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Endocrinología, Diabetes y Nutrición (English ed.)
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Inicio Endