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2. HLA‐DQ‐conferred risk for type 1 diabetes does not alter neutralizing antibody response to a widely used enterovirus vaccine, the poliovirus vaccine

Author

Sioofy‐Khojine, A. (Amir‐Babak), Lehtonen, J. P. (Jussi P.), Nurminen, N. (Noora), Laiho, J. E. (Jutta E.), Toppari, J. (Jorma), Veijola, R. (Riitta), Lempainen, J. (Johanna), Ilonen, J. (Jorma), Knip, M. (Mikael), Hyöty, H. (Heikki), Sioofy‐Khojine, A. (Amir‐Babak), Lehtonen, J. P. (Jussi P.), Nurminen, N. (Noora), Laiho, J. E. (Jutta E.), Toppari, J. (Jorma), Veijola, R. (Riitta), Lempainen, J. (Johanna), Ilonen, J. (Jorma), Knip, M. (Mikael), and Hyöty, H. (Heikki)

Abstract

This study investigated whether children with HLA-DQ-conferred risk for type 1 diabetes (T1D) have an altered immune response to the widely-used enterovirus vaccine, namely poliovirus vaccine, and whether initiation of autoimmunity to pancreatic islets modulates this response. Neutralizing antibodies induced by the inactivated poliovirus vaccine against poliovirus type 1 (Salk) were analysed as a marker of protective immunity at the age of 18 months in a prospective birth cohort. No differences were observed in antibody titers between children with and without genetic risk for T1D (odds ratio [OR] = 0.90 [0.83, 1.06], p = 0.30). In the presence of the genetic risk, no difference was observed between children with and without islet autoimmunity (OR = 1.00 [0.78, 1.28], p = 1.00). This did not change when only children with the autoimmunity before 18 months of age were included in the analyses (OR = 1.00 [0.85, 1.18], p = 1.00). No effect was observed when groups were stratified based on autoantigen specificity of the first-appearing autoantibody (IAA or GADA). The children in each comparison group were matched for sex, calendar year and month of birth, and municipality. Accordingly, we found no indication that children who are at risk to develop islet autoimmunity would have a compromised humoral immune response which could have increased their susceptibility for enterovirus infections. In addition, the proper immune response supports the idea of testing novel enterovirus vaccines for the prevention of T1D among these individuals.

Published
2023

3. Dietary fatty acid intake in childhood and the risk of islet autoimmunity and type 1 diabetes:the DIPP birth cohort study

Author

Hakola, L. (Leena), Vuorinen, A.-L. (Anna-Leena), Hanna‑Mari, H. (Hanna‑Mari), Niinistö, S. (Sari), Ahonen, S. (Suvi), Rautanen, J. (Jenna), Peltonen, E. J. (Essi J.), Nevalainen, J. (Jaakko), Ilonen, J. (Jorma), Toppari, J. (Jorma), Veijola, R. (Riitta), Knip, M. (Mikael), Virtanen, S. M. (Suvi M.), Hakola, L. (Leena), Vuorinen, A.-L. (Anna-Leena), Hanna‑Mari, H. (Hanna‑Mari), Niinistö, S. (Sari), Ahonen, S. (Suvi), Rautanen, J. (Jenna), Peltonen, E. J. (Essi J.), Nevalainen, J. (Jaakko), Ilonen, J. (Jorma), Toppari, J. (Jorma), Veijola, R. (Riitta), Knip, M. (Mikael), and Virtanen, S. M. (Suvi M.)

Abstract

Purpose: The aim was to study the associations between dietary intake of fatty acids in childhood and the risk of islet autoimmunity and type 1 diabetes (T1D). Methods: The prospective Finnish Type 1 Diabetes Prediction and Prevention (DIPP) Study included children with genetic susceptibility to T1D born between 1996 and 2004. Participants were followed up every 3 to 12 months up to 6 years for diet, islet autoantibodies, and T1D. Dietary intake of several fatty acids at the age of 3 months to 6 years was assessed 1–8 times per participant with a 3-day food record. Joint models adjusted for energy intake, sex, HLA genotype and familial diabetes were used to investigate the associations of longitudinal intake of fatty acids and the development of islet autoimmunity and T1D. Results: During the 6-year follow-up, 247 (4.4%) children of 5626 developed islet autoimmunity and 94 (1.7%) children of 5674 developed T1D. Higher intake of monounsaturated fatty acids (HR 0.63; 95% CI 0.47, 0.82), arachidonic acid (0.69; 0.50, 0.94), total n-3 fatty acids (0.64; 0.48, 0.84), and long-chain n-3 fatty acids (0.14; 0.04, 0.43), was associated with a decreased risk of islet autoimmunity with and without energy adjustment. Higher intake of total fat (0.73; 0.53, 0.98), and saturated fatty acids (0.55; 0.33, 0.90) was associated with a decreased risk of T1D only when energy adjusted. Conclusion: Intake of several fatty acids was associated with a decreased risk of islet autoimmunity or T1D among high-risk children. Our findings support the idea that dietary factors, including n-3 fatty acids, may play a role in the disease process of T1D.

Published
2023

4. Identification of monogenic variants in more than ten per cent of children without type 1 diabetes-related autoantibodies at diagnosis in the Finnish Pediatric Diabetes Register

Author

Harsunen, M. (Minna), Kettunen, J. L. (Jarno L. T.), Härkönen, T. (Taina), Dwivedi, O. (Om), Lehtovirta, M. (Mikko), Vähäsalo, P. (Paula), Veijola, R. (Riitta), Ilonen, J. (Jorma), Miettinen, P. J. (Päivi J.), Knip, M. (Mikael), Tuomi, T. (Tiinamaija), Harsunen, M. (Minna), Kettunen, J. L. (Jarno L. T.), Härkönen, T. (Taina), Dwivedi, O. (Om), Lehtovirta, M. (Mikko), Vähäsalo, P. (Paula), Veijola, R. (Riitta), Ilonen, J. (Jorma), Miettinen, P. J. (Päivi J.), Knip, M. (Mikael), and Tuomi, T. (Tiinamaija)

Abstract

Aims/hypothesis: Monogenic forms of diabetes (MODY, neonatal diabetes mellitus and syndromic forms) are rare, and affected individuals may be misclassified and treated suboptimally. The prevalence of type 1 diabetes is high in Finnish children but systematic screening for monogenic diabetes has not been conducted. We assessed the prevalence and clinical manifestations of monogenic diabetes in children initially registered with type 1 diabetes in the Finnish Pediatric Diabetes Register (FPDR) but who had no type 1 diabetes-related autoantibodies (AABs) or had only low-titre islet cell autoantibodies (ICAs) at diagnosis. Methods: The FPDR, covering approximately 90% of newly diagnosed diabetic individuals aged ≤15 years in Finland starting from 2002, includes data on diabetes-associated HLA genotypes and AAB data (ICA, and autoantibodies against insulin, GAD, islet antigen 2 and zinc transporter 8) at diagnosis. A next generation sequencing gene panel including 42 genes was used to identify monogenic diabetes. We interpreted the variants in HNF1A by using the gene-specific standardised criteria and reported pathogenic and likely pathogenic findings only. For other genes, we also reported variants of unknown significance if an individual’s phenotype suggested monogenic diabetes. Results: Out of 6482 participants, we sequenced DNA for 152 (2.3%) testing negative for all AABs and 49 (0.8%) positive only for low-titre ICAs (ICAlow). A monogenic form of diabetes was revealed in 19 (12.5%) of the AAB-negative patients (14 [9.2%] had pathogenic or likely pathogenic variants) and two (4.1%) of the ICAlow group. None had ketoacidosis at diagnosis or carried HLA genotypes conferring high risk for type 1 diabetes. The affected genes were GCK, HNF1A, HNF4A, HNF1B, INS, KCNJ11, RFX6, LMNA and WFS1. A switch from insulin to oral medication was successful in four of five patients with variants in HNF1A, HNF4A or KCNJ11.

Published
2023

5. Intake and sources of dietary fibre and dietary fibre fractions in Finnish children

Author

Salo, T. E. (Tuuli E. I.), Niinistö, S. (Sari), Korhonen, T. E. (Tuuli E.), Pastell, H. (Helena), Reinivuo, H. (Heli), Takkinen, H.-M. (Hanna-Mari), Ilonen, J. (Jorma), Toppari, J. (Jorma), Knip, M. (Mikael), Veijola, R. (Riitta), Virtanen, S. M. (Suvi M.), Salo, T. E. (Tuuli E. I.), Niinistö, S. (Sari), Korhonen, T. E. (Tuuli E.), Pastell, H. (Helena), Reinivuo, H. (Heli), Takkinen, H.-M. (Hanna-Mari), Ilonen, J. (Jorma), Toppari, J. (Jorma), Knip, M. (Mikael), Veijola, R. (Riitta), and Virtanen, S. M. (Suvi M.)

