Mutations in HNF1A Result in Marked Alterations of Plasma Glycan Profile

A recent genome-wide association study identified hepatocyte nuclear factor 1-α (HNF1A) as a key regulator of fucosylation. We hypothesized that loss-of-function HNF1A mutations causal for maturity-onset diabetes of the young (MODY) would display altered fucosylation of N-linked glycans on plasma pr...

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Autores principales: Thanabalasingham, Gaya, Huffman, Jennifer E., Kattla, Jayesh J., Novokmet, Mislav, Rudan, Igor, Gloyn, Anna L., Hayward, Caroline, Adamczyk, Barbara, Reynolds, Rebecca M., Muzinic, Ana, Hassanali, Neelam, Pucic, Maja, Bennett, Amanda J., Essafi, Abdelkader, Polasek, Ozren, Mughal, Saima A., Redzic, Irma, Primorac, Dragan, Zgaga, Lina, Kolcic, Ivana, Hansen, Torben, Gasperikova, Daniela, Tjora, Erling, Strachan, Mark W.J., Nielsen, Trine, Stanik, Juraj, Klimes, Iwar, Pedersen, Oluf B., Njølstad, Pål R., Wild, Sarah H., Gyllensten, Ulf, Gornik, Olga, Wilson, James F., Hastie, Nicholas D., Campbell, Harry, McCarthy, Mark I., Rudd, Pauline M., Owen, Katharine R., Lauc, Gordan, Wright, Alan F.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Diabetes Association 2013
Materias:
Original Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3609552/
https://www.ncbi.nlm.nih.gov/pubmed/23274891
http://dx.doi.org/10.2337/db12-0880
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author Thanabalasingham, Gaya
Huffman, Jennifer E.
Kattla, Jayesh J.
Novokmet, Mislav
Rudan, Igor
Gloyn, Anna L.
Hayward, Caroline
Adamczyk, Barbara
Reynolds, Rebecca M.
Muzinic, Ana
Hassanali, Neelam
Pucic, Maja
Bennett, Amanda J.
Essafi, Abdelkader
Polasek, Ozren
Mughal, Saima A.
Redzic, Irma
Primorac, Dragan
Zgaga, Lina
Kolcic, Ivana
Hansen, Torben
Gasperikova, Daniela
Tjora, Erling
Strachan, Mark W.J.
Nielsen, Trine
Stanik, Juraj
Klimes, Iwar
Pedersen, Oluf B.
Njølstad, Pål R.
Wild, Sarah H.
Gyllensten, Ulf
Gornik, Olga
Wilson, James F.
Hastie, Nicholas D.
Campbell, Harry
McCarthy, Mark I.
Rudd, Pauline M.
Owen, Katharine R.
Lauc, Gordan
Wright, Alan F.
author_facet Thanabalasingham, Gaya
Huffman, Jennifer E.
Kattla, Jayesh J.
Novokmet, Mislav
Rudan, Igor
Gloyn, Anna L.
Hayward, Caroline
Adamczyk, Barbara
Reynolds, Rebecca M.
Muzinic, Ana
Hassanali, Neelam
Pucic, Maja
Bennett, Amanda J.
Essafi, Abdelkader
Polasek, Ozren
Mughal, Saima A.
Redzic, Irma
Primorac, Dragan
Zgaga, Lina
Kolcic, Ivana
Hansen, Torben
Gasperikova, Daniela
Tjora, Erling
Strachan, Mark W.J.
Nielsen, Trine
Stanik, Juraj
Klimes, Iwar
Pedersen, Oluf B.
Njølstad, Pål R.
Wild, Sarah H.
Gyllensten, Ulf
Gornik, Olga
Wilson, James F.
Hastie, Nicholas D.
Campbell, Harry
McCarthy, Mark I.
Rudd, Pauline M.
Owen, Katharine R.
Lauc, Gordan
Wright, Alan F.
author_sort Thanabalasingham, Gaya
collection PubMed
description A recent genome-wide association study identified hepatocyte nuclear factor 1-α (HNF1A) as a key regulator of fucosylation. We hypothesized that loss-of-function HNF1A mutations causal for maturity-onset diabetes of the young (MODY) would display altered fucosylation of N-linked glycans on plasma proteins and that glycan biomarkers could improve the efficiency of a diagnosis of HNF1A-MODY. In a pilot comparison of 33 subjects with HNF1A-MODY and 41 subjects with type 2 diabetes, 15 of 29 glycan measurements differed between the two groups. The DG9-glycan index, which is the ratio of fucosylated to nonfucosylated triantennary glycans, provided optimum discrimination in the pilot study and was examined further among additional subjects with HNF1A-MODY (n = 188), glucokinase (GCK)-MODY (n = 118), hepatocyte nuclear factor 4-α (HNF4A)-MODY (n = 40), type 1 diabetes (n = 98), type 2 diabetes (n = 167), and nondiabetic controls (n = 98). The DG9-glycan index was markedly lower in HNF1A-MODY than in controls or other diabetes subtypes, offered good discrimination between HNF1A-MODY and both type 1 and type 2 diabetes (C statistic ≥0.90), and enabled us to detect three previously undetected HNF1A mutations in patients with diabetes. In conclusion, glycan profiles are altered substantially in HNF1A-MODY, and the DG9-glycan index has potential clinical value as a diagnostic biomarker of HNF1A dysfunction.
