A combined risk score enhances prediction of type 1 diabetes among susceptible children

Committees

doi:10.1038/s41591-020-0930-4

A combined risk score enhances prediction of type 1 diabetes among susceptible children

Committees

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Abstract

Type 1 diabetes (T1D)—an autoimmune disease that destroys the pancreatic islets, resulting in insulin deficiency—often begins early in life when islet autoantibody appearance signals high risk¹. However, clinical diabetes can follow in weeks or only after decades, and is very difficult to predict. Ketoacidosis at onset remains common^2,3 and is most severe in the very young^4,5, in whom it can be life threatening and difficult to treat^6–9. Autoantibody surveillance programs effectively prevent most ketoacidosis^10–12 but require frequent evaluations whose expense limits public health adoption¹³. Prevention therapies applied before onset, when greater islet mass remains, have rarely been feasible¹⁴ because individuals at greatest risk of impending T1D are difficult to identify. To remedy this, we sought accurate, cost-effective estimation of future T1D risk by developing a combined risk score incorporating both fixed and variable factors (genetic, clinical and immunological) in 7,798 high-risk children followed closely from birth for 9.3 years. Compared with autoantibodies alone, the combined model dramatically improves T1D prediction at ≥2 years of age over horizons up to 8 years of age (area under the receiver operating characteristic curve ≥ 0.9), doubles the estimated efficiency of population-based newborn screening to prevent ketoacidosis, and enables individualized risk estimates for better prevention trial selection.

Original language	English (US)
Pages (from-to)	1247-1255
Number of pages	9
Journal	Nature Medicine
Volume	26
Issue number	8
DOIs	https://doi.org/10.1038/s41591-020-0930-4
State	Published - Aug 1 2020

ASJC Scopus subject areas

Biochemistry, Genetics and Molecular Biology(all)

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1038/s41591-020-0930-4

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@article{5f123dfa454949ef95dc3bad68eb3223,

title = "A combined risk score enhances prediction of type 1 diabetes among susceptible children",

abstract = "Type 1 diabetes (T1D)—an autoimmune disease that destroys the pancreatic islets, resulting in insulin deficiency—often begins early in life when islet autoantibody appearance signals high risk1. However, clinical diabetes can follow in weeks or only after decades, and is very difficult to predict. Ketoacidosis at onset remains common2,3 and is most severe in the very young4,5, in whom it can be life threatening and difficult to treat6–9. Autoantibody surveillance programs effectively prevent most ketoacidosis10–12 but require frequent evaluations whose expense limits public health adoption13. Prevention therapies applied before onset, when greater islet mass remains, have rarely been feasible14 because individuals at greatest risk of impending T1D are difficult to identify. To remedy this, we sought accurate, cost-effective estimation of future T1D risk by developing a combined risk score incorporating both fixed and variable factors (genetic, clinical and immunological) in 7,798 high-risk children followed closely from birth for 9.3 years. Compared with autoantibodies alone, the combined model dramatically improves T1D prediction at ≥2 years of age over horizons up to 8 years of age (area under the receiver operating characteristic curve ≥ 0.9), doubles the estimated efficiency of population-based newborn screening to prevent ketoacidosis, and enables individualized risk estimates for better prevention trial selection.",

author = "Committees and Ferrat, {Lauric A.} and Kendra Vehik and Sharp, {Seth A.} and {\AA}ke Lernmark and Rewers, {Marian J.} and She, {Jin Xiong} and Ziegler, {Anette G.} and Jorma Toppari and Beena Akolkar and Krischer, {Jeffrey P.} and Weedon, {Michael N.} and Oram, {Richard A.} and Hagopian, {William A.} and Simell, {Olli G.} and Annika Adamsson and Suvi Ahonen and Mari {\AA}kerlund and Leena Hakola and Anne Hekkala and Henna Holappa and Heikki Hy{\"o}ty and Anni Ikonen and Jorma Ilonen and Sinikka J{\"a}minki and Sanna Jokipuu and Leena Karlsson and Jukka Kero and Miia K{\"a}h{\"o}nen and Mikael Knip and Koivikko, {Minna Liisa} and Merja Koskinen and Mirva Koreasalo and Kalle Kurppa and Jarita Kyt{\"o}l{\"a} and Tiina Latva-aho and Katri Lindfors and Maria L{\"o}nnrot and Elina M{\"a}ntym{\"a}ki and Markus Mattila and Maija Miettinen and Katja Multasuo and Teija Mykk{\"a}nen and Tiina Niininen and Sari Niinist{\"o} and Mia Nyblom and Sami Oikarinen and Paula Ollikainen and Zhian Othmani and Richard McIndoe and Ashok Sharma",

