There are seasonal variations and gender differences in incidence of type 1 diabetes (T1D), metabolic control and responses to immune interventions at onset of the disease. We hypothesized that there are seasonal and gender differences in residual insulin secretion already at diagnosis of T1D. Methods In 2005, a national study, the Better Diabetes Diagnosis, was started to classify all newly diagnosed children and adolescents with diabetes. About 95% (3824/4017) of the patients were classified as T1D, and our analyses are based on the patients with T1D. Results C-peptide was lower in younger children, 0–10 years of age (0.23 ± 0.20 nmol/L) than in older children, 11–18 years of age (0.34 ± 0.28 nmol/L) (p < 0.000 ). There was a seasonal variation in non-fasting serum C-peptide, significantly correlated to the seasonal variation of diagnosis (p < 0.01). Most children were diagnosed in January, February and March as well as in October when C-peptide was highest, whereas fewer patients were diagnosed in April and May when serum C-peptide was significantly lower (p < 0.01). The seasonal variation of C-peptide was more pronounced in boys than in girls (p < 0.000 and p < 0.01, respectively). Girls had higher C-peptide than boys (p < 0.05), especially in early puberty. Conclusions Both seasonal and gender differences in residual beta cell function exist already at diagnosis of T1D. These observations have consequences for treatment and for randomizing patients in immune intervention clinical trials., Funding Agencies|Swedish Child Diabetes Foundation (Barndiabetesfonden)

Published

2013

14. Thyroid autoimmunity in relation to islet autoantibodies and HLA-DQ genotype in newly diagnosed type 1 diabetes in children and adolescents

Author

Jonsdottir, B, Andersson, C, Carlsson, A, Delli, A, Forsander, G, Ludvigsson, Johnny, Marcus, C, Samuelsson, Ulf, Ortqvist, E, Lernmark, A, Ivarsson, S-A, Elding Larsson, H, Jonsdottir, B, Andersson, C, Carlsson, A, Delli, A, Forsander, G, Ludvigsson, Johnny, Marcus, C, Samuelsson, Ulf, Ortqvist, E, Lernmark, A, Ivarsson, S-A, and Elding Larsson, H

Abstract

The aim of this work was to investigate, in children newly diagnosed with type 1 diabetes: (1) the prevalence of autoantibodies against thyroid peroxidase (TPOAb) and thyroglobulin (TGAb); and (2) the association between TPOAb, TGAb or both, with either islet autoantibodies or HLA-DQ genes. less thanbrgreater than less thanbrgreater thanBlood samples from 2,433 children newly diagnosed with type 1 diabetes were analysed for TPOAb and TGAb in addition to autoantibodies against arginine zinc transporter 8 (ZnT8RA), tryptophan zinc transporter 8 (ZnT8WA), glutamine zinc transporter 8 (ZnT8QA), glutamic acid decarboxylase (GADA), insulin (IAA), insulinoma-associated protein-2 (IA-2A), HLA-DQA-B1 genotypes, thyroid-stimulating hormone (TSH) and free thyroxine (T4). less thanbrgreater than less thanbrgreater thanAt type 1 diabetes diagnosis, 12% of the children had thyroid autoantibodies (60% were girls; p andlt; 0.0001). GADA was positively associated with TPOAb (p andlt; 0.001) and with TGAb (p andlt; 0.001). In addition, ZnT8A was associated with both TPOAb (p = 0.039) and TGAb (p = 0.015). DQB1*05:01 in any genotype was negatively associated with TPOAb (OR 0.55, 95% CI 0.37, 0.83, p value corrected for multiple comparisons (p (c)) = 0.012) and possibly with TGAb (OR 0.55, 95% CI 0.35, 0.87, p (c) = 0.07). Thyroid autoimmunity in children newly diagnosed with type 1 diabetes was rarely (0.45%) associated with onset of clinical thyroid disease based on TSH and free T4. less thanbrgreater than less thanbrgreater thanGADA and ZnT8A increased the risk for thyroid autoimmunity at the time of clinical diagnosis of type 1 diabetes, while HLA-DQB1*05:01 reduced the risk. However, the associations between thyroid autoimmunity and HLA-DQ genotype were weak and did not fully explain the co-occurrence of islet and thyroid autoimmunity., Funding Agencies|Swedish Research Council|14064|Swedish Child Diabetes Foundation||Swedish Diabetes Association||National Institutes of Health|DK26190|SUS Fund||Knut and Alice Wallenberg Foundation||Skane County Council for Research and Development

Published

2013

15. Residual beta cell function at diagnosis of type 1 diabetes in children and adolescents varies with gender and season

Author

Samuelsson, Ulf, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S, Kockum, I, Lernmark, A, Marcus, C, Ludvigsson, Johnny, Samuelsson, Ulf, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S, Kockum, I, Lernmark, A, Marcus, C, and Ludvigsson, Johnny

Abstract

Background There are seasonal variations and gender differences in incidence of type 1 diabetes (T1D), metabolic control and responses to immune interventions at onset of the disease. We hypothesized that there are seasonal and gender differences in residual insulin secretion already at diagnosis of T1D. Methods In 2005, a national study, the Better Diabetes Diagnosis, was started to classify all newly diagnosed children and adolescents with diabetes. About 95% (3824/4017) of the patients were classified as T1D, and our analyses are based on the patients with T1D. Results C-peptide was lower in younger children, 0–10 years of age (0.23 ± 0.20 nmol/L) than in older children, 11–18 years of age (0.34 ± 0.28 nmol/L) (p < 0.000 ). There was a seasonal variation in non-fasting serum C-peptide, significantly correlated to the seasonal variation of diagnosis (p < 0.01). Most children were diagnosed in January, February and March as well as in October when C-peptide was highest, whereas fewer patients were diagnosed in April and May when serum C-peptide was significantly lower (p < 0.01). The seasonal variation of C-peptide was more pronounced in boys than in girls (p < 0.000 and p < 0.01, respectively). Girls had higher C-peptide than boys (p < 0.05), especially in early puberty. Conclusions Both seasonal and gender differences in residual beta cell function exist already at diagnosis of T1D. These observations have consequences for treatment and for randomizing patients in immune intervention clinical trials., Funding Agencies|Swedish Child Diabetes Foundation (Barndiabetesfonden)

Published

2013

16. Thyroid autoimmunity in relation to islet autoantibodies and HLA-DQ genotype in newly diagnosed type 1 diabetes in children and adolescents.

