Identification of pathogenic GCK variants in patients with common type 2 diabetes can lead to discontinuation of pharmacological treatment

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Identification of pathogenic GCK variants in patients with common type 2 diabetes can lead to discontinuation of pharmacological treatment. / Thuesen, Anne Cathrine Baun; Jensen, Rasmus Tanderup; Maagensen, Henrik; Kristiansen, Maja Refshauge; Sørensen, Henrik Toft; Vaag, Allan; Beck-Nielsen, Henning; Pedersen, Oluf B.; Grarup, Niels; Nielsen, Jens Steen; Rungby, Jørgen; Gjesing, Anette Prior; Storgaard, Heidi; Vilsbøll, Tina; Hansen, Torben.

I: Molecular Genetics and Metabolism Reports, Bind 35, 100972, 2023.

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningfagfællebedømt

Harvard

Thuesen, ACB, Jensen, RT, Maagensen, H, Kristiansen, MR, Sørensen, HT, Vaag, A, Beck-Nielsen, H, Pedersen, OB, Grarup, N, Nielsen, JS, Rungby, J, Gjesing, AP, Storgaard, H, Vilsbøll, T & Hansen, T 2023, 'Identification of pathogenic GCK variants in patients with common type 2 diabetes can lead to discontinuation of pharmacological treatment', Molecular Genetics and Metabolism Reports, bind 35, 100972. https://doi.org/10.1016/j.ymgmr.2023.100972

APA

Thuesen, A. C. B., Jensen, R. T., Maagensen, H., Kristiansen, M. R., Sørensen, H. T., Vaag, A., Beck-Nielsen, H., Pedersen, O. B., Grarup, N., Nielsen, J. S., Rungby, J., Gjesing, A. P., Storgaard, H., Vilsbøll, T., & Hansen, T. (2023). Identification of pathogenic GCK variants in patients with common type 2 diabetes can lead to discontinuation of pharmacological treatment. Molecular Genetics and Metabolism Reports, 35, [100972]. https://doi.org/10.1016/j.ymgmr.2023.100972

Vancouver

Thuesen ACB, Jensen RT, Maagensen H, Kristiansen MR, Sørensen HT, Vaag A o.a. Identification of pathogenic GCK variants in patients with common type 2 diabetes can lead to discontinuation of pharmacological treatment. Molecular Genetics and Metabolism Reports. 2023;35. 100972. https://doi.org/10.1016/j.ymgmr.2023.100972

Author

Thuesen, Anne Cathrine Baun ; Jensen, Rasmus Tanderup ; Maagensen, Henrik ; Kristiansen, Maja Refshauge ; Sørensen, Henrik Toft ; Vaag, Allan ; Beck-Nielsen, Henning ; Pedersen, Oluf B. ; Grarup, Niels ; Nielsen, Jens Steen ; Rungby, Jørgen ; Gjesing, Anette Prior ; Storgaard, Heidi ; Vilsbøll, Tina ; Hansen, Torben. / Identification of pathogenic GCK variants in patients with common type 2 diabetes can lead to discontinuation of pharmacological treatment. I: Molecular Genetics and Metabolism Reports. 2023 ; Bind 35.