note = "Funding Information: The TEDDY study is included in ClinicalTrials.gov under the identifier NCT00279318. The TEDDY Study Group is funded by U01 DK63829, U01 DK63861, U01 DK63821, U01 DK63865, U01 DK63863, U01 DK63836, U01 DK63790, UC4 DK63829, UC4 DK63861, UC4 DK63821, UC4 DK63865, UC4 DK63863, UC4 DK63836, UC4 DK95300, UC4 DK100238, UC4 DK106955, UC4 DK112243, UC4 DK117483 and UC4 DK100238, and by contract number HHSN267200700014C from the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK), National Institute of Allergy and Infectious Diseases (NIAID), Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD), National Institute of Environmental Health Sciences (NIEHS), Centers for Disease Control and Prevention (CDC) and JDRF. This work is supported in part by the National Institutes of Health/National Center for Advancing Translational Sciences Clinical and Translational Science Awards (UL1 TR000064 (University of Florida) and UL1 TR001082 (University of Colorado)) and Diabetes Research Center (5P30 DK017047; University of Washington). R.A.O. is supported by a Diabetes UK Harry Keen Fellowship (16/0005529). S.A.S. is supported by a Diabetes UK PhD studentship (17/0005757). M.N.W. is supported by the Wellcome Trust Institutional Strategic Support Fund (WT097835MF). R.A.O., L.A.F., W.A.H. and K.V. are supported by a JDRF strategic research agreement (3-SRA-2019-827-S-B). The authors thank the following former staff members at TEDDY Study Group centers: Michael Abbondondolo, Lori Ballard, David Hadley, Hye-Seung Lee, Wendy McLeod, Steven Meulemans, Henry Erlich, Steven J. Mack and Anna Lisa Fear. Publisher Copyright: {\textcopyright} 2020, The Author(s), under exclusive licence to Springer Nature America, Inc.",

year = "2020",

month = aug,

day = "1",

doi = "10.1038/s41591-020-0930-4",

language = "English (US)",

volume = "26",

pages = "1247--1255",

journal = "Nature Medicine",

issn = "1078-8956",

publisher = "Nature Publishing Group",

number = "8",

}

TY - JOUR

T1 - A combined risk score enhances prediction of type 1 diabetes among susceptible children

AU - Committees

AU - Ferrat, Lauric A.

AU - Vehik, Kendra

AU - Sharp, Seth A.

AU - Lernmark, Åke

AU - Rewers, Marian J.

AU - She, Jin Xiong

AU - Ziegler, Anette G.

AU - Toppari, Jorma

AU - Akolkar, Beena

AU - Krischer, Jeffrey P.

AU - Weedon, Michael N.

AU - Oram, Richard A.

AU - Hagopian, William A.

AU - Simell, Olli G.