Author

Jonsdottir, Berglind, Andersson, Cecilia K, Carlsson, Annelie, Delli, Ahmed, Forsander, G, Ludvigsson, J, Marcus, C, Samuelsson, Ulla, Ortqvist, E, Lernmark, Åke, Ivarsson, S-A, Larsson, H Elding, Jonsdottir, Berglind, Andersson, Cecilia K, Carlsson, Annelie, Delli, Ahmed, Forsander, G, Ludvigsson, J, Marcus, C, Samuelsson, Ulla, Ortqvist, E, Lernmark, Åke, Ivarsson, S-A, and Larsson, H Elding

Abstract

AIMS/HYPOTHESIS: The aim of this work was to investigate, in children newly diagnosed with type 1 diabetes: (1) the prevalence of autoantibodies against thyroid peroxidase (TPOAb) and thyroglobulin (TGAb); and (2) the association between TPOAb, TGAb or both, with either islet autoantibodies or HLA-DQ genes. METHODS: Blood samples from 2,433 children newly diagnosed with type 1 diabetes were analysed for TPOAb and TGAb in addition to autoantibodies against arginine zinc transporter 8 (ZnT8RA), tryptophan zinc transporter 8 (ZnT8WA), glutamine zinc transporter 8 (ZnT8QA), glutamic acid decarboxylase (GADA), insulin (IAA), insulinoma-associated protein-2 (IA-2A), HLA-DQA-B1 genotypes, thyroid-stimulating hormone (TSH) and free thyroxine (T4). RESULTS: At type 1 diabetes diagnosis, 12% of the children had thyroid autoantibodies (60% were girls; p < 0.0001). GADA was positively associated with TPOAb (p < 0.001) and with TGAb (p < 0.001). In addition, ZnT8A was associated with both TPOAb (p = 0.039) and TGAb (p = 0.015). DQB1*05:01 in any genotype was negatively associated with TPOAb (OR 0.55, 95% CI 0.37, 0.83, p value corrected for multiple comparisons (p c) = 0.012) and possibly with TGAb (OR 0.55, 95% CI 0.35, 0.87, p c = 0.07). Thyroid autoimmunity in children newly diagnosed with type 1 diabetes was rarely (0.45%) associated with onset of clinical thyroid disease based on TSH and free T4. CONCLUSIONS/INTERPRETATION: GADA and ZnT8A increased the risk for thyroid autoimmunity at the time of clinical diagnosis of type 1 diabetes, while HLA-DQB1*05:01 reduced the risk. However, the associations between thyroid autoimmunity and HLA-DQ genotype were weak and did not fully explain the co-occurrence of islet and thyroid autoimmunity.

Published

2013

17. Low risk HLA-DQ and increased body mass index in newly diagnosed type 1 diabetes children in the Better Diabetes Diagnosis study in Sweden

Author

Carlsson, A, Kockum, I, Lindblad, B, Engleson, L, Nilsson, A, Forsander, G, Karlsson, A-K, Kernell, A, Ludvigsson, Johnny, Marcus, C, Zachrisson, I, Ivarsson, S-A, Lernmak, A, Carlsson, A, Kockum, I, Lindblad, B, Engleson, L, Nilsson, A, Forsander, G, Karlsson, A-K, Kernell, A, Ludvigsson, Johnny, Marcus, C, Zachrisson, I, Ivarsson, S-A, and Lernmak, A

Abstract

Objective: Type 1 diabetes and obesity has increased in childhood. We therefore tested the hypothesis that type 1 diabetes human leukocyte antigen DQ (HLA-DQ) risk genotypes may be associated with increased body mass index (BMI). less thanbrgreater than less thanbrgreater thanDesign: The type 1 diabetes high-risk HLA-DQ A1*05:01-B1*02:01/A1*03:01-B1*03:02 genotype along with lower risk DQ genotypes were determined at the time of clinical onset by PCR and hybridization with allele-specific probes. BMI was determined after diabetes was stabilized. less thanbrgreater than less thanbrgreater thanSubjects: A total of 2403 incident type 1 diabetes children below 18 years of age were ascertained in the Swedish national Better Diabetes Diagnosis (BDD) study between May 2005 to September 2009. All children classified with type 1 diabetes, including positivity for at least one islet autoantibody, were investigated. less thanbrgreater than less thanbrgreater thanResults: Overall, type 1 diabetes HLA-DQ risk was negatively associated with BMI (Pandlt;0.0008). The proportion of the highest risk A1*05:01-B1*02:01/A1*03:01-B1*03:02 genotype decreased with increasing BMI (Pandlt;0.0004). However, lower risk type 1 diabetes DQ genotypes were associated with an increased proportion of patients who were overweight or obese (Pandlt;0.0001). Indeed, the proportion of patients with the low-risk A1*05:01-B1*02:01/A1*05:01-B1*02:01 genotype increased with increasing BMI (Pandlt;0.003). The magnitude of association on the multiplicative scale between the A1*05:01-B1*02:01/A1*05:01-B1*02:01 genotype and increased BMI was significant (Pandlt;0.006). The odds ratio in patients with this genotype of being obese was 1.80 (95% confidence interval 1.21-2.61; Pandlt;0.006). The increased proportion of overweight type 1 diabetes children with the A1*05:01-B1*02:01 haplotype was most pronounced in children diagnosed between 5 and 9 years of age. less thanbrgreater than less thanbrgreater thanConclusi, Funding Agencies|Swedish Child Diabetes Foundation||National Institutes of Health|DK63861DK26190|Swedish Research Council||Swedish Diabetes Association||Knut & Alice Wallenberg Foundation||Lion Club International District 101-S||Skane County Council for Research and Development

Published

2012

18. C-peptide in the classification of diabetes in children and adolescents

Author

Ludvigsson, Johnny, Carlsson, A, Forsander, G, Ivarsson, S, Kockume, I, Lernmark, A, Lindblad, B, Marcus, C, Samuelsson, Ulf, Ludvigsson, Johnny, Carlsson, A, Forsander, G, Ivarsson, S, Kockume, I, Lernmark, A, Lindblad, B, Marcus, C, and Samuelsson, Ulf