Abstract

The current definition of dietary fibre was adopted by the Codex Alimentarius Commission in 2009, but implementation requires updating food composition databases with values based on appropriate analysis methods. Previous data on population intakes of dietary fibre fractions are sparse. We studied the intake and sources of total dietary fibre (TDF) and dietary fibre fractions insoluble dietary fibre (IDF), dietary fibre soluble in water but insoluble in 76 % aqueous ethanol (SDFP) and dietary fibre soluble in water and soluble in 76 % aqueous ethanol (SDFS) in Finnish children based on new CODEX-compliant values of the Finnish National Food Composition Database Fineli. Our sample included 5193 children at increased genetic risk of type 1 diabetes from the Type 1 Diabetes Prediction and Prevention birth cohort, born between 1996 and 2004. We assessed the intake and sources based on 3-day food records collected at the ages of 6 months, 1, 3 and 6 years. Both absolute and energy-adjusted intakes of TDF were associated with age, sex and breast-feeding status of the child. Children of older parents, parents with a higher level of education, non-smoking mothers and children with no older siblings had higher energy-adjusted TDF intake. IDF was the major dietary fibre fraction in non-breastfed children, followed by SDFP and SDFS. Cereal products, fruits and berries, potatoes and vegetables were major food sources of dietary fibre. Breast milk was a major source of dietary fibre in 6-month-olds due to its human milk oligosaccharide content and resulted in high SDFS intakes in breastfed children.

Published
2023

6. What is the role of puberty in the development of islet autoimmunity and progression to type 1 diabetes?

Author

Peltonen, E. J. (Essi J.), Veijola, R. (Riitta), Ilonen, J. (Jorma), Knip, M. (Mikael), Niinikoski, H. (Harri), Toppari, J. (Jorma), Virtanen, H. E. (Helena E.), Virtanen, S. M. (Suvi M.), Peltonen, J. (Jaakko), Nevalainen, J. (Jaakko), Peltonen, E. J. (Essi J.), Veijola, R. (Riitta), Ilonen, J. (Jorma), Knip, M. (Mikael), Niinikoski, H. (Harri), Toppari, J. (Jorma), Virtanen, H. E. (Helena E.), Virtanen, S. M. (Suvi M.), Peltonen, J. (Jaakko), and Nevalainen, J. (Jaakko)

Abstract

In many populations, the peak period of incidence of type 1 diabetes (T1D) has been observed to be around 10–14 years of age, coinciding with puberty, but direct evidence of the role of puberty in the development of T1D is limited. We therefore aimed to investigate whether puberty and the timing of its onset are associated with the development of islet autoimmunity (IA) and subsequent progression to T1D. A Finnish population-based cohort of children with HLA-DQB1-conferred susceptibility to T1D was followed from 7 years of age until 15 years of age or until a diagnosis of T1D (n = 6920). T1D-associated autoantibodies and growth were measured at 3- to 12-month intervals, and pubertal onset timing was assessed based on growth. The analyses used a three-state survival model. IA was defined as being either positive for islet cell antibodies plus at least one biochemical autoantibody (ICA + 1) or as being repeatedly positive for at least one biochemical autoantibody (BC1). Depending on the IA definition, either 303 (4.4%, ICA + 1) or 435 (6.3%, BC1) children tested positive for IA by the age of 7 years, and 211 (3.2%, ICA + 1)) or 198 (5.3%, BC1) developed IA during follow-up. A total of 172 (2.5%) individuals developed T1D during follow-up, of whom 169 were positive for IA prior to the clinical diagnosis. Puberty was associated with an increase in the risk of progression to T1D, but only from ICA + 1-defined IA (hazard ratio 1.57; 95% confidence interval 1.14, 2.16), and the timing of pubertal onset did not affect the association. No association between puberty and the risk of IA was detected. In conclusion, puberty may affect the risk of progression but is not a risk factor for IA.

Published
2023

7. DNA methylation differences within INS, PTPN22 and IL2RA promoters in lymphocyte subsets in children with type 1 diabetes and controls

Author

Pahkuri, S. (Sirpa), Ekman, I. (Ilse), Vandamme, C. (Céline), Näntö-Salonen, K. (Kirsti), Toppari, J. (Jorma), Veijola, R. (Riitta), Knip, M. (Mikael), Kinnunen, T. (Tuure), Ilonen, J. (Jorma), Lempainen, J. (Johanna), Pahkuri, S. (Sirpa), Ekman, I. (Ilse), Vandamme, C. (Céline), Näntö-Salonen, K. (Kirsti), Toppari, J. (Jorma), Veijola, R. (Riitta), Knip, M. (Mikael), Kinnunen, T. (Tuure), Ilonen, J. (Jorma), and Lempainen, J. (Johanna)

Abstract

We elucidated the effect of four known T1D-susceptibility associated single nucleotide polymorphism (SNP) markers in three genes (rs12722495 and rs2104286 in IL2RA, rs689 in INS and rs2476601 in PTPN22) on CpG site methylation of their proximal promoters in different lymphocyte subsets using pyrosequencing. The study cohort comprised 25 children with newly diagnosed T1D and 25 matched healthy controls. The rs689 SNP was associated with methylation at four CpG sites in INS promoter: −234, −206, −102 and −69. At all four CpG sites, the susceptibility genotype AA was associated with a higher methylation level compared to the other genotypes. We also found an association between rs12722495 and methylation at CpG sites −373 and −356 in IL2RA promoter in B cells, where the risk genotype AA was associated with lower methylation level compared to the AG genotype. The other SNPs analyzed did not demonstrate significant associations with CpG site methylation in the examined genes. Additionally, we compared the methylation between children with T1D and controls, and found statistically significant methylation differences at CpG −135 in INS in CD8+ T cells (p = 0.034), where T1D patients had a slightly higher methylation compared to controls (87.3 ± 7.2 vs. 78.8 ± 8.9). At the other CpG sites analyzed, the methylation was similar. Our results not only confirm the association between INS methylation and rs689 discovered in earlier studies but also report this association in sorted immune cells. We also report an association between rs12722495 and IL2RA promoter methylation in B cells. These results suggest that at least part of the genetic effect of rs689 and rs12722495 on T1D pathogenesis may be conveyed by DNA methylation.

Published
2023

8. Circulating metabolic signatures of rapid and slow progression to type 1 diabetes in islet autoantibody-positive children

Author

Lamichhane, S. (Santosh), Sen, P. (Partho), Dickens, A. M. (Alex M.), Kråkström, M. (Matilda), Ilonen, J. (Jorma), Lempainen, J. (Johanna), Hyöty, H. (Heikki), Lahesmaa, R. (Riitta), Veijola, R. (Riitta), Toppari, J. (Jorma), Hyötyläinen, T. (Tuulia), Knip, M. (Mikael), Orešič, M. (Matej), Lamichhane, S. (Santosh), Sen, P. (Partho), Dickens, A. M. (Alex M.), Kråkström, M. (Matilda), Ilonen, J. (Jorma), Lempainen, J. (Johanna), Hyöty, H. (Heikki), Lahesmaa, R. (Riitta), Veijola, R. (Riitta), Toppari, J. (Jorma), Hyötyläinen, T. (Tuulia), Knip, M. (Mikael), and Orešič, M. (Matej)

Abstract

Aims/hypothesis: Appearance of multiple islet cell autoantibodies in early life is indicative of future progression to overt type 1 diabetes, however, at varying rates. Here, we aimed to study whether distinct metabolic patterns could be identified in rapid progressors (RP, disease manifestation within 18 months after the initial seroconversion to autoantibody positivity) vs. slow progressors (SP, disease manifestation at 60 months or later from the appearance of the first autoantibody). Methods: Longitudinal samples were collected from RP (n=25) and SP (n=41) groups at the ages of 3, 6, 12, 18, 24, or ≥ 36 months. We performed a comprehensive metabolomics study, analyzing both polar metabolites and lipids. The sample series included a total of 239 samples for lipidomics and 213 for polar metabolites. Results: We observed that metabolites mediated by gut microbiome, such as those involved in tryptophan metabolism, were the main discriminators between RP and SP. The study identified specific circulating molecules and pathways, including amino acid (threonine), sugar derivatives (hexose), and quinic acid that may define rapid vs. slow progression to type 1 diabetes. However, the circulating lipidome did not appear to play a major role in differentiating between RP and SP. Conclusion/interpretation: Our study suggests that a distinct metabolic profile is linked with the type 1 diabetes progression. The identification of specific metabolites and pathways that differentiate RP from SP may have implications for early intervention strategies to delay the development of type 1 diabetes.