AU - Adamsson, Annika

AU - Ahonen, Suvi

AU - Åkerlund, Mari

AU - Hakola, Leena

AU - Hekkala, Anne

AU - Holappa, Henna

AU - Hyöty, Heikki

AU - Ikonen, Anni

AU - Ilonen, Jorma

AU - Jäminki, Sinikka

AU - Jokipuu, Sanna

AU - Karlsson, Leena

AU - Kero, Jukka

AU - Kähönen, Miia

AU - Knip, Mikael

AU - Koivikko, Minna Liisa

AU - Koskinen, Merja

AU - Koreasalo, Mirva

AU - Kurppa, Kalle

AU - Kytölä, Jarita

AU - Latva-aho, Tiina

AU - Lindfors, Katri

AU - Lönnrot, Maria

AU - Mäntymäki, Elina

AU - Mattila, Markus

AU - Miettinen, Maija

AU - Multasuo, Katja

AU - Mykkänen, Teija

AU - Niininen, Tiina

AU - Niinistö, Sari

AU - Nyblom, Mia

AU - Oikarinen, Sami

AU - Ollikainen, Paula

AU - Othmani, Zhian

AU - McIndoe, Richard

AU - Sharma, Ashok

N1 - Funding Information: The TEDDY study is included in ClinicalTrials.gov under the identifier NCT00279318. The TEDDY Study Group is funded by U01 DK63829, U01 DK63861, U01 DK63821, U01 DK63865, U01 DK63863, U01 DK63836, U01 DK63790, UC4 DK63829, UC4 DK63861, UC4 DK63821, UC4 DK63865, UC4 DK63863, UC4 DK63836, UC4 DK95300, UC4 DK100238, UC4 DK106955, UC4 DK112243, UC4 DK117483 and UC4 DK100238, and by contract number HHSN267200700014C from the National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK), National Institute of Allergy and Infectious Diseases (NIAID), Eunice Kennedy Shriver National Institute of Child Health and Human Development (NICHD), National Institute of Environmental Health Sciences (NIEHS), Centers for Disease Control and Prevention (CDC) and JDRF. This work is supported in part by the National Institutes of Health/National Center for Advancing Translational Sciences Clinical and Translational Science Awards (UL1 TR000064 (University of Florida) and UL1 TR001082 (University of Colorado)) and Diabetes Research Center (5P30 DK017047; University of Washington). R.A.O. is supported by a Diabetes UK Harry Keen Fellowship (16/0005529). S.A.S. is supported by a Diabetes UK PhD studentship (17/0005757). M.N.W. is supported by the Wellcome Trust Institutional Strategic Support Fund (WT097835MF). R.A.O., L.A.F., W.A.H. and K.V. are supported by a JDRF strategic research agreement (3-SRA-2019-827-S-B). The authors thank the following former staff members at TEDDY Study Group centers: Michael Abbondondolo, Lori Ballard, David Hadley, Hye-Seung Lee, Wendy McLeod, Steven Meulemans, Henry Erlich, Steven J. Mack and Anna Lisa Fear. Publisher Copyright: © 2020, The Author(s), under exclusive licence to Springer Nature America, Inc.

PY - 2020/8/1

Y1 - 2020/8/1

N2 - Type 1 diabetes (T1D)—an autoimmune disease that destroys the pancreatic islets, resulting in insulin deficiency—often begins early in life when islet autoantibody appearance signals high risk1. However, clinical diabetes can follow in weeks or only after decades, and is very difficult to predict. Ketoacidosis at onset remains common2,3 and is most severe in the very young4,5, in whom it can be life threatening and difficult to treat6–9. Autoantibody surveillance programs effectively prevent most ketoacidosis10–12 but require frequent evaluations whose expense limits public health adoption13. Prevention therapies applied before onset, when greater islet mass remains, have rarely been feasible14 because individuals at greatest risk of impending T1D are difficult to identify. To remedy this, we sought accurate, cost-effective estimation of future T1D risk by developing a combined risk score incorporating both fixed and variable factors (genetic, clinical and immunological) in 7,798 high-risk children followed closely from birth for 9.3 years. Compared with autoantibodies alone, the combined model dramatically improves T1D prediction at ≥2 years of age over horizons up to 8 years of age (area under the receiver operating characteristic curve ≥ 0.9), doubles the estimated efficiency of population-based newborn screening to prevent ketoacidosis, and enables individualized risk estimates for better prevention trial selection.

AB - Type 1 diabetes (T1D)—an autoimmune disease that destroys the pancreatic islets, resulting in insulin deficiency—often begins early in life when islet autoantibody appearance signals high risk1. However, clinical diabetes can follow in weeks or only after decades, and is very difficult to predict. Ketoacidosis at onset remains common2,3 and is most severe in the very young4,5, in whom it can be life threatening and difficult to treat6–9. Autoantibody surveillance programs effectively prevent most ketoacidosis10–12 but require frequent evaluations whose expense limits public health adoption13. Prevention therapies applied before onset, when greater islet mass remains, have rarely been feasible14 because individuals at greatest risk of impending T1D are difficult to identify. To remedy this, we sought accurate, cost-effective estimation of future T1D risk by developing a combined risk score incorporating both fixed and variable factors (genetic, clinical and immunological) in 7,798 high-risk children followed closely from birth for 9.3 years. Compared with autoantibodies alone, the combined model dramatically improves T1D prediction at ≥2 years of age over horizons up to 8 years of age (area under the receiver operating characteristic curve ≥ 0.9), doubles the estimated efficiency of population-based newborn screening to prevent ketoacidosis, and enables individualized risk estimates for better prevention trial selection.

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UR - http://www.scopus.com/inward/citedby.url?scp=85089358607&partnerID=8YFLogxK

U2 - 10.1038/s41591-020-0930-4

DO - 10.1038/s41591-020-0930-4

M3 - Article

C2 - 32770166

AN - SCOPUS:85089358607

SN - 1078-8956

VL - 26

SP - 1247

EP - 1255

JO - Nature Medicine

JF - Nature Medicine

IS - 8

ER -

A combined risk score enhances prediction of type 1 diabetes among susceptible children

Abstract

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