Abstract

Aim: To report C-peptide results in newly diagnosed patients and the relation to clinical diagnosis of diabetes. less thanbrgreater than less thanbrgreater thanMethods: A nation-wide cohort, the Better Diabetes Diagnosis study was used to determine serum C-peptide at diagnosis in 2734 children and adolescents. Clinical data were collected at diagnosis and follow-up. C-peptide was determined in a validated and controlled time-resolved fluoroimmunoassay. less thanbrgreater than less thanbrgreater thanResults: The clinical classification of diabetes, before any information on human leukocyte antigen, islet autoantibodies, or C-peptide was received, was type 1 diabetes (T1D) in 93%, type 2 diabetes (T2D) in 1.9%, maturity onset diabetes of the young (MODY) in 0.8%, secondary diabetes (0.6%), while 3.3% could not be classified. In a random, non-fasting serum sample at diagnosis, 56% of the patients had a C-peptide value andgt; 0.2 nmol/L. Children classified as T2D had the highest mean C-peptide (1.83 + 1.23 nmol/L) followed by MODY (1.04 +/- 0.71 nmol/L) and T1D (0.28 +/- 0.25 nmol/L). Only 1/1037 children who had C-peptide andlt; 0.2 nmol/L at diagnosis was classified with a type of diabetes other than T1D. Predictive value of C-peptide andgt; 1.0 nmol/L for the classification of either T2D or MODY was 0.46 [confidence interval 0.37-0.58]. less thanbrgreater than less thanbrgreater thanConclusions: More than half of children with newly diagnosed diabetes have clinically important residual beta-cell function. As the clinical diagnosis is not always straightforward, a random C-peptide taken at diagnosis may help to classify diabetes. There is an obvious use for C-peptide determinations to evaluate beta-cell function in children with diabetes., Funding Agencies|Barndiabetesfonden (the Swedish Child Diabetes Foundation)

Published

2012

19. Age-dependent variation of genotypes in MHC II transactivator gene (CIITA) in controls and association to type 1 diabetes

Author

Gyllenberg, A, Asad, S, Piehl, F, Swanberg, M, Padyukov, L, Van Yserloo, B, Rutledge, E A, McNeney, B, Graham, J, Orho-Melander, M, Lindholm, E, Graff, C, Forsell, C, Akesson, K, Landin-Olsson, M, Carlsson, A, Forsander, G, Ivarsson, S A, Larsson, H, Lindblad, B, Ludvigsson, Johnny, Marcus, C, Lernmark, A, Alfredsson, L, Olsson, T, Kockum, I, Gyllenberg, A, Asad, S, Piehl, F, Swanberg, M, Padyukov, L, Van Yserloo, B, Rutledge, E A, McNeney, B, Graham, J, Orho-Melander, M, Lindholm, E, Graff, C, Forsell, C, Akesson, K, Landin-Olsson, M, Carlsson, A, Forsander, G, Ivarsson, S A, Larsson, H, Lindblad, B, Ludvigsson, Johnny, Marcus, C, Lernmark, A, Alfredsson, L, Olsson, T, and Kockum, I

Abstract

The major histocompatibility complex class II transactivator (CIITA) gene (16p13) has been reported to associate with susceptibility to multiple sclerosis, rheumatoid arthritis and myocardial infarction, recently also to celiac disease at genome-wide level. However, attempts to replicate association have been inconclusive. Previously, we have observed linkage to the CIITA region in Scandinavian type 1 diabetes (T1D) families. Here we analyze five Swedish T1D cohorts and a combined control material from previous studies of CIITA. We investigate how the genotype distribution within the CIITA gene varies depending on age, and the association to T1D. Unexpectedly, we find a significant difference in the genotype distribution for markers in CIITA (rs11074932, P = 4 x 10(-5) and rs3087456, P = 0.05) with respect to age, in the collected control material. This observation is replicated in an independent cohort material of about 2000 individuals (P = 0.006, P = 0.007). We also detect association to T1D for both markers, rs11074932 (P = 0.004) and rs3087456 (P = 0.001), after adjusting for age at sampling. The association remains independent of the adjacent T1D risk gene CLEC16A. Our results indicate an age-dependent variation in CIITA allele frequencies, a finding of relevance for the contrasting outcomes of previously published association studies., Funding Agencies|Juvenile Diabetes Research Foundation International|2-2000-5701-2001-873|Swedish Research Council||Swedish Diabetes Foundation (Svenska Diabetes Fonden)||Swedish Child Diabetes Foundation (Barndiabetes Fonden)||Novo Nordisk Foundation||Magnus Bergvalls Foundation||NIH|DK-17047|Swedish Brain Power initiative||Gun and Bertil Stohnes Foundation||Foundation for Old Servants||Alzheimer Foundation||LIONS Foundation for Research of Age Related Disorders||AFA foundation||Soderberg Foundation||Knut and Alice Wallenbergs Foundation||Neuropromise|LSHM-CT-2005-018637

Published

2012

20. Clinical and genetical characterisation of a series of patients with type 1 diabetes induced by interferon therapy in DIABETOLOGIA, vol 53, issue , pp S119-S120

Author

Delli, A J, Vaziri-Sani, F, Carlsson, A, Forsander, G, Ivarsson, S A, Lindblad, B, Ludvigsson, Johnny, Marcus, C, Lernmark, A, Delli, A J, Vaziri-Sani, F, Carlsson, A, Forsander, G, Ivarsson, S A, Lindblad, B, Ludvigsson, Johnny, Marcus, C, and Lernmark, A

Abstract

n/a

Published

2010

21. Novel triples mix radio binding assay for the ZnT8 (ZnT8RWQ) autoantibody variants in children with newly diagnosed diabetes in DIABETOLOGIA, vol 53, issue , pp S116-S116

Author

Vaziri-Sani, F, Delli, A J, Larsson, H E, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S A, Ludvigsson, Johnny, Marcus, C, Lernmark, A, Vaziri-Sani, F, Delli, A J, Larsson, H E, Lindblad, B, Carlsson, A, Forsander, G, Ivarsson, S A, Ludvigsson, Johnny, Marcus, C, and Lernmark, A

Abstract

n/a

Published

2010

22. The non-inherited maternal HLA haplotype affects the risk for type 1 diabetes

Author

Åkesson, K, Carlsson, A, Ivarsson, S A, Johansson, C, Weidby, B M, Ludvigsson, Johnny, Gustavsson, B, Lernmark, A, Kockum, I, Åkesson, K, Carlsson, A, Ivarsson, S A, Johansson, C, Weidby, B M, Ludvigsson, Johnny, Gustavsson, B, Lernmark, A, and Kockum, I

Abstract

The aim was to test the hypothesis that the human leucocyte antigen (HLA) haplotype that is not inherited from the mother, that is, the non-inherited maternal antigen (NIMA) affects the risk for type 1 diabetes (T1D). A total of 563 children with T1D and 286 non-diabetic control children from Sweden were genotyped for DRB1, DQA1 and DQB1 alleles. The frequency of positively (DR4-DQA1*0301-B1*0302 and DR3-DQA1*0501-B1*0201), negatively (DR15-DQ A1*0102-B1*0602) or neutrally (all other) T1D associated HLA haplotypes were compared between NIMA and non-inherited paternal antigen (NIPA). All comparisons were carried out between HLA-matched patients and controls. The frequency of positively associated NIMA was higher among both DR4/X-positive healthy individuals compared wit DR4/X-positive patients (P < 0.00003) and DR3/X-positive healthy individuals compared with DR3/X-positive patients (P < 0.009). No such difference was observed for NIPA. High-risk NIMA was increased compared to NIPA among healthy DR3/X- and DR4/X-positive children (P < 0.05). There was no difference in frequency of positively associated haplotypes between patient NIMA and NIPA. The NIMA but not the NIPA affects the risk for T1D, suggesting that not only the inherited but also non-inherited maternal HLA haplotypes, perhaps through microchimerism or other mechanisms, may influence the risk for the disease.