Bibtex

@article{0c8f4e3d903046c9a5f2b05807caf26d,
title = "Identification of pathogenic GCK variants in patients with common type 2 diabetes can lead to discontinuation of pharmacological treatment",
abstract = "Background: Functionally disruptive variants in the glucokinase gene (GCK) cause a form of mild non-progressive hyperglycemia, which does not require pharmacological treatment. A substantial proportion of patients with type 2 diabetes (T2D) carry GCK variants. We aimed to investigate whether carriers of rare GCK variants diagnosed with T2D have a glycemic phenotype and treatment response consistent with GCK-diabetes. Methods: Eight patients diagnosed with T2D from the Danish DD2 cohort who had previously undergone sequencing of GCK participated. Clinical examinations at baseline included an oral glucose tolerance test and continuous glucose monitoring. Carriers with a glycemic phenotype consistent with GCK-diabetes took part in a three-month treatment withdrawal. Results: Carriers of pathogenic and likely pathogenic variants had lower median fasting glucose and C-peptide levels compared to carriers of variants of uncertain significance and benign variants (median fasting glucose: 7.3 (interquartile range: 0.4) mmol/l vs. 9.5 (1.6) mmol/l, p = 0.04; median fasting C-peptide 902 (85) pmol/l vs. 1535 (295) pmol/l, p = 0.03). Four participants who discontinued metformin treatment and one diet-treated participant were reevaluated after three months. There was no deterioration of HbA1c or fasting glucose (median baseline HbA1c: 49 (3) vs. 51 (6) mmol/mol after three months, p = 0.4; median baseline fasting glucose: 7.3 (0.4) mmol/l vs. 7.0 (0.6) mmol/l after three months, p = 0.5). Participants did not consistently fulfill best practice guidelines for GCK screening nor clinical criteria for monogenic diabetes. Discussion: Carriers of pathogenic or likely pathogenic GCK variants identified by unselected screening in T2D should be reported, as they have a glycemic phenotype and treatment response consistent with GCK-diabetes. Variants of uncertain significance should be interpreted with care. Systematic genetic screening of patients with common T2D receiving routine care can lead to the identification and precise care of patients with misclassified GCK-diabetes who are not identifiable through common genetic screening criteria.",
keywords = "Diagnosis, MODY (maturity-onset diabetes of the young), T2D (type 2 diabetes), Treatment",
author = "Thuesen, {Anne Cathrine Baun} and Jensen, {Rasmus Tanderup} and Henrik Maagensen and Kristiansen, {Maja Refshauge} and S{\o}rensen, {Henrik Toft} and Allan Vaag and Henning Beck-Nielsen and Pedersen, {Oluf B.} and Niels Grarup and Nielsen, {Jens Steen} and J{\o}rgen Rungby and Gjesing, {Anette Prior} and Heidi Storgaard and Tina Vilsb{\o}ll and Torben Hansen",
note = "Publisher Copyright: {\textcopyright} 2023",
year = "2023",
doi = "10.1016/j.ymgmr.2023.100972",
language = "English",
volume = "35",
journal = "Molecular Genetics and Metabolism Reports",
issn = "2214-4269",
publisher = "Elsevier",

}

RIS

TY - JOUR

T1 - Identification of pathogenic GCK variants in patients with common type 2 diabetes can lead to discontinuation of pharmacological treatment

AU - Thuesen, Anne Cathrine Baun

AU - Jensen, Rasmus Tanderup

AU - Maagensen, Henrik

AU - Kristiansen, Maja Refshauge

AU - Sørensen, Henrik Toft

AU - Vaag, Allan

AU - Beck-Nielsen, Henning

AU - Pedersen, Oluf B.