Published
2023

9. Serum APOC1 levels are decreased in young autoantibody positive children who rapidly progress to type 1 diabetes

Author

Hirvonen, M. K. (M. Karoliina), Lietzén, N. (Niina), Moulder, R. (Robert), Bhosale, S. D. (Santosh D.), Koskenniemi, J. (Jaakko), Vähä-Mäkilä, M. (Mari), Nurmio, M. (Mirja), Orešič, M. (Matej), Ilonen, J. (Jorma), Toppari, J. (Jorma), Veijola, R. (Riitta), Hyöty, H. (Heikki), Lähdesmäki, H. (Harri), Knip, M. (Mikael), Cheng, L. (Lu), Lahesmaa, R. (Riitta), Hirvonen, M. K. (M. Karoliina), Lietzén, N. (Niina), Moulder, R. (Robert), Bhosale, S. D. (Santosh D.), Koskenniemi, J. (Jaakko), Vähä-Mäkilä, M. (Mari), Nurmio, M. (Mirja), Orešič, M. (Matej), Ilonen, J. (Jorma), Toppari, J. (Jorma), Veijola, R. (Riitta), Hyöty, H. (Heikki), Lähdesmäki, H. (Harri), Knip, M. (Mikael), Cheng, L. (Lu), and Lahesmaa, R. (Riitta)

Abstract

Better understanding of the early events in the development of type 1 diabetes is needed to improve prediction and monitoring of the disease progression during the substantially heterogeneous presymptomatic period of the beta cell damaging process. To address this concern, we used mass spectrometry-based proteomics to analyse longitudinal pre-onset plasma sample series from children positive for multiple islet autoantibodies who had rapidly progressed to type 1 diabetes before 4 years of age (n = 10) and compared these with similar measurements from matched children who were either positive for a single autoantibody (n = 10) or autoantibody negative (n = 10). Following statistical analysis of the longitudinal data, targeted serum proteomics was used to verify 11 proteins putatively associated with the disease development in a similar yet independent and larger cohort of children who progressed to the disease within 5 years of age (n = 31) and matched autoantibody negative children (n = 31). These data reiterated extensive age-related trends for protein levels in young children. Further, these analyses demonstrated that the serum levels of two peptides unique for apolipoprotein C1 (APOC1) were decreased after the appearance of the first islet autoantibody and remained relatively less abundant in children who progressed to type 1 diabetes, in comparison to autoantibody negative children.

Published
2023

11. Maternal diet during pregnancy and lactation and cow's milk allergy in offspring

Author

Tuokkola, J., Luukkainen, P., Tapanainen, H., Kaila, M., Vaarala, O., Kenward, M.G., Virta, L.J., Veijola, R., Simell, O., Ilonen, J., Knip, M., and Virtanen, S.M.

Subjects
Milk -- Health aspects, Infants -- Health aspects, Lactation, Pregnant women -- Food and nutrition, Food allergy -- Risk factors, Food/cooking/nutrition, Health
Abstract

BACKGROUND/OBJECTIVES: Diet during pregnancy and lactation may have a role in the development of allergic diseases. There are few human studies on the topic, especially focusing on food allergies. We sought to study the associations between maternal diet during pregnancy and lactation and cow's milk allergy (CMA) in offspring. SUBJECTS/METHODS: A population-based birth cohort with human leukocyte antigen-conferred susceptibility to type 1 diabetes was recruited in Finland between 1997 and 2004 (n = 6288). Maternal diet during pregnancy and lactation was assessed by a validated, 181item semi-quantitative food frequency questionnaire. Register-based information on diagnosed CMA was obtained from the Social Insurance Institution and completed with parental reports. The associations between maternal food consumption and CMA were assessed using logistic regression, comparing the highest and the lowest quarters to the middle half of consumption. RESULTS: Consumption of milk products in the highest quarter during pregnancy was associated with a lower risk of CMA in offspring (odds ratio (OR) 0.56, 95% confidence interval (CI) 0.37-0.86;P < 0.01). When stratified by maternal allergic rhinitis and asthma, there was evidence of an inverse association between high use of milk products and CMA in offspring of non-allergic mothers (OR 0.30, 95% CI 0.13-0.69, P < 0.001). Cord blood IgA correlated positively with the consumption of milk products during pregnancy, indicating exposure to CMA and activation of antigen-specific immunity in the infant during pregnancy. CONCLUSIONS: High maternal consumption of milk products during pregnancy may protect children from developing CMA, especially in offspring of non-allergic mothers. European Journal of Clinical Nutrition (2016) 70, 554-559; doi: 10.1038/ejcn.2015.223; published online 13 January 2016, INTRODUCTION Very little is known about dietary determinants of food allergies, but there is some evidence that early nutrition has a role in the development of other allergic diseases and [...]

Published
2016
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12. Object Evidence Extraction Using Simple Gabor Features and Statistical Ranking

Author

Kamarainen, J. -K., Ilonen, J., Paalanen, P., Hamouz, M., Kälviäinen, H., Kittler, J., Hutchison, David, editor, Kanade, Takeo, editor, Kittler, Josef, editor, Kleinberg, Jon M., editor, Mattern, Friedemann, editor, Mitchell, John C., editor, Naor, Moni, editor, Nierstrasz, Oscar, editor, Pandu Rangan, C., editor, Steffen, Bernhard, editor, Sudan, Madhu, editor, Terzopoulos, Demetri, editor, Tygar, Dough, editor, Vardi, Moshe Y., editor, Weikum, Gerhard, editor, Kalviainen, Heikki, editor, Parkkinen, Jussi, editor, and Kaarna, Arto, editor

Published
2005
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13. Toward Automatic Motor Condition Diagnosis

Author

Ilonen, J., Paalanen, P., Kamarainen, J. -K., Lindh, T., Ahola, J., Kälviäinen, H., Partanen, J., Hutchison, David, editor, Kanade, Takeo, editor, Kittler, Josef, editor, Kleinberg, Jon M., editor, Mattern, Friedemann, editor, Mitchell, John C., editor, Naor, Moni, editor, Nierstrasz, Oscar, editor, Pandu Rangan, C., editor, Steffen, Bernhard, editor, Sudan, Madhu, editor, Terzopoulos, Demetri, editor, Tygar, Dough, editor, Vardi, Moshe Y., editor, Weikum, Gerhard, editor, Kalviainen, Heikki, editor, Parkkinen, Jussi, editor, and Kaarna, Arto, editor

Published
2005
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15. First-emerging islet autoantibody and glucose metabolism:search for type 1 diabetes subtypes

Author

Helminen, O. (Olli), Pokka, T. (Tytti), Aspholm, S. (Susanna), Ilonen, J. (Jorma), Simell, O. G. (Olli G), Knip, M. (Mikael), Veijola, R. (Riitta), Helminen, O. (Olli), Pokka, T. (Tytti), Aspholm, S. (Susanna), Ilonen, J. (Jorma), Simell, O. G. (Olli G), Knip, M. (Mikael), and Veijola, R. (Riitta)

Abstract

Objectives: Subtypes in type 1 diabetes pathogenesis have been implicated based on the first-appearing autoantibody (primary autoantibody). We set out to describe the glucose metabolism in preclinical diabetes in relation to the primary autoantibody in children with HLA-conferred disease susceptibility. Design and methods: Dysglycemic markers are defined as a 10% increase in HbA1c in a 3–12 months interval or HbA1c ≥5.9% (41 mmol/mol) in two consecutive samples, impaired fasting glucose or impaired glucose tolerance, or a random plasma glucose value ≥7.8 mmol/L. A primary autoantibody could be detected in 295 children who later developed at least 1 additional biochemical autoantibody. These children were divided into three groups: insulin autoantibody (IAA) multiple (n = 143), GAD antibody (GADA) multiple (n = 126) and islet antigen 2 antibody (IA-2A) multiple (n = 26). Another 229 children seroconverted to positivity only for a single biochemical autoantibody and were grouped as IAA only (n = 87), GADA only (n = 114) and IA-2A only (n = 28). Results: No consistent differences were observed in selected autoantibody groups during the preclinical period. At diagnosis, children with IAA only showed the highest HbA1c (P < 0.001 between groups) and the highest random plasma glucose (P = 0.005 between groups). Children with IA-2A only progressed to type 1 diabetes as frequently as those with IA-2A multiple (46% vs 54%, P = 0.297) whereas those with IAA only or GADA only progressed less often than children with IAA multiple or GADA multiple (22% vs 62% (P < 0.001) and 7% vs 43% (P < 0.001)), respectively. Conclusions: The phenotype of preclinical diabetes defined by the primary autoantibody is not associated with any discernible differences in glucose metabolism before the clinical disease manifestation.

