<i>HLA-A*24</i> Is an Independent Predictor of 5-Year Progression to Diabetes in Autoantibody-Positive First-Degree Relatives of Type 1 Diabetic Patients

Mbunwe, Eric; Auwera, Bart J. Van der; Vermeulen, Ilse; Demeester, Simke; Dalem, Annelien Van; Balti, Eric Vounsia; Aken, Sara Van; Derdelinckx, L.; Dorchy, Harry; Schepper, Jean De; Schravendijk, Christiaan Van; Wenzlau, Janet M.; Hutton, John C.; Pipeleers, Daniël; Weets, Ilse; Gorus, Frans

doi:10.2337/db12-0747

Cited by 20 publications

(40 citation statements)

References 25 publications

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“…Similarly, as many ENDIT participants were adults, only a minority had IAA and this may have limited our ability to identify subtle effects of HLA-A*24 on IAA prevalence and levels [10]. In contrast with other studies of at-risk relatives [2], we did not observe accelerated progression in HLA-A*24-positive ENDIT participants. The individuals at highest risk, including HLA-A*24 carriers, may have developed diabetes between ICA screening and study entry.…”

Section: Discussioncontrasting

confidence: 93%

“…The rate of beta cell destruction is heterogeneous among multiple islet autoantibody-positive individuals, but the reasons for this are poorly defined. The main type 1 diabetes susceptibility alleles are in the HLA class II region, but the class I allele HLA-A*24 has been linked with accelerated diabetes progression, acute diabetes onset and early and complete beta cell destruction [2]. Islet autoantibody characteristics in HLA-A*24 individuals with diabetes have proved counterintuitive; one might expect an overwhelming islet autoantibody response to be associated with rapid progression, but the opposite appears true.…”

Section: Introductionmentioning

confidence: 99%

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Attenuated humoral responses in HLA-A*24-positive individuals at risk of type 1 diabetes

Ye¹,

Long²,

Pearson³

et al. 2015

Diabetologia

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Section: Discussioncontrasting

confidence: 93%

Section: Introductionmentioning

confidence: 99%

Attenuated humoral responses in HLA-A*24-positive individuals at risk of type 1 diabetes

Ye¹,

Long²,

Pearson³

et al. 2015

Diabetologia

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“…The current results indicate that similar to observations in pre-type 1 diabetes, the presence of HLA-A*24 or autoantibody surges predicts b-cell loss during an inflammatory and/or immune process in islet allograft recipients (7,8). The association of early autoantibody rises with poor graft outcome confirms previous observations and has been explained as the consequence of autoantigen release after b-cell death (12).…”

Section: Discussionsupporting

confidence: 90%

“…Assays were validated by participation in successive Diabetes Antibody Standardization Programs (10). HLA-DQ2/DQ8 and -A*24 were determined by allele-specific oligotyping (8). The hyperglycemic clamp procedure was performed as previously described (6).…”

Section: Assays and Outcome Measuresmentioning

confidence: 99%

“…However, a positive outcome can be counteracted by other factors, including preexisting autoreactive T cells, HLA alloantibodies, or high lymphocyte counts (2-4). In recipients of a sufficiently large intraportal islet allograft (5,6), we investigated whether the presence of HLA-A*24, HLA-DQ2/DQ8, or rising islet autoantibody levels, previously shown to independently predict rapid b-cell loss in prediabetes (7,8), associates with poor functional graft outcome. …”