AU - Grarup, Niels

AU - Nielsen, Jens Steen

AU - Rungby, Jørgen

AU - Gjesing, Anette Prior

AU - Storgaard, Heidi

AU - Vilsbøll, Tina

AU - Hansen, Torben

N1 - Publisher Copyright: © 2023

PY - 2023

Y1 - 2023

N2 - Background: Functionally disruptive variants in the glucokinase gene (GCK) cause a form of mild non-progressive hyperglycemia, which does not require pharmacological treatment. A substantial proportion of patients with type 2 diabetes (T2D) carry GCK variants. We aimed to investigate whether carriers of rare GCK variants diagnosed with T2D have a glycemic phenotype and treatment response consistent with GCK-diabetes. Methods: Eight patients diagnosed with T2D from the Danish DD2 cohort who had previously undergone sequencing of GCK participated. Clinical examinations at baseline included an oral glucose tolerance test and continuous glucose monitoring. Carriers with a glycemic phenotype consistent with GCK-diabetes took part in a three-month treatment withdrawal. Results: Carriers of pathogenic and likely pathogenic variants had lower median fasting glucose and C-peptide levels compared to carriers of variants of uncertain significance and benign variants (median fasting glucose: 7.3 (interquartile range: 0.4) mmol/l vs. 9.5 (1.6) mmol/l, p = 0.04; median fasting C-peptide 902 (85) pmol/l vs. 1535 (295) pmol/l, p = 0.03). Four participants who discontinued metformin treatment and one diet-treated participant were reevaluated after three months. There was no deterioration of HbA1c or fasting glucose (median baseline HbA1c: 49 (3) vs. 51 (6) mmol/mol after three months, p = 0.4; median baseline fasting glucose: 7.3 (0.4) mmol/l vs. 7.0 (0.6) mmol/l after three months, p = 0.5). Participants did not consistently fulfill best practice guidelines for GCK screening nor clinical criteria for monogenic diabetes. Discussion: Carriers of pathogenic or likely pathogenic GCK variants identified by unselected screening in T2D should be reported, as they have a glycemic phenotype and treatment response consistent with GCK-diabetes. Variants of uncertain significance should be interpreted with care. Systematic genetic screening of patients with common T2D receiving routine care can lead to the identification and precise care of patients with misclassified GCK-diabetes who are not identifiable through common genetic screening criteria.

AB - Background: Functionally disruptive variants in the glucokinase gene (GCK) cause a form of mild non-progressive hyperglycemia, which does not require pharmacological treatment. A substantial proportion of patients with type 2 diabetes (T2D) carry GCK variants. We aimed to investigate whether carriers of rare GCK variants diagnosed with T2D have a glycemic phenotype and treatment response consistent with GCK-diabetes. Methods: Eight patients diagnosed with T2D from the Danish DD2 cohort who had previously undergone sequencing of GCK participated. Clinical examinations at baseline included an oral glucose tolerance test and continuous glucose monitoring. Carriers with a glycemic phenotype consistent with GCK-diabetes took part in a three-month treatment withdrawal. Results: Carriers of pathogenic and likely pathogenic variants had lower median fasting glucose and C-peptide levels compared to carriers of variants of uncertain significance and benign variants (median fasting glucose: 7.3 (interquartile range: 0.4) mmol/l vs. 9.5 (1.6) mmol/l, p = 0.04; median fasting C-peptide 902 (85) pmol/l vs. 1535 (295) pmol/l, p = 0.03). Four participants who discontinued metformin treatment and one diet-treated participant were reevaluated after three months. There was no deterioration of HbA1c or fasting glucose (median baseline HbA1c: 49 (3) vs. 51 (6) mmol/mol after three months, p = 0.4; median baseline fasting glucose: 7.3 (0.4) mmol/l vs. 7.0 (0.6) mmol/l after three months, p = 0.5). Participants did not consistently fulfill best practice guidelines for GCK screening nor clinical criteria for monogenic diabetes. Discussion: Carriers of pathogenic or likely pathogenic GCK variants identified by unselected screening in T2D should be reported, as they have a glycemic phenotype and treatment response consistent with GCK-diabetes. Variants of uncertain significance should be interpreted with care. Systematic genetic screening of patients with common T2D receiving routine care can lead to the identification and precise care of patients with misclassified GCK-diabetes who are not identifiable through common genetic screening criteria.

KW - Diagnosis

KW - MODY (maturity-onset diabetes of the young)

KW - T2D (type 2 diabetes)

KW - Treatment

U2 - 10.1016/j.ymgmr.2023.100972

DO - 10.1016/j.ymgmr.2023.100972

M3 - Journal article

C2 - 37008541

AN - SCOPUS:85151087995

VL - 35

JO - Molecular Genetics and Metabolism Reports

JF - Molecular Genetics and Metabolism Reports

SN - 2214-4269

M1 - 100972

ER -

ID: 342497917