Published
2022

16. Torque teno virus primary infection kinetics in early childhood

Author

Väisänen, E. (Elina), Kuisma, I. (Inka), Mäkinen, M. (Marjaana), Ilonen, J. (Jorma), Veijola, R. (Riitta), Toppari, J. (Jorma), Hedman, K. (Klaus), Söderlund-Venermo, M. (Maria), Väisänen, E. (Elina), Kuisma, I. (Inka), Mäkinen, M. (Marjaana), Ilonen, J. (Jorma), Veijola, R. (Riitta), Toppari, J. (Jorma), Hedman, K. (Klaus), and Söderlund-Venermo, M. (Maria)

Abstract

Human torque teno viruses (TTVs) are a diverse group of small nonenveloped viruses with circular, single-stranded DNA genomes. These elusive anelloviruses are harbored in the blood stream of most humans and have thus been considered part of the normal flora. Whether the primary infection as a rule take(s) place before or after birth has been debated. The aim of our study was to determine the time of TTV primary infection and the viral load and strain variations during infancy and follow-up for up to 7 years. TTV DNAs were quantified in serial serum samples from 102 children by a pan-TTV quantitative PCR, and the amplicons from representative time points were cloned and sequenced to disclose the TTV strain diversity. We detected an unequivocal rise in TTV-DNA prevalence, from 39% at 4 months of age to 93% at 2 years; all children but one, 99%, became TTV-DNA positive before age 4 years. The TTV-DNA quantities ranged from 5 × 101 to 4 × 107 copies/mL, both within and between the children. In conclusion, TTV primary infections occur mainly after birth, and increase during the first two years with high intra- and interindividual variation in both DNA quantities and virus strains.

Published
2022

17. Early glucose metabolism in children at risk for type 1 diabetes based on islet autoantibodies compared to low-risk control groups

Author

Helminen, O. (Olli), Pokka, T. (Tytti), Aspholm, S. (Susanna), Ilonen, J. (Jorma), Simell, O. (Olli), Knip, M. (Mikael), Veijola, R. (Riitta), Helminen, O. (Olli), Pokka, T. (Tytti), Aspholm, S. (Susanna), Ilonen, J. (Jorma), Simell, O. (Olli), Knip, M. (Mikael), and Veijola, R. (Riitta)

Abstract

Background: Anatomic variation or early differences in glucose metabolism have been linked to the development of type 1 diabetes. We aimed to describe early glucose metabolism based on HbA1c, oral glucose tolerance test (OGTT), and random plasma glucose years before the presentation of type 1 diabetes in five risk groups based on autoantibody combinations. For the first time, we were able to include for comparison children with very low risk of progression to type 1 diabetes. Methods: The Finnish Diabetes Prediction and Prevention birth cohort study screened newborn infants for HLA susceptibility to type 1 diabetes since 1994. Those carrying a risk genotype were prospectively followed up with islet autoantibody testing. Glucose parameters were obtained starting from the time of seroconversion. By 31 August 2014, 1162 children had developed at least one islet autoantibody and were included in the current study. Type 1 diabetes was diagnosed in 335 children (progressors). In the non-progressor groups, 207 developed multiple (≥2) biochemical islet autoantibodies, 229 a single biochemical autoantibody, 370 ICA only, and 64 transient autoantibodies. Children were divided into five risk groups. Glucose metabolism was evaluated. Results: We observed lower HbA1c values in early follow-up 4.5 to 6.0 years before diagnosis in the progressors when compared to the same time in children with a single biochemical autoantibody or low-risk (ICA only and transient) participants, who did not progress to clinical type 1 diabetes. However, no such differences were observed in OGTTs or random plasma glucose. The variation was minimal in glucose values in the low-risk groups. Conclusion: We report the possibility of early alteration in glucose metabolism in future progressors. This could suggest early defects in multiple glucose-regulating hormones.

Published
2022

18. Umbilical cord blood DNA methylation in children who later develop type 1 diabetes

Author

Laajala, E. (Essi), Kalim, U. U. (Ubaid Ullah), Grönroos, T. (Toni), Rasool, O. (Omid), Halla-aho, V. (Viivi), Konki, M. (Mikko), Kattelus, R. (Roosa), Mykkänen, J. (Juha), Nurmio, M. (Mirja), Vähä-Mäkilä, M. (Mari), Kallionpää, H. (Henna), Lietzén, N. (Niina), Ghimire, B. R. (Bishwa R.), Laiho, A. (Asta), Hyöty, H. (Heikki), Elo, L. L. (Laura L.), Ilonen, J. (Jorma), Knip, M. (Mikael), Lund, R. J. (Riikka J.), Orešič, M. (Matej), Veijola, R. (Riitta), Lähdesmäki, H. (Harri), Toppari, J. (Jorma), Lahesmaa, R. (Riitta), Laajala, E. (Essi), Kalim, U. U. (Ubaid Ullah), Grönroos, T. (Toni), Rasool, O. (Omid), Halla-aho, V. (Viivi), Konki, M. (Mikko), Kattelus, R. (Roosa), Mykkänen, J. (Juha), Nurmio, M. (Mirja), Vähä-Mäkilä, M. (Mari), Kallionpää, H. (Henna), Lietzén, N. (Niina), Ghimire, B. R. (Bishwa R.), Laiho, A. (Asta), Hyöty, H. (Heikki), Elo, L. L. (Laura L.), Ilonen, J. (Jorma), Knip, M. (Mikael), Lund, R. J. (Riikka J.), Orešič, M. (Matej), Veijola, R. (Riitta), Lähdesmäki, H. (Harri), Toppari, J. (Jorma), and Lahesmaa, R. (Riitta)

Abstract

Aims/hypothesis: Distinct DNA methylation patterns have recently been observed to precede type 1 diabetes in whole blood collected from young children. Our aim was to determine whether perinatal DNA methylation is associated with later progression to type 1 diabetes. Methods: Reduced representation bisulphite sequencing (RRBS) analysis was performed on umbilical cord blood samples collected within the Finnish Type 1 Diabetes Prediction and Prevention (DIPP) Study. Children later diagnosed with type 1 diabetes and/or who tested positive for multiple islet autoantibodies (n = 43) were compared with control individuals (n = 79) who remained autoantibody-negative throughout the DIPP follow-up until 15 years of age. Potential confounding factors related to the pregnancy and the mother were included in the analysis. Results: No differences in the umbilical cord blood methylation patterns were observed between the cases and controls at a false discovery rate <0.05. Conclusions/interpretation: Based on our results, differences between children who progress to type 1 diabetes and those who remain healthy throughout childhood are not yet present in the perinatal DNA methylome. However, we cannot exclude the possibility that such differences would be found in a larger dataset.