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confidence: 99%

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HLA-A24*Carrier Status and Autoantibody Surges Posttransplantation Associate With Poor Functional Outcome in Recipients of an Islet Allograft

et al. 2016

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OBJECTIVEWe investigated whether changes in islet autoantibody profile and presence of HLA risk markers, reported to predict rapid b-cell loss in pre-type 1 diabetes, associate with poor functional outcome in islet allograft recipients. RESEARCH DESIGN AND METHODSForty-one patients received ‡2.3 million b-cells/kg body wt in one to two intraportal implantations. Outcome after 6-18 months was assessed by C-peptide (random and stimulated), insulin dose, and HbA 1c . RESULTSPatients carrying HLA-A*24-positive or experiencing a significant autoantibody surge within 6 months after the first transplantation (n 5 19) had lower C-peptide levels (P £ 0.003) and higher insulin needs (P < 0.001) despite higher HbA 1c levels (P £ 0.018). They became less often insulin independent (16% vs. 68%, P 5 0.002) and remained less often C-peptide positive (47% vs. 100%, P < 0.001) than recipients lacking both risk factors. HLA-A*24 positivity or an autoantibody surge predicted insulin dependence (P 5 0.007). CONCLUSIONSHLA-A*24 and early autoantibody surge after islet implantation associate with poor functional graft outcome.The success rate of an intraportal islet graft for achieving insulin independence critically hinges on the amount of donor tissue implanted (1). However, a positive outcome can be counteracted by other factors, including preexisting autoreactive T cells, HLA alloantibodies, or high lymphocyte counts (2-4). In recipients of a sufficiently large intraportal islet allograft (5,6), we investigated whether the presence of HLA-A*24, HLA-DQ2/DQ8, or rising islet autoantibody levels, previously shown to independently predict rapid b-cell loss in prediabetes (7,8), associates with poor functional graft outcome. RESEARCH DESIGN AND METHODS Transplant ProtocolForty-one patients with C-peptide-negative type 1 diabetes (median age 45 years) with a history of recurrent hypoglycemia and negative for preexisting HLA class I and class II antibodies (4) received $2.3 million b-cells (;4,600 islet equivalents)/kg

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Type 1 Diabetes: Current Perspectives

Kozhakhmetova

Gillespie

2015

Methods in Molecular Biology

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Type 1 diabetes, resulting from the autoimmune destruction of insulin producing islet beta cells is caused by genetic and environmental determinants. Recent studies agree that counterintuitively, the major genetic susceptibility factors are decreasing in frequency as the incidence of the condition increases. This suggests a growing role for environmental determinants but these have been difficult to identify and our understanding of gene/environment effects are limited. Individuals "at risk" can be identified accurately through the presence of multiple islet autoantibodies and current efforts in type 1 diabetes research focus on improved biomarkers and strategies to prevent or reverse the condition through immunotherapy.

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HLA-A24* Is an Independent Predictor of 5-Year Progression to Diabetes in Autoantibody-Positive First-Degree Relatives of Type 1 Diabetic Patients

Cited by 20 publications

References 25 publications

Attenuated humoral responses in HLA-A*24-positive individuals at risk of type 1 diabetes

Attenuated humoral responses in HLA-A*24-positive individuals at risk of type 1 diabetes

HLA-A24*Carrier Status and Autoantibody Surges Posttransplantation Associate With Poor Functional Outcome in Recipients of an Islet Allograft

Type 1 Diabetes: Current Perspectives

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HLA-A*24 Is an Independent Predictor of 5-Year Progression to Diabetes in Autoantibody-Positive First-Degree Relatives of Type 1 Diabetic Patients

Cited by 20 publications

References 25 publications

Attenuated humoral responses in HLA-A*24-positive individuals at risk of type 1 diabetes

Attenuated humoral responses in HLA-A*24-positive individuals at risk of type 1 diabetes

HLA-A*24Carrier Status and Autoantibody Surges Posttransplantation Associate With Poor Functional Outcome in Recipients of an Islet Allograft

Type 1 Diabetes: Current Perspectives

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HLA-A24* Is an Independent Predictor of 5-Year Progression to Diabetes in Autoantibody-Positive First-Degree Relatives of Type 1 Diabetic Patients

HLA-A24*Carrier Status and Autoantibody Surges Posttransplantation Associate With Poor Functional Outcome in Recipients of an Islet Allograft