Published

2009

23. The type 1 diabetes protective HLA DQB1*0602 allele is less frequent in gestational diabetes mellitus.

Author

Papadopoulou, Anastasia, Lynch, Kristian, Shaat, Nael, Nilsson, Anita, Lernmark, Barbro, Berntorp, Kerstin, Ivarsson, S-A, Agardh, Carl-David, Lernmark, Åke, Carlsson, Annelie, DiPiS Study Group, Papadopoulou, Anastasia, Lynch, Kristian, Shaat, Nael, Nilsson, Anita, Lernmark, Barbro, Berntorp, Kerstin, Ivarsson, S-A, Agardh, Carl-David, Lernmark, Åke, Carlsson, Annelie, and DiPiS Study Group

Abstract

AIMS/HYPOTHESIS: We tested whether gestational diabetes mellitus (GDM) is associated with HLA-DQ genotypes. METHODS: A total of 764 mothers with non-autoimmune (GAD65, insulinoma-associated protein 2 [IA-2] and insulin autoantibody-negative) GDM were ascertained between September 2000 and August 2004 in the population-based Diabetes Prediction in Skåne (DiPiS) study. HLA-DQB1 genotypes were determined in these mothers and in 1191 randomly selected non-diabetic control mothers also negative for islet autoantibodies. The data were analysed in relation to maternal age, country of birth, number of pregnancies/siblings and pregnancy weight gain. RESULTS: The frequency of type 1 diabetes high-risk HLA-DQ alleles (DQB1*0201, DQB1*0302) did not differ between GDM mothers and controls. In contrast, the low-risk DQB1*0602 allele was less prevalent (OR 0.64, 95% CI = 0.51-0.80, p = 0.0006) in GDM than in control mothers. The difference in DQB1*0602 frequency between GDM mothers and controls remained after multiple logistic regression analysis correcting for maternal age, country of birth, number of pregnancies/siblings and weight gain during pregnancy (OR 0.67, 95% CI 0.51-0.88, p = 0.009). CONCLUSIONS/INTERPRETATION: The negative association between mothers who have non-autoimmune GDM and HLA-DQ*0602 suggest that this allele may protect not only from type 1 diabetes but also from GDM.

Published

2009

24. Temporal trends of HLA genotype frequencies of type 1 diabetes patients in Sweden from 1986 to 2005 suggest altered risk

Author

Resic-Lindehammer, Sabina, Larsson, K., Örtqvist, E., Carlsson, A., Cederwall, E., Cilio, C. M., Ivarsson, S-A., Jönsson, B. A., Larsson, H. E., Lynch, K., Neiderud, J., Nilsson, A., Sjöblad, S., Lernmark, Å., Aili, M., Bååth, L. E., Carlsson, E., Edenwall, H., Forsander, G., Granstro, B. W., Gustavsson, I., Hanås, R., Hellenberg, L., Hellgren, H., Holmberg, E., Hörnell, H., Ivarsson, Sten-A., Johansson, C., Jonsell, G., Kockum, K., Lindblad, B., Lindh, A., Ludvigsson, J., Myrdal, U., Segnestam, K., Skogsberg, L., Strömberg, L., Ståhle, U., Thalme, B., Tullus, K., Tuvemo, Torsten, Wallensteen, M., Westphal, O., Aman, J., Resic-Lindehammer, Sabina, Larsson, K., Örtqvist, E., Carlsson, A., Cederwall, E., Cilio, C. M., Ivarsson, S-A., Jönsson, B. A., Larsson, H. E., Lynch, K., Neiderud, J., Nilsson, A., Sjöblad, S., Lernmark, Å., Aili, M., Bååth, L. E., Carlsson, E., Edenwall, H., Forsander, G., Granstro, B. W., Gustavsson, I., Hanås, R., Hellenberg, L., Hellgren, H., Holmberg, E., Hörnell, H., Ivarsson, Sten-A., Johansson, C., Jonsell, G., Kockum, K., Lindblad, B., Lindh, A., Ludvigsson, J., Myrdal, U., Segnestam, K., Skogsberg, L., Strömberg, L., Ståhle, U., Thalme, B., Tullus, K., Tuvemo, Torsten, Wallensteen, M., Westphal, O., and Aman, J.

Abstract

The aim of this study was to compare the frequency of human leukocyte antigen (HLA) genotypes in 1-18-year-old patients with type 1 diabetes newly diagnosed in 1986-1987 (n = 430), 1996-2000 (n = 342) and in 2003-2005 (n = 171). We tested the hypothesis that the HLA DQ genotype distribution changes over time. Swedish type 1 diabetes patients and controls were typed for HLA using polymerase chain reaction amplification and allele specific probes for DQ A1* and B1* alleles. The most common type 1 diabetes HLA DQA1*-B1*genotype 0501-0201/0301-0302 was 36% (153/430) in 1986-1987 and 37% (127/342) in 1996-2000, but decreased to 19% (33/171) in 2003-2005 (P \ 0.0001). The 0501-0201/0501-0201 genotype increased from 1% in 1986-1987 to 7% in 1996-2000 (P = 0.0047) and to 5% in 2003-2005 (P > 0.05). This study in 1-18-year-old Swedish type 1 diabetes patients supports the notion that there is a temporal change in HLA risk.

Published

2008

25. Children developing type 1 diabetes before 6 years of age have increased linear growth independent of HLA genotypes

Author

Larsson, H. Elding, Hansson, G., Carlsson, A., Cederwall, E., Jonsson, Björn, Jönsson, B., Larsson, K., Lynch, K., Neiderud, J., Lernmark, A., Ivarsson, S. -A., Larsson, H. Elding, Hansson, G., Carlsson, A., Cederwall, E., Jonsson, Björn, Jönsson, B., Larsson, K., Lynch, K., Neiderud, J., Lernmark, A., and Ivarsson, S. -A.