Published
2022

19. Heterogeneity in the presentation of clinical type 1 diabetes defined by the level of risk conferred by human leukocyte antigen class II genotypes

Author

Taka, A.-M. (Antti-Mathias), Härkönen, T. (Taina), Vähäsalo, P. (Paula), Lempainen, J. (Johanna), Veijola, R. (Riitta), Ilonen, J. (Jorma), Knip, M. (Mikael), t. F. (the Finnish Pediatric Diabetes Register), Taka, A.-M. (Antti-Mathias), Härkönen, T. (Taina), Vähäsalo, P. (Paula), Lempainen, J. (Johanna), Veijola, R. (Riitta), Ilonen, J. (Jorma), Knip, M. (Mikael), and t. F. (the Finnish Pediatric Diabetes Register)

Abstract

Objectives: The association between human leukocyte antigen (HLA) class II genotypes and susceptibility to type 1 diabetes (T1D) is well established. This study aimed at examining whether there are differences in the presentation of T1D depending on the HLA genotype. Research Design and Methods: We divided the study participants (N = 5798) in the Finnish Pediatric Diabetes Register into two groups based on the T1D risk conferred by their HLA genotype (high and moderate-risk genotypes, Group 1 vs. other genotypes, Group 2). We then examined differences in clinical, metabolic, and immunological characteristics. Children included in the study were 0–14-year-old and diagnosed between January 2003 and December 2019. Results: Participants in Group 1 were younger at the time of diagnosis (P < 0.001) and had more frequently family members affected by T1D (P < 0.001). Diabetic ketoacidosis (DKA) was more frequent among participants in Group 2 (P = 0.014) who also had a longer duration of symptoms before diagnosis (P < 0.001) and higher hemoglobin A1c (P = 0.001) at diagnosis. The HLA genotype was not, however, directly related to the DKA frequency. The frequency of islet cell antibodies (P < 0.003), insulin autoantibodies (P < 0.001), and islet antigen 2 autoantibodies (P < 0.001) was higher in Group 1 whereas glutamic acid decarboxylase autoantibodies were more frequent (P < 0.001) in Group 2. Group 1 had more participants with multiple autoantibodies (P = 0.027) whereas antibody negativity was more frequent in Group 2 (P = 0.003). Conclusions: These findings indicate disease heterogeneity in relation to both clinical disease presentation and humoral autoimmunity, in particular. This heterogeneity is, at least partly, defined by HLA Class II genotypes.

Published
2022

20. Detection of enterovirus RNA in peripheral blood mononuclear cells correlates with the presence of the predisposing allele of the type 1 diabetes risk gene IFIH1 and with disease stage

Author

Sioofy-Khojine, A.-B. (Amir-Babak), Richardson, S. J. (Sarah J.), Locke, J. M. (Jonathan M.), Oikarinen, S. (Sami), Nurminen, N. (Noora), Laine, A.-P. (Antti-Pekka), Downes, K. (Kate), Lempainen, J. (Johanna), Todd, J. A. (John A.), Veijola, R. (Riitta), Ilonen, J. (Jorma), Knip, M. (Mikael), Morgan, N. G. (Noel G.), Hyöty, H. (Heikki), Peakman, M. (Mark), Eichmann, M. (Martin), Sioofy-Khojine, A.-B. (Amir-Babak), Richardson, S. J. (Sarah J.), Locke, J. M. (Jonathan M.), Oikarinen, S. (Sami), Nurminen, N. (Noora), Laine, A.-P. (Antti-Pekka), Downes, K. (Kate), Lempainen, J. (Johanna), Todd, J. A. (John A.), Veijola, R. (Riitta), Ilonen, J. (Jorma), Knip, M. (Mikael), Morgan, N. G. (Noel G.), Hyöty, H. (Heikki), Peakman, M. (Mark), and Eichmann, M. (Martin)

Abstract

Aims/hypothesis: Enteroviral infection has been implicated consistently as a key environmental factor correlating with the appearance of autoimmunity and/or the presence of overt type 1 diabetes, in which pancreatic insulin-producing beta cells are destroyed by an autoimmune response. Genetic predisposition through variation in the type 1 diabetes risk gene IFIH1 (interferon induced with helicase C domain 1), which encodes the viral pattern-recognition receptor melanoma differentiation-associated protein 5 (MDA5), supports a potential link between enterovirus infection and type 1 diabetes. Methods: We used molecular techniques to detect enterovirus RNA in peripheral blood samples (in separated cellular compartments or plasma) from two cohorts comprising 79 children or 72 adults that include individuals with and without type 1 diabetes who had multiple autoantibodies. We also used immunohistochemistry to detect the enteroviral protein VP1 in the pancreatic islets of post-mortem donors (n=43) with type 1 diabetes. Results: We observed enhanced detection sensitivity when sampling the cellular compartment compared with the non-cellular compartment of peripheral blood (OR 21.69; 95% CI 3.64, 229.20; p<0.0001). In addition, we show that children with autoimmunity are more likely to test positive for enterovirus RNA than those without autoimmunity (OR 11.60; 95% CI 1.89, 126.90; p=0.0065). Furthermore, we found that individuals carrying the predisposing allele (946Thr) of the common variant in IFIH1 (rs1990760, Thr946Ala) are more likely to test positive for enterovirus in peripheral blood (OR 3.07; 95% CI 1.02, 8.58; p=0.045). In contrast, using immunohistochemistry, there was no correlation between the common variant in IFIH1 and detection of enteroviral VP1 protein in the pancreatic islets of donors with type 1 diabetes. Conclusions/interpretation: Our data indicate that, in peripheral blood, antigen-presenting cells are the predominant source of enterovirus

Published
2022

21. Autoantibodies to N-terminally truncated GAD₆₅(96‐585):HLA associations and predictive value for type 1 diabetes

Author

Pöllänen, P. M. (Petra M.), Härkönen, T. (Taina), Ilonen, J. (Jorma), Toppari, J. (Jorma), Veijola, R. (Riitta), Siljander, H. (Heli), Knip, M. (Mikael), Pöllänen, P. M. (Petra M.), Härkönen, T. (Taina), Ilonen, J. (Jorma), Toppari, J. (Jorma), Veijola, R. (Riitta), Siljander, H. (Heli), and Knip, M. (Mikael)

Abstract

Objective: To evaluate the role of autoantibodies to N-terminally truncated glutamic acid decarboxylase GAD₆₅(96‐585) (t-GADA) as a marker for type 1 diabetes (T1D) and to assess the potential human leukocyte antigen (HLA) associations with such autoantibodies. Methods: In this cross-sectional study combining data from the Finnish Pediatric Diabetes Register, the Type 1 Diabetes Prediction and Prevention study, the DIABIMMUNE study, and the Early Dietary Intervention and Later Signs of Beta-Cell Autoimmunity study, venous blood samples from 760 individuals (53.7% males) were analyzed for t-GADA, autoantibodies to full-length GAD65 (f-GADA), and islet cell antibodies. Epitope-specific GAD autoantibodies were analyzed from 189 study participants. Results: T1D had been diagnosed in 174 (23%) participants. Altogether 631 (83%) individuals tested positive for f-GADA and 451 (59%) for t-GADA at a median age of 9.0 (range 0.2‐61.5) years. t-GADA demonstrated higher specificity (46%) and positive predictive value (30%) for T1D than positivity for f-GADA alone (15% and 21%, respectively). Among participants positive for f-GADA, those who tested positive for t-GADA carried more frequently HLA genotypes conferring increased risk for T1D than those who tested negative for t-GADA (77% vs 53%; P < 0.001). Conclusions: Autoantibodies to N-terminally truncated GAD improve the screening for T1D compared to f-GADA and may facilitate the selection of participants for clinical trials. HLA class II-mediated antigen presentation of GAD(96‐585)-derived or structurally similar peptides might comprise an important pathomechanism in T1D.

Published
2022

22. Consumption of differently processed milk products and the risk of asthma in children

Author

Koivusaari, K. (Katariina), Syrjälä, E. (Essi), Niinistö, S. (Sari), Ahonen, S. (Suvi), Åkerlund, M. (Mari), Korhonen, T. E. (Tuuli E.), Toppari, J. (Jorma), Ilonen, J. (Jorma), Kaila, M. (Minna), Knip, M. (Mikael), Alatossava, T. (Tapani), Veijola, R. (Riitta), Virtanen, S. M. (Suvi M.), Koivusaari, K. (Katariina), Syrjälä, E. (Essi), Niinistö, S. (Sari), Ahonen, S. (Suvi), Åkerlund, M. (Mari), Korhonen, T. E. (Tuuli E.), Toppari, J. (Jorma), Ilonen, J. (Jorma), Kaila, M. (Minna), Knip, M. (Mikael), Alatossava, T. (Tapani), Veijola, R. (Riitta), and Virtanen, S. M. (Suvi M.)