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spelling pubmed-36095522014-04-01 Mutations in HNF1A Result in Marked Alterations of Plasma Glycan Profile Thanabalasingham, Gaya Huffman, Jennifer E. Kattla, Jayesh J. Novokmet, Mislav Rudan, Igor Gloyn, Anna L. Hayward, Caroline Adamczyk, Barbara Reynolds, Rebecca M. Muzinic, Ana Hassanali, Neelam Pucic, Maja Bennett, Amanda J. Essafi, Abdelkader Polasek, Ozren Mughal, Saima A. Redzic, Irma Primorac, Dragan Zgaga, Lina Kolcic, Ivana Hansen, Torben Gasperikova, Daniela Tjora, Erling Strachan, Mark W.J. Nielsen, Trine Stanik, Juraj Klimes, Iwar Pedersen, Oluf B. Njølstad, Pål R. Wild, Sarah H. Gyllensten, Ulf Gornik, Olga Wilson, James F. Hastie, Nicholas D. Campbell, Harry McCarthy, Mark I. Rudd, Pauline M. Owen, Katharine R. Lauc, Gordan Wright, Alan F. Diabetes Original Research A recent genome-wide association study identified hepatocyte nuclear factor 1-α (HNF1A) as a key regulator of fucosylation. We hypothesized that loss-of-function HNF1A mutations causal for maturity-onset diabetes of the young (MODY) would display altered fucosylation of N-linked glycans on plasma proteins and that glycan biomarkers could improve the efficiency of a diagnosis of HNF1A-MODY. In a pilot comparison of 33 subjects with HNF1A-MODY and 41 subjects with type 2 diabetes, 15 of 29 glycan measurements differed between the two groups. The DG9-glycan index, which is the ratio of fucosylated to nonfucosylated triantennary glycans, provided optimum discrimination in the pilot study and was examined further among additional subjects with HNF1A-MODY (n = 188), glucokinase (GCK)-MODY (n = 118), hepatocyte nuclear factor 4-α (HNF4A)-MODY (n = 40), type 1 diabetes (n = 98), type 2 diabetes (n = 167), and nondiabetic controls (n = 98). The DG9-glycan index was markedly lower in HNF1A-MODY than in controls or other diabetes subtypes, offered good discrimination between HNF1A-MODY and both type 1 and type 2 diabetes (C statistic ≥0.90), and enabled us to detect three previously undetected HNF1A mutations in patients with diabetes. In conclusion, glycan profiles are altered substantially in HNF1A-MODY, and the DG9-glycan index has potential clinical value as a diagnostic biomarker of HNF1A dysfunction. American Diabetes Association 2013-04 2013-03-14 /pmc/articles/PMC3609552/ /pubmed/23274891 http://dx.doi.org/10.2337/db12-0880 Text en © 2013 by the American Diabetes Association. Readers may use this article as long as the work is properly cited, the use is educational and not for profit, and the work is not altered. See http://creativecommons.org/licenses/by-nc-nd/3.0/ for details.
spellingShingle Original Research
Thanabalasingham, Gaya
Huffman, Jennifer E.
Kattla, Jayesh J.
Novokmet, Mislav
Rudan, Igor
Gloyn, Anna L.
Hayward, Caroline
Adamczyk, Barbara
Reynolds, Rebecca M.
Muzinic, Ana
Hassanali, Neelam
Pucic, Maja
Bennett, Amanda J.
Essafi, Abdelkader
Polasek, Ozren
Mughal, Saima A.
Redzic, Irma
Primorac, Dragan
Zgaga, Lina
Kolcic, Ivana
Hansen, Torben
Gasperikova, Daniela
Tjora, Erling
Strachan, Mark W.J.
Nielsen, Trine
Stanik, Juraj
Klimes, Iwar
Pedersen, Oluf B.
Njølstad, Pål R.
Wild, Sarah H.
Gyllensten, Ulf
Gornik, Olga
Wilson, James F.
Hastie, Nicholas D.
Campbell, Harry
McCarthy, Mark I.
Rudd, Pauline M.
Owen, Katharine R.
Lauc, Gordan
Wright, Alan F.
Mutations in HNF1A Result in Marked Alterations of Plasma Glycan Profile
title Mutations in HNF1A Result in Marked Alterations of Plasma Glycan Profile
title_full Mutations in HNF1A Result in Marked Alterations of Plasma Glycan Profile
title_fullStr Mutations in HNF1A Result in Marked Alterations of Plasma Glycan Profile
title_full_unstemmed Mutations in HNF1A Result in Marked Alterations of Plasma Glycan Profile
title_short Mutations in HNF1A Result in Marked Alterations of Plasma Glycan Profile
title_sort mutations in hnf1a result in marked alterations of plasma glycan profile
topic Original Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3609552/
https://www.ncbi.nlm.nih.gov/pubmed/23274891
http://dx.doi.org/10.2337/db12-0880
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