Abstract

Aims/hypothesis High birthweight and increased childhood growth are risk factors for type 1 diabetes. Relative birthweight is associated with HLA genotypes that confer a high risk of diabetes. Our aims were to test whether young children prior to clinical onset of type 1 diabetes have increased: (1) birthweight or birth length standard deviation scores (SDS), (2) height development SDS, or (3) BMI SDS during first 18 months of life and whether these parameters are related to HLA genotypes or mid-parental height (MPH). Methods Birthweight, birth length, weight and height were obtained from 58 type 1 diabetes children and 155 controls matched for HLA or not in the Diabetes Prediction in Skane study. Results Birth length SDS corrected for MPH was increased in children developing diabetes compared with all (p < , 0.048) and with non-HLA- (p < , 0.050) but not with HLA-matched controls. Children developing diabetes had increased height gain at 0 to 18 months of age (p < ; 0.005). Diabetic children were significantly taller from 6 to 18 months of age when correcting for MPH compared with non-HLA-matched as well as HLA-matched controls, but BMI was not increased. Conclusions/interpretation Birth length SDS was associated with diabetes risk HLA. When corrected for MPH, children developing diabetes were taller at birth than non-HLA- but not taller than HLA-matched controls. Diabetic children had increased MPH-corrected height up to 18 months of age compared with both HLA- and non-HLA-matched controls. High-risk HLA affects prenatal growth, but other factors may explain the increased postnatal linear growth in children developing diabetes.

Published

2008

26. GAD treatment and insulin secretion in recent-onset type 1 diabetes

Author

Ludvigsson, J, Faresjö, Maria, Hedman, M, Axelsson, S, Chéramy, M, Phil, M, Vaarala, O, Forsander, G, Ivarsson, S, Johansson, C, Lindh, A, Nilsson, N-Ö, Åman, J, Örtqvist, E, Zerhouni, P, Casas, R, Ludvigsson, J, Faresjö, Maria, Hedman, M, Axelsson, S, Chéramy, M, Phil, M, Vaarala, O, Forsander, G, Ivarsson, S, Johansson, C, Lindh, A, Nilsson, N-Ö, Åman, J, Örtqvist, E, Zerhouni, P, and Casas, R

Published

2008

27. Temporal trends of HLA genotype frequencies of type 1 diabetes patients in Sweden from 1986 to 2005 suggest altered risk

Author

Resic-Lindehammer, Sabina, Larsson, K., Örtqvist, E., Carlsson, A., Cederwall, E., Cilio, C. M., Ivarsson, S.-A., Jönsson, B. A., Larsson, H. E., Lynch, K., Neiderud, J., Nilsson, A., Sjöblad, S., Lernmark, Å., Resic-Lindehammer, Sabina, Larsson, K., Örtqvist, E., Carlsson, A., Cederwall, E., Cilio, C. M., Ivarsson, S.-A., Jönsson, B. A., Larsson, H. E., Lynch, K., Neiderud, J., Nilsson, A., Sjöblad, S., and Lernmark, Å.

Abstract

The aim of this study was to compare the frequency of human leukocyte antigen (HLA) genotypes in 1-18-year-old patients with type 1 diabetes newly diagnosed in 1986-1987 (n = 430), 1996-2000 (n = 342) and in 2003-2005 (n = 171). We tested the hypothesis that the HLA DQ genotype distribution changes over time. Swedish type 1 diabetes patients and controls were typed for HLA using polymerase chain reaction amplification and allele specific probes for DQ A1* and B1* alleles. The most common type 1 diabetes HLA DQA1*-B1*genotype 0501-0201/0301-0302 was 36% (153/430) in 1986-1987 and 37% (127/342) in 1996-2000, but decreased to 19% (33/171) in 2003-2005 (P \ 0.0001). The 0501-0201/0501-0201 genotype increased from 1% in 1986-1987 to 7% in 1996-2000 (P = 0.0047) and to 5% in 2003-2005 (P > 0.05). This study in 1-18-year-old Swedish type 1 diabetes patients supports the notion that there is a temporal change in HLA risk.

Published

2008

28. Eta Carinae across the 2003.5 minimum: Spectroscopic Evidence for Massive Binary Interactions

Author

Nielsen, K. E., Corcoran, M. F., Gull, T. R., Hillier, D. J., Hamaguchi, K., Ivarsson, S., Lindler, D. J., Nielsen, K. E., Corcoran, M. F., Gull, T. R., Hillier, D. J., Hamaguchi, K., Ivarsson, S., and Lindler, D. J.

Abstract

We have analyzed high spatial, moderate spectral resolution observations of Eta Carinae obtained with the STIS from 1998.0 to 2004.3. The spectra show prominent P-Cygni lines in H I, Fe II and He I which are complicated by blends and contamination by nebular emission and absorption along the line-of-sight toward the observer. All lines show phase and species dependent variations in emission and absorption. For most of the cycle the He I emission is blueshifted relative to the H I and Fe II P-Cygni emission lines, which are approximately centered at system velocity. The blueshifted He I absorption varies in intensity and velocity throughout the 2024 day period. We construct radial velocity curves for the absorption component of the He I and H I lines. The He I absorption shows significant radial velocity variations throughout the cycle, with a rapid change of over 200 km/s near the 2003.5 event. The H I velocity curve is similar to that of the He I absorption, though offset in phase and reduced in amplitude. We interpret the complex line profile variations in He I, H I and Fe II to be a consequence of the dynamic interaction of the dense wind of Eta Car A with the less dense, faster wind plus the radiation field of a hot companion star, Eta Car B. During most of the orbit, Eta Car B and the He+ recombination zone are on the near side of Eta Car A, producing blueshifted He I emission. He I absorption is formed in the part of the He+ zone that intersects the line-of-sight toward Eta Car. We use the variations seen in He I and the other P-Cygni lines to constrain the geometry of the orbit and the character of Eta Car B., Comment: 16 pages, 18 figures

Published

2007

29. Eta Carinae across the 2003.5 minimum: Spectroscopic Evidence for Massive Binary Interactions

Author

Nielsen, K. E., Corcoran, M. F., Gull, T. R., Hillier, D. J., Hamaguchi, K., Ivarsson, S., Lindler, D. J., Nielsen, K. E., Corcoran, M. F., Gull, T. R., Hillier, D. J., Hamaguchi, K., Ivarsson, S., and Lindler, D. J.