Abstract

Background: Consumption of unprocessed cow’s milk has been associated with a lower risk of childhood asthma and/or atopy. Not much is known about differently processed milk products. We aimed to study the association between the consumption of differently processed milk products and asthma risk in a Finnish birth cohort. Methods: We included 3053 children from the Finnish Type 1 Diabetes Prediction and Prevention (DIPP) Nutrition Study. Asthma and its subtypes were assessed at the age of 5 years, and food consumption by food records, at the age of 3 and 6 months and 1, 2, 3, 4, and 5 years. We used conventional and processing (heat treatment and homogenization)-based classifications for milk products. The data were analyzed using a joint model for longitudinal and time-to-event data. Results: At the age of 5 years, 184 (6.0%) children had asthma, of whom 101 (54.9%) were atopic, 75 (40.8%) were nonatopic, and eight (4.3%) could not be categorized. Consumption of infant formulas [adjusted hazard ratio (95% confidence intervals) 1.15 (1.07, 1.23), p < 0.001] and strongly heat-treated milk products [1.06 (1.01, 1.10), p = 0.01] was associated with the risk of all asthma. Consumption of all cow’s milk products [1.09 (1.03, 1.15), p = 0.003], nonfermented milk products [1.08 (1.02, 1.14), p = 0.008], infant formulas [1.23 (1.13, 1.34), p < 0.001], and strongly heat-treated milk products [1.08 (1.02, 1.15), p = 0.006] was associated with nonatopic asthma risk. All these associations remained statistically significant after multiple testing correction. Conclusions: High consumption of infant formula and other strongly heat-treated milk products may be associated with the development of asthma.

Published
2022

25. Non-HLA gene polymorphisms in the pathogenesis of type 1 diabetes:phase and endotype specific effects

Author

Laine, A.-P. (Antti-Pekka), Valta, M. (Milla), Toppari, J. (Jorma), Knip, M. (Mikael), Veijola, R. (Riitta), Ilonen, J. (Jorma), and Lempainen, J. (Johanna)

Subjects
autoantibodies, type 1 diabetes, follow-up-cohort, seroconversion, survival analysis
Abstract

The non-HLA loci conferring susceptibility to type 1 diabetes determine approximately half of the genetic disease risk, and several of them have been shown to affect immune-cell or pancreatic β-cell functions. A number of these loci have shown associations with the appearance of autoantibodies or with progression from seroconversion to clinical type 1 diabetes. In the current study, we have re-analyzed 21 of our loci with prior association evidence using an expanded DIPP follow-up cohort of 976 autoantibody positive cases and 1,910 matched controls. Survival analysis using Cox regression was applied for time periods from birth to seroconversion and from seroconversion to type 1 diabetes. The appearance of autoantibodies was also analyzed in endotypes, which are defined by the first appearing autoantibody, either IAA or GADA. Analyzing the time period from birth to seroconversion, we were able to replicate our previous association findings at PTPN22, INS, and NRP1. Novel findings included associations with ERBB3, UBASH3A, PTPN2, and FUT2. In the time period from seroconversion to clinical type 1 diabetes, prior associations with PTPN2, CD226, and PTPN22 were replicated, and a novel association with STAT4 was observed. Analyzing the appearance of autoantibodies in endotypes, the PTPN22 association was specific for IAA-first. In the progression phase, STAT4 was specific for IAA-first and ERBB3 to GADA-first. In conclusion, our results further the knowledge of the function of non-HLA risk polymorphisms in detailing endotype specificity and timing of disease development.

Published
2022

26. Determining the timing of pubertal onset via a multicohort analysis of growth

Author

Syrjälä, E. (Essi), Niinikoski, H. (Harri), Virtanen, H. E. (Helena E.), Ilonen, J. (Jorma), Knip, M. (Mikael), Hutri-Kähönen, N. (Nina), Pahkala, K. (Katja), Raitakari, O. T. (Olli T.), Rodprasert, W. (Wiwat), Toppari, J. (Jorma), Virtanen, S. M. (Suvi M.), Veijola, R. (Riitta), Peltonen, J. (Jaakko), Nevalainen, J. (Jaakko), Tampere University, Health Sciences, Department of Paediatrics, Clinical Medicine, Pediatrics, Computing Sciences, HUS Children and Adolescents, Doctoral Programme in Clinical Research, Children's Hospital, and CAMM - Research Program for Clinical and Molecular Metabolism

Subjects
Male, Physiology, Growth, Adolescents, Cohort Studies, Families, Endocrinology, Medical Conditions, Risk Factors, 3123 Gynaecology and paediatrics, Medicine and Health Sciences, Breast, Age of Onset, Child, Children, 112 Statistics and probability, Finland, Biological Phenomena, Men, 3142 Public health care science, environmental and occupational health, Physiological Parameters, Research Design, Medicine, Female, Infants, Research Article, Childhood Obesity, Adolescent, Endocrine Disorders, Science, Research and Analysis Methods, Diabetes Mellitus, Humans, Women, Genitalia, Obesity, Endocrine Physiology, Puberty, Body Weight, Biology and Life Sciences, Models, Theoretical, Overweight, Body Height, 3141 Health care science, Age Groups, Metabolic Disorders, People and Places, Population Groupings, Forecasting
Abstract

Objective Growth-based determination of pubertal onset timing would be cheap and practical. We aimed to determine this timing based on pubertal growth markers. Secondary aims were to estimate the differences in growth between cohorts and identify the role of overweight in onset timing. Design This multicohort study includes data from three Finnish cohorts—the Type 1 Diabetes Prediction and Prevention (DIPP, N = 2,825) Study, the Special Turku Coronary Risk Factor Intervention Project (STRIP, N = 711), and the Boy cohort (N = 66). Children were monitored for growth and Tanner staging (except in DIPP). Methods The growth data were analyzed using a Super-Imposition by Translation And Rotation growth curve model, and pubertal onset analyses were run using a time-to-pubertal onset model. Results The time-to-pubertal onset model used age at peak height velocity (aPHV), peak height velocity (PHV), and overweight status as covariates, with interaction between aPHV and overweight status for girls, and succeeded in determining the onset timing. Cross-validation showed a good agreement (71.0% for girls, 77.0% for boys) between the observed and predicted onset timings. Children in STRIP were taller overall (girls: 1.7 [95% CI: 0.9, 2.5] cm, boys: 1.0 [0.3, 2.2] cm) and had higher PHV values (girls: 0.13 [0.02, 0.25] cm/year, boys: 0.35 [0.21, 0.49] cm/year) than those in DIPP. Boys in the Boy cohort were taller (2.3 [0.3, 4.2] cm) compared with DIPP. Overweight girls showed pubertal onset at 1.0 [0.7, 1.4] year earlier compared with other girls. In boys, there was no such difference. Conclusions The novel modeling approach provides an opportunity to evaluate the Tanner breast/genital stage–based pubertal onset timing in cohort studies including longitudinal data on growth but lacking pubertal follow-up.

Published
2021

27. Maternal antioxidant intake during pregnancy and the development of cows’ milk allergy in the offspring

Author

Tuokkola, J. (Jetta), Lamminsalo, A. (Anni), Metsälä, J. (Johanna), Takkinen, H.-M. (Hanna-Mari), Tapanainen, H. (Heli), Åkerlund, M. (Mari), Niinistö, S. (Sari), Toppari, J. (Jorma), Ilonen, J. (Jorma), Veijola, R. (Riitta), Knip, M. (Mikael), Kaila, M. (Minna), Virtanen, S. M. (Suvi M), Tuokkola, J. (Jetta), Lamminsalo, A. (Anni), Metsälä, J. (Johanna), Takkinen, H.-M. (Hanna-Mari), Tapanainen, H. (Heli), Åkerlund, M. (Mari), Niinistö, S. (Sari), Toppari, J. (Jorma), Ilonen, J. (Jorma), Veijola, R. (Riitta), Knip, M. (Mikael), Kaila, M. (Minna), and Virtanen, S. M. (Suvi M)

Abstract

Cows’ milk allergy (CMA) is the most common food allergy in young children, and it is often the first manifestation of atopic diseases. Accordingly, very early environmental factors, such as maternal diet during pregnancy, may play a role in the development of CMA, but the evidence is limited. The aim of this study was to investigate the association between maternal intake of antioxidant nutrients during pregnancy and the subsequent development of CMA in the offspring in a prospective, population-based birth cohort within the Finnish Type 1 Diabetes Prediction and Prevention Study. Maternal dietary information during pregnancy was collected with a detailed, validated FFQ. The maternal dietary information and the information on putative confounding factors were available for 4403 children. Information on diagnosed CMA (n 448) was obtained from a medical registry and queried from the parents up to child’s age of 3 years. The Finnish food composition database was used to calculate the average daily intake of nutrients. Logistic regression was applied for statistical analyses, and the nutrient intakes were adjusted for energy intake. OR are presented per 1 sd increment of the particular nutrient intake. Maternal total and dietary intake of β-carotene was associated with an increased risk of CMA in the offspring when adjusted for the putative confounding factors (total OR 1·10, 95 % CI 1·02, 1·20; dietary OR 1·10; 95 % CI 1·01, 1·19). Using dietary supplements containing antioxidants in addition to a balanced diet may not confer any additional benefits.

Published
2021

28. Association of different enteroviruses with atopy and allergic diseases in early childhood

Author

Palmu, T. (Tiina), Lehtonen, J. (Jussi), Korhonen, L. (Laura), Virtanen, S. M. (Suvi M.), Niemelä, O. (Onni), Toppari, J. (Jorma), Ilonen, J. (Jorma), Veijola, R. (Riitta), Knip, M. (Mikael), Laitinen, O. H. (Olli H.), Lönnrot, M. (Maria), Hyöty, H. (Heikki), Palmu, T. (Tiina), Lehtonen, J. (Jussi), Korhonen, L. (Laura), Virtanen, S. M. (Suvi M.), Niemelä, O. (Onni), Toppari, J. (Jorma), Ilonen, J. (Jorma), Veijola, R. (Riitta), Knip, M. (Mikael), Laitinen, O. H. (Olli H.), Lönnrot, M. (Maria), and Hyöty, H. (Heikki)

Abstract

Background: Enterovirus (EV) infections, being among the most prevalent viruses worldwide, have been associated with reduced risk of allergic diseases. We sought to determine the association between EVs and allergic sensitization and disease in early childhood. Methods: The study was carried out in a nested case-control setting within a prospective birth cohort in Finland. We included 138 case children who had specific IgE (s-IgE) sensitization at the age of 5 years and 138 control children without s-IgE sensitization. Allergic disease was recorded at study visits and identified with the ISAAC questionnaire. We screened for the presence of serotype-specific antibodies against 41 EVs at 1–5 years of age and assessed their association with allergic sensitization and disease. Results: The overall number of EV infections did not differ between s-IgE–sensitized children and non-sensitized control children. However, there was a tendency of case children with an allergic disease having less EV infections than their controls. This observation was statistically significant for species A EVs in case children with atopic dermatitis vs. control children: OR 0.6 (95% CI 0.36–0.99), p = .048. Conclusion: This study supports the evidence that EV exposure and development of allergic disease are inversely associated. Interestingly, the inverse association was not observed for bare atopic IgE sensitization, but for IgE sensitization coupled with clinical atopic disease. This suggests that environmental factors influencing IgE sensitization may differ from those influencing progression to clinical allergic disease.

Published
2021

29. Frailty modeling under a selective sampling protocol:an application to type 1 diabetes related autoantibodies

Author

Nevalainen, J. (Jaakko), Datta, S. (Somnath), Toppari, J. (Jorma), Ilonen, J. (Jorma), Hyöty, H. (Heikki), Veijola, R. (Riitta), Knip, M. (Mikael), Virtanen, S. M. (Suvi M.), Nevalainen, J. (Jaakko), Datta, S. (Somnath), Toppari, J. (Jorma), Ilonen, J. (Jorma), Hyöty, H. (Heikki), Veijola, R. (Riitta), Knip, M. (Mikael), and Virtanen, S. M. (Suvi M.)

Abstract

In studies following selective sampling protocols for secondary outcomes, conventional analyses regarding their appearance could provide misguided information. In the large type 1 diabetes prevention and prediction (DIPP) cohort study monitoring type 1 diabetes-associated autoantibodies, we propose to model their appearance via a multivariate frailty model, which incorporates a correlation component that is important for unbiased estimation of the baseline hazards under the selective sampling mechanism. As further advantages, the frailty model allows for systematic evaluation of the association and the differences in regression parameters among the autoantibodies. We demonstrate the properties of the model by a simulation study and the analysis of the autoantibodies and their association with background factors in the DIPP study, in which we found that high genetic risk is associated with the appearance of all the autoantibodies, whereas the association with sex and urban municipality was evident for IA-2A and IAA autoantibodies.

Published
2021

30. Tri-SNP polymorphism in the intron of HLA-DRA1 affects type 1 diabetes susceptibility in the Finnish population

Author

Nygård, L. (Lucas), Laine, A.-P. (Antti-Pekka), Kiviniemi, M. (Minna), Toppari, J. (Jorma), Härkönen, T. (Taina), Knip, M. (Mikael), Veijola, R. (Riitta), Lempainen, J. (Johanna), Ilonen, J. (Jorma), Nygård, L. (Lucas), Laine, A.-P. (Antti-Pekka), Kiviniemi, M. (Minna), Toppari, J. (Jorma), Härkönen, T. (Taina), Knip, M. (Mikael), Veijola, R. (Riitta), Lempainen, J. (Johanna), and Ilonen, J. (Jorma)

Abstract

Genes in the HLA class II region include the most important inherited risk factors for type 1 diabetes (T1D) although also polymorphisms outside the HLA region modulate the predisposition to T1D. This study set out to confirm a recent observation in which a novel expression quantitative trait locus was formed by three single nucleotide polymorphisms (SNP) in the intron of HLA-DRA1 in DR3-DQ2 haplotypes. The SNPs significantly increased the risk for T1D in DR3-DQ2 homozygous individuals and we intended to further explore this association, in the Finnish population, by comparing two DR3-DQ2 positive genotypes. Cohorts with DR3-DQ2/DR3-DQ2 (N = 570) and DR3-DQ2/DR1-DQ5 (N = 1035) genotypes were studied using TaqMan analysis that typed for rs3135394, rs9268645 and rs3129877. The tri-SNP haplotype was significantly more common in cases than controls in the DR3-DQ2/DR3-DQ2 cohort (OR = 1.70 CI 95% = 1.15–2.51P = 0.007). However, no significant associations could be observed in the DR3-DQ2/DR1-DQ5 cohort.

Published
2021

31. Maternal vitamin C and iron intake during pregnancy and the risk of islet autoimmunity and type 1 diabetes in children:a birth cohort study

Author

Mattila, M. (Markus), Hakola, L. (Leena), Niinistö, S. (Sari), Tapanainen, H. (Heli), Takkinen, H.-M. (Hanna-Mari), Ahonen, S. (Suvi), Ilonen, J. (Jorma), Toppari, J. (Jorma), Veijola, R. (Riitta), Knip, M. (Mikael), Virtanen, S. M. (Suvi M.), Mattila, M. (Markus), Hakola, L. (Leena), Niinistö, S. (Sari), Tapanainen, H. (Heli), Takkinen, H.-M. (Hanna-Mari), Ahonen, S. (Suvi), Ilonen, J. (Jorma), Toppari, J. (Jorma), Veijola, R. (Riitta), Knip, M. (Mikael), and Virtanen, S. M. (Suvi M.)

Abstract

Our aim was to study the associations between maternal vitamin C and iron intake during pregnancy and the offspring’s risk of developing islet autoimmunity and type 1 diabetes. The study was a part of the Finnish Type 1 Diabetes Prediction and Prevention (DIPP) prospective birth cohort including children genetically at risk of type 1 diabetes born between 1997–2004. The diets of 4879 mothers in late pregnancy were assessed with a validated food frequency questionnaire. The outcomes were islet autoimmunity and type 1 diabetes. Cox proportional hazards regression analysis adjusted for energy, family history of diabetes, human leukocyte antigen (HLA) genotype and sex was used for statistical analyses. Total intake of vitamin C or iron from food and supplements was not associated with the risk of islet autoimmunity (vitamin C: HR 0.91: 95% CI (0.80, 1.03), iron: 0.98 (0.87, 1.10)) or type 1 diabetes (vitamin C: 1.01 (0.87, 1.17), iron: 0.92 (0.78, 1.08)), neither was the use of vitamin C or iron supplements associated with the outcomes. In conclusion, no association was found between maternal vitamin C or iron intake during pregnancy and the risk of islet autoimmunity or type 1 diabetes in the offspring.