Abstract

We have analyzed high spatial, moderate spectral resolution observations of Eta Carinae obtained with the STIS from 1998.0 to 2004.3. The spectra show prominent P-Cygni lines in H I, Fe II and He I which are complicated by blends and contamination by nebular emission and absorption along the line-of-sight toward the observer. All lines show phase and species dependent variations in emission and absorption. For most of the cycle the He I emission is blueshifted relative to the H I and Fe II P-Cygni emission lines, which are approximately centered at system velocity. The blueshifted He I absorption varies in intensity and velocity throughout the 2024 day period. We construct radial velocity curves for the absorption component of the He I and H I lines. The He I absorption shows significant radial velocity variations throughout the cycle, with a rapid change of over 200 km/s near the 2003.5 event. The H I velocity curve is similar to that of the He I absorption, though offset in phase and reduced in amplitude. We interpret the complex line profile variations in He I, H I and Fe II to be a consequence of the dynamic interaction of the dense wind of Eta Car A with the less dense, faster wind plus the radiation field of a hot companion star, Eta Car B. During most of the orbit, Eta Car B and the He+ recombination zone are on the near side of Eta Car A, producing blueshifted He I emission. He I absorption is formed in the part of the He+ zone that intersects the line-of-sight toward Eta Car. We use the variations seen in He I and the other P-Cygni lines to constrain the geometry of the orbit and the character of Eta Car B., Comment: 16 pages, 18 figures

Published

2007

30. Reduction of tissue transglutaminase autoantibody levels by gluten-free diet is associated with changes in subsets of peripheral blood lymphocytes in children with newly diagnosed coeliac disease.

Author

Agardh, Daniel, Lynch, Kristian, Brundin, Charlotte, Ivarsson, S-A, Lernmark, Åke, Cilio, C M, Agardh, Daniel, Lynch, Kristian, Brundin, Charlotte, Ivarsson, S-A, Lernmark, Åke, and Cilio, C M

Published

2006

31. A possible implication of soluble CTLA-4 in Type 1 Diabetes.

Author

Nyholm, J, Rigolio, R, Zaigham, I, Ivarsson, S, Cilio, C, Cilio, CM, RIGOLIO, ROBERTA, Nyholm, J, Rigolio, R, Zaigham, I, Ivarsson, S, Cilio, C, Cilio, CM, and RIGOLIO, ROBERTA

Published

2005

32. A possible implication of soluble CTLA-4 in type 1 diabetes

Author

Nyholm, J, Rigolio, R, Zaigham, I, Ivarsson, S, Cilio, C, Cilio, CM, Nyholm, J, Rigolio, R, Zaigham, I, Ivarsson, S, Cilio, C, and Cilio, CM

Published

2005

33. Improved oscillator strengths and wavelengths for Os I and Ir I, and new results on early r-process nucleosynthesis

Author

Ivarsson, S., Andersen, J., Nordström, B., Dai, X., Johansson, S., Lundberg, H., Nilsson, H., Hill, V., Lundqvist, M., Wyart, J.F., Ivarsson, S., Andersen, J., Nordström, B., Dai, X., Johansson, S., Lundberg, H., Nilsson, H., Hill, V., Lundqvist, M., and Wyart, J.F.

Abstract

Os I, lr I

Published

2003

34. Improved oscillator strengths and wavelengths for Os I and Ir I, and new results on early r-process nucleosynthesis

Author

Ivarsson, S., Andersen, J., Nordström, B., Dai, X., Johansson, S., Lundberg, H., Nilsson, H., Hill, V., Lundqvist, M., Wyart, J.F., Ivarsson, S., Andersen, J., Nordström, B., Dai, X., Johansson, S., Lundberg, H., Nilsson, H., Hill, V., Lundqvist, M., and Wyart, J.F.

Abstract

Os I, lr I

Published

2003

35. Timing of oestrogen therapy in girls with Turner syndrome: the Swedish experiences and a review. In : Optimizing Health Care for Turner Patients in the 21st Century. Proceedings of the 5th International Turner Symposium held in Naples on 23-25 March 2000

Author

Nilsson, K O, Albertsson-Wikland, K, Alm, J, Aronson, S, Gustafsson, J, Hagenäs, L, Häger, A, Ivarsson, S A, Kriström, B, Marcus, C, Moell, C, Ritzén, M, Tuvemo, T, Westgren, U, Westphal, O, Åman, J, Nilsson, K O, Albertsson-Wikland, K, Alm, J, Aronson, S, Gustafsson, J, Hagenäs, L, Häger, A, Ivarsson, S A, Kriström, B, Marcus, C, Moell, C, Ritzén, M, Tuvemo, T, Westgren, U, Westphal, O, and Åman, J

Published

2000

36. Effect of growth hormone (GH) during puberty in GH-deficient children : preliminary results from an ongoing randomized trial with different dose regimens

Author

Albertsson Wikland, K, Alm, F, Aronsson, S, Gustafsson, J, Hagenas, L, Hager, A, Ivarsson, S, Kristrom, B, Marcus, C, Moell, C, Nilsson, KO, Ritzen, M, Tuvemo, T, Westgren, U, Westphal, O, Aman, J, Albertsson Wikland, K, Alm, F, Aronsson, S, Gustafsson, J, Hagenas, L, Hager, A, Ivarsson, S, Kristrom, B, Marcus, C, Moell, C, Nilsson, KO, Ritzen, M, Tuvemo, T, Westgren, U, Westphal, O, and Aman, J

Published

1999

37. Prevalence of coeliac disease in Turner syndrome

Author

Ivarsson, S-A, Carlsson, A, Bredberg, A, Alm, J, Aronsson, S, Gustafsson, J, Hagenas, L, Hager, A, Kristrom, B, Marcus, C, Moell, C, Nilsson, K-O, Tuvemo, T, Westphal, O, Albertsson-Wikland, K, Aman, J, Ivarsson, S-A, Carlsson, A, Bredberg, A, Alm, J, Aronsson, S, Gustafsson, J, Hagenas, L, Hager, A, Kristrom, B, Marcus, C, Moell, C, Nilsson, K-O, Tuvemo, T, Westphal, O, Albertsson-Wikland, K, and Aman, J

Published

1999

38. Effect of growth hormone (GH) during puberty in GH-deficient children : preliminary results from an ongoing randomized trial with different dose regimens.

Author

Albertsson Wikland, K, Alm, F, Aronsson, S, Gustafsson, J, Hagenäs, L, Häger, A, Ivarsson, S, Kriström, Berit, Marcus, C, Moëll, C, Nilsson, K O, Ritzén, M, Tuvemo, T, Westgren, U, Westphal, O, Aman, J, Albertsson Wikland, K, Alm, F, Aronsson, S, Gustafsson, J, Hagenäs, L, Häger, A, Ivarsson, S, Kriström, Berit, Marcus, C, Moëll, C, Nilsson, K O, Ritzén, M, Tuvemo, T, Westgren, U, Westphal, O, and Aman, J

Abstract

This paper reports results from an ongoing, randomized, multicentre national trial. The aim is to elucidate whether a dose of growth hormone (GH) of 0.2 IU/kg (0.07 mg/kg), given either as once-daily or twice-daily injections during puberty, is more effective than a once-daily dose of 0.1 IU/kg/day (0.03 mg/kg/day) in improving final height in children with GH deficiency (GHD). The twice-daily regimen comes closer to the spontaneous GH secretion pattern in puberty. Ninety-two children with GHD who had been receiving GH therapy for at least 1 year, and with spontaneous puberty or who were prepubertal and due to be started on replacement therapy to induce puberty, were randomly assigned to receive GH as follows: group A, 0.1 IU/kg/day (0.03 mg/kg/day), administered once daily; group B, 0.2 IU/kg/day (0.07 mg/kg/day), administered once daily; and group C, 0.2 IU/kg/day (0.07 mg/kg/day), divided into two equal injections given at 12-hour intervals. Pubertal height gain was 0.7, 0.7 and 1.3 SDS for groups A, B and C, respectively. The gain in height during puberty was thus most marked in group C. Mean final height, when corrected for parental height, was between 0 and 1 SDS in all treatment groups. All but seven children reached a final height within +/- 2 SD of the general population. There was a wide range of final heights in all three treatment groups. This variation in response suggests the need to individualize treatment in order to achieve an appropriate final height for most individuals.

Published

1999

39. Prevalence of coeliac disease in Turner syndrome.

Author

Ivarsson, S A, Carlsson, A, Bredberg, A, Alm, J, Aronsson, S, Gustafsson, J, Hagenäs, L, Häger, A, Kriström, Berit, Marcus, C, Moëll, C, Nilsson, K O, Tuvemo, T, Westphal, O, Albertsson-Wikland, K, Aman, J, Ivarsson, S A, Carlsson, A, Bredberg, A, Alm, J, Aronsson, S, Gustafsson, J, Hagenäs, L, Häger, A, Kriström, Berit, Marcus, C, Moëll, C, Nilsson, K O, Tuvemo, T, Westphal, O, Albertsson-Wikland, K, and Aman, J

Abstract

This study was undertaken to investigate the prevalence of coeliac disease in children and adolescents with Turner syndrome. Eighty-seven children and adolescents with Turner syndrome were screened for IgA-antiendomysium antibodies (EMA) and IgA-antigliadin antibodies (AGA), 5% (4/87) being found to be EMA-positive, and 15% (13/87) to have AGA levels above normal. Of the 10 patients who were either AGA- or EMA-positive and further investigated with intestinal biopsy, four manifested villous atrophy (i.e. all three of the EMA-positive patients, but only one of the seven AGA-positive patients). The results suggest EMA-positivity to be a good immunological marker for use in screening for coeliac disease, and such screening to be justified in patients with Turner syndrome.

Published

1999

40. Effect of growth hormone (GH) during puberty in GH-deficient children : preliminary results from an ongoing randomized trial with different dose regimens.

Author

Albertsson Wikland, K, Alm, F, Aronsson, S, Gustafsson, J, Hagenäs, L, Häger, Anders, Ivarsson, S, Kriström, B, Marcus, C, Moell, C, Nilsson, KO, Ritzén, M, Tuvemo, T, Westergren, U, Westphal, O, Åman, J, Albertsson Wikland, K, Alm, F, Aronsson, S, Gustafsson, J, Hagenäs, L, Häger, Anders, Ivarsson, S, Kriström, B, Marcus, C, Moell, C, Nilsson, KO, Ritzén, M, Tuvemo, T, Westergren, U, Westphal, O, and Åman, J

Published

1999

41. Skolan har del i ansvaret för barn med typ 1-diabetes.

Author

Thernlund, G, Fredin, K, Hägglöf, B, Ivarsson, S, Lernmark, B, Ludvigsson, Johnny, Sjöblad, S, Thernlund, G, Fredin, K, Hägglöf, B, Ivarsson, S, Lernmark, B, Ludvigsson, Johnny, and Sjöblad, S

Published

1999

42. Thyroid dysfunction in Down's syndrome : relation to age and thyroid autoimmunity

Author

Karlsson, B, Gustafsson, J, Hedov, Gerth, Ivarsson, S A, Annerén, Göran, Karlsson, B, Gustafsson, J, Hedov, Gerth, Ivarsson, S A, and Annerén, Göran

Abstract

BACKGROUND: The prevalence of thyroid disease is increased in Down's syndrome. Most available data come from cross sectional studies. AIMS: To study longitudinally thyroid function in patients with Down's syndrome in Uppsala county (85 patients) up to the age of 25 years. METHODS: Observational study based on yearly follow up in a children's clinic. Thyroid function tests were performed at each visit to the clinic. RESULTS: Hypothyroidism was found in 30 and hyperthyroidism was found in two of the 85 patients. No sex difference was seen. Half of the patients with hypothyroidism acquired the condition before the age of 8 years, but only one of them displayed thyroid autoantibodies at diagnosis. Most patients who developed hypothyroidism after this age had thyroid autoantibodies. In the prepubertal patients with hypothyroidism, growth velocity was lower during the year before the start of thyroxine treatment than during the year after treatment began; it was also lower than that of sex and age matched euthyroidic children with Down's syndrome. CONCLUSION: Thyroid dysfunction in patients with Down's syndrome is common in childhood. Consequently, annual screening is important. Autoimmune thyroid disease is uncommon in young children with Down's syndrome but is common after 8 years of age.

Published

1998

43. Thyroid dysfunction in Down's syndrome : relation to age and thyroid autoimmunity.

Author

Karlsson, Bengt, Gustafsson, Jan, Hedov, Gerth, Ivarsson, S A, Annerén, Göran, Karlsson, Bengt, Gustafsson, Jan, Hedov, Gerth, Ivarsson, S A, and Annerén, Göran

Abstract

BACKGROUND: The prevalence of thyroid disease is increased in Down's syndrome. Most available data come from cross sectional studies. AIMS: To study longitudinally thyroid function in patients with Down's syndrome in Uppsala county (85 patients) up to the age of 25 years. METHODS: Observational study based on yearly follow up in a children's clinic. Thyroid function tests were performed at each visit to the clinic. RESULTS: Hypothyroidism was found in 30 and hyperthyroidism was found in two of the 85 patients. No sex difference was seen. Half of the patients with hypothyroidism acquired the condition before the age of 8 years, but only one of them displayed thyroid autoantibodies at diagnosis. Most patients who developed hypothyroidism after this age had thyroid autoantibodies. In the prepubertal patients with hypothyroidism, growth velocity was lower during the year before the start of thyroxine treatment than during the year after treatment began; it was also lower than that of sex and age matched euthyroidic children with Down's syndrome. CONCLUSION: Thyroid dysfunction in patients with Down's syndrome is common in childhood. Consequently, annual screening is important. Autoimmune thyroid disease is uncommon in young children with Down's syndrome but is common after 8 years of age.