Published
2021

32. Enterovirus infections are associated with the development of celiac disease in a birth cohort study

Author

Oikarinen, M. (Maarit), Puustinen, L. (Leena), Lehtonen, J. (Jussi), Hakola, L. (Leena), Simell, S. (Satu), Toppari, J. (Jorma), Ilonen, J. (Jorma), Veijola, R. (Riitta), Virtanen, S. M. (Suvi M.), Knip, M. (Mikae), Hyöty, H. (Heikki), Oikarinen, M. (Maarit), Puustinen, L. (Leena), Lehtonen, J. (Jussi), Hakola, L. (Leena), Simell, S. (Satu), Toppari, J. (Jorma), Ilonen, J. (Jorma), Veijola, R. (Riitta), Virtanen, S. M. (Suvi M.), Knip, M. (Mikae), and Hyöty, H. (Heikki)

Abstract

Enterovirus and adenovirus infections have been linked to the development of celiac disease. We evaluated this association in children who developed biopsy-proven celiac disease (N = 41) during prospective observation starting from birth, and in control children (N = 53) matched for the calendar time of birth, sex, and HLA-DQ genotype. Enterovirus and adenovirus infections were diagnosed by seroconversions in virus antibodies in longitudinally collected sera using EIA. Enterovirus infections were more frequent in case children before the appearance of celiac disease-associated tissue transglutaminase autoantibodies compared to the corresponding period in control children (OR 6.3, 95% CI 1.8–22.3; p = 0.005). No difference was observed in the frequency of adenovirus infections. The findings suggest that enterovirus infections may contribute to the process leading to celiac disease.

Published
2021

45. Type 1 diabetes linked PTPN22 gene polymorphism is associated with the frequency of circulating regulatory T cells

Author

Valta, M. (Milla), Gazali, A. M. (Ahmad Mahfuz), Viisanen, T. (Tyyne), Ihantola, E. (Emmi‐Leena), Ekman, I. (Ilse), Toppari, J. (Jorma), Knip, M. (Mikael), Veijola, R. (Riitta), Ilonen, J. (Jorma), Lempainen, J. (Johanna), and Kinnunen, T. (Tuure)

Subjects
Type 1 diabetes, endocrine system diseases, Autoimmunity, Regulatory T cells, PTPN22, Human
Abstract

Dysfunction of FOXP3‐positive regulatory T cells (Tregs) likely plays a major role in the pathogenesis of multiple autoimmune diseases including type 1 diabetes (T1D). Whether genetic polymorphisms associated with the risk of autoimmune diseases affect Treg frequency or function is currently unclear. Here, we analysed the effect of T1D‐associated major HLA class II haplotypes and seven single nucleotide polymorphisms in six non‐HLA genes [INS (rs689), PTPN22 (rs2476601), IL2RA (rs12722495 and rs2104286), PTPN2 (rs45450798), CTLA4 (rs3087243), and ERBB3 (rs2292239)] on peripheral blood Treg frequencies. These were determined by flow cytometry in 65 subjects who had progressed to T1D, 86 islet autoantibody‐positive at‐risk subjects, and 215 islet autoantibody‐negative healthy controls. The PTPN22 rs2476601 risk allele A was associated with an increase in total (p = 6 × 10⁻⁶) and naïve (p = 4 × 10⁻⁵) CD4+CD25+CD127lowFOXP3+ Treg frequencies. These findings were validated in a separate cohort comprising ten trios of healthy islet autoantibody‐negative children carrying each of the three PTPN22 rs2476601 genotypes AA, AG, and GG (p = 0.005 for total and p = 0.03 for naïve Tregs, respectively). In conclusion, our analysis implicates the autoimmune PTPN22 rs2476601 risk allele A in controlling the frequency of Tregs in human peripheral blood.

Published
2020

46. HLA-DR-DQ haplotypes and specificity of the initial autoantibody in islet specific autoimmunity

Author

Mikk, M.-L. (Mari-Liis), Pfeiffer, S. (Sophie), Kiviniemi, M. (Minna), Laine, A.-P. (Antti-Pekka), Lempainen, J. (Johanna), Härkönen, T. (Taina), Toppari, J. (Jorma), Veijola, R. (Riitta), Knip, M. (Mikael), Ilonen, J. (Jorma), and T. F. (The Finnish Pediatric Diabetes Register)

Subjects
type 1 diabetes, HLA genotypes, islet specific autoantibodies
Abstract

Objective: We aimed to clarify the association of various HLA risk alleles with different types of autoantibodies initiating islet specific autoimmunity. Methods: Follow-up cohorts from the Finnish Type 1 Diabetes Prediction and Prevention (DIPP) study and children diagnosed with type 1 diabetes (T1D) from the Finnish Pediatric Diabetes Register (FPDR) were analyzed for the presence of autoantibodies to insulin (IAA), glutamic acid decarboxylase (GADA), IA-2 antigen (IA-2A), and zinc transporter 8 (ZnT8A); and genotyped for HLA DR/DQ alleles. In the DIPP study, autoantibodies were regularly analyzed from birth up to 15 years of age. Results: In the DIPP cohort, 621 children developed one single persistent autoantibody, GADA in 284, IAA in 268, and IA-2A in 40 cases. Highly significant differences in the specificity of the first autoantibody were observed between HLA genotypes. Homozygotes for the DR3-DQ2 haplotype had almost exclusively GADA as the first autoantibody, whereas a more even distribution between GADA and IAA was found in DR3-DQ2/DR4-DQ8 as well as DR3-DQ/x and DR4-DQ8/x genotypes (x referring to neutral haplotypes). In DR4-DQ8 positive genotypes with the DRB1*04:01 allele IAA was more often the first autoantibody than in DRB1*04:04 positive genotypes. Various neutral haplotypes also significantly affected the relative proportions of different initial autoantibodies. These findings were confirmed and expanded in a series of 1591 T1D children under the age of 10 years from FPDR. Conclusions: These results emphasize the importance of HLA class II polymorphisms in the recognition of autoantigen epitopes in the initiation of various pathways of the autoimmune response.

Published
2020

50. Mucosal-associated invariant T cell alterations during the development of human type 1 diabetes

Author

Gazali, A. M. (Ahmad M.), Schroderus, A.-M. (Anna-Mari), Näntö-Salonen, K. (Kirsti), Rintamäki, R. (Reeta), Pihlajamäki, J. (Jussi), Knip, M. (Mikael), Veijola, R. (Riitta), Toppari, J. (Jorma), Ilonen, J. (Jorma), Kinnunen, T. (Tuure), Gazali, A. M. (Ahmad M.), Schroderus, A.-M. (Anna-Mari), Näntö-Salonen, K. (Kirsti), Rintamäki, R. (Reeta), Pihlajamäki, J. (Jussi), Knip, M. (Mikael), Veijola, R. (Riitta), Toppari, J. (Jorma), Ilonen, J. (Jorma), and Kinnunen, T. (Tuure)

Abstract

Aims/hypothesis: Mucosal-associated invariant T (MAIT) cells are innate-like T cells that recognise derivatives of bacterial riboflavin metabolites presented by MHC-Ib-related protein 1 (MR1) molecules and are important effector cells for mucosal immunity. Their development can be influenced by the intestinal microbiome. Since the development of type 1 diabetes has been associated with changes in the gut microbiome, this can be hypothesised to lead to alterations in circulating MAIT cells. Accordingly, peripheral blood MAIT cell alterations have been reported previously in patients with type 1 diabetes. However, a comprehensive analysis of the frequency and phenotype of circulating MAIT cells at different stages of type 1 diabetes progression is currently lacking. Methods: We analysed the frequency, phenotype and functionality of peripheral blood MAIT cells, as well as γδ T cells, invariant natural killer T (iNKT) cells and natural killer (NK) cells with flow cytometry in a cross-sectional paediatric cohort (aged 2–15) consisting of 51 children with newly diagnosed type 1 diabetes, 27 autoantibody-positive (AAb+) at-risk children, and 113 healthy control children of similar age and HLA class II background. The frequency of MAIT cells was also assessed in a separate cross-sectional adult cohort (aged 19–39) of 33 adults with established type 1 diabetes and 37 healthy individuals of similar age. Results: Children with newly diagnosed type 1 diabetes displayed a proportional increase of CD8⁻CD27⁻ MAIT cells compared with healthy control children (median 4.6% vs 3.1% of MAIT cells, respectively, p = 0.004), which was associated with reduced expression of C-C chemokine receptor (CCR)5 (median 90.0% vs 94.3% of MAIT cells, p = 0.02) and β7 integrin (median 73.5% vs 81.7% of MAIT cells, p = 0.004), as well as decreased production of IFN-γ (median 57.1% vs 69.3% of MAIT cells, p = 0.04) by the MAIT cells. The frequency of MAIT cells was also decreased in AAb⁺ child

Published
2020

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