Published

1998

44. Improved final height in girls with Turner's syndrome treated with growth hormone and oxandrolone.

Author

Nilsson, K O, Albertsson-Wikland, K, Alm, J, Aronson, S, Gustafsson, J, Hagenäs, L, Häger, A, Ivarsson, S A, Karlberg, J, Kriström, Berit, Marcus, C, Moell, C, Ritzen, M, Tuvemo, T, Wattsgård, C, Westgren, U, Westphal, O, Aman, J, Nilsson, K O, Albertsson-Wikland, K, Alm, J, Aronson, S, Gustafsson, J, Hagenäs, L, Häger, A, Ivarsson, S A, Karlberg, J, Kriström, Berit, Marcus, C, Moell, C, Ritzen, M, Tuvemo, T, Wattsgård, C, Westgren, U, Westphal, O, and Aman, J

Abstract

The spontaneous growth process in Turner's syndrome is characterized by a progressive decline in height velocity during childhood and no pubertal growth spurt. Therefore, therapy aimed at improving height during childhood as well as increasing final height is desirable for most girls with Turner's syndrome. Forty-five girls with Turner's syndrome, 9-16 yr of age (mean age, 12.2 yr), were allocated to three study groups. Group 1 (n = 13) was initially treated with oxandrolone alone; after 1 yr of treatment, GH without (group 1a; n = 6) or with (group 1b; n = 7) ethinyl estradiol was added. Group 2 (n = 17) was treated with GH plus oxandrolone. Group 3 (n = 15) was treated with GH, oxandrolone, and ethinyl estradiol. The dosage were: GH, 0.1 IU/kg.day; oxandrolone, 0.05 mg/kg.day; and ethinyl estradiol, 100 ng/kg.day. A height of 150 cm or more was achieved in 61%, 75%, and 60% of the girls in groups 1, 2, and 3, respectively. The most impressive increase in height was seen in group 2. In this group the mean final height was 154.2 cm (SD = 6.6), which is equivalent to a mean net gain of 8.5 cm (SD = 4.6) over the projected final height. In group 3, in which ethinyl estradiol was included from the start of therapy, the initially good height velocity decelerated after 1-2 yr of treatment. Their mean final height was 151.1 (SD = 4.6) cm, equivalent to a mean net gain of 3.0 cm (SD = 3.8). A similar growth-decelerating effect of ethinyl estradiol was seen in group 1b. We conclude that in girls with Turner's syndrome who are older than 9 yr of age, treatment with GH in combination with oxandrolone results in significant growth acceleration, imitating that in normal puberty, leading to a more favorable height during childhood. This mode of treatment also results in a significantly increased final height, permitting a great number of the girls to attain a final height of more than 150 cm. However, early addition of estrogen decelerates the height velocity and reduces the gai

Published

1996

45. Relations between age, metabolic control, disease adjustment and psychological aspects in insulin-dependent diabetes mellitus

Author

Lernmark, B, Dahlquist, Gisela, Fransson, P, Hägglöf, Bruno, Ivarsson, S A, Ludvigsson, J, Sjöblad, S, Thernlund, G, Lernmark, B, Dahlquist, Gisela, Fransson, P, Hägglöf, Bruno, Ivarsson, S A, Ludvigsson, J, Sjöblad, S, and Thernlund, G

Abstract

The relations between age, metabolic control, disease adjustment, and psychological factors in boys and girls with recently diagnosed insulin-dependent diabetes mellitus (IDDM) were studied. Older girls had significant higher postremission glycosylated haemoglobin A (Hb AIc) levels (p = 0.008). Girls with more hospitalizations had a lower developmental level (p = 0.05), and had significantly more problems in the behavioural rating (p = 0.05). Boys with more hospitalizations had a more external locus of control (p = 0.01), more difficulties with disease adjustment, more emotional problems, and were also clinically assessed as having more behavioural problems. Boys showing more difficulties in psychological adjustment to the disease also had higher postremission Hb AIc levels (p = 0.02). Although Swedish children with IDDM of short disease duration do not differ from healthy children in important psychological aspects, older girls and a small group of problematic younger boys are at risk of developing metabolic imbalance after a short disease duration.

Published

1996

46. Thyroid antibodies are not a risk factor for pregnancies with Down syndrome

Author

Gustafsson, J, Anneren, G, Ericsson, U-B, Svanberg, L, Ivarsson, S-A, Gustafsson, J, Anneren, G, Ericsson, U-B, Svanberg, L, and Ivarsson, S-A

Published

1995

47. Thyroid autoantibodies, Turner's syndrome and growth hormone therapy

Author

Ivarsson, S-A, Eriksson, U-B, Nilsson, KO, Gustafsson, J, Hagenas, L, Hager, A, Moell, C, Tuvemo, T, Westphal, O, Albertsson-Wikland, K, Aman, J, Ivarsson, S-A, Eriksson, U-B, Nilsson, KO, Gustafsson, J, Hagenas, L, Hager, A, Moell, C, Tuvemo, T, Westphal, O, Albertsson-Wikland, K, and Aman, J

Published

1995

48. Thyroid autoantibodies, Turner's syndrome and growth hormone therapy

Author

Ivarsson, S-A, Eriksson, U-B, Nilsson, KO, Gustafsson, J, Hagenas, L, Hager, A, Moell, C, Tuvemo, T, Westphal, O, Albertsson-Wikland, K, Aman, J, Ivarsson, S-A, Eriksson, U-B, Nilsson, KO, Gustafsson, J, Hagenas, L, Hager, A, Moell, C, Tuvemo, T, Westphal, O, Albertsson-Wikland, K, and Aman, J

Published

1995

49. Thyroid antibodies are not a risk factor for pregnancies with Down syndrome

Author

Gustafsson, J, Anneren, G, Ericsson, U-B, Svanberg, L, Ivarsson, S-A, Gustafsson, J, Anneren, G, Ericsson, U-B, Svanberg, L, and Ivarsson, S-A

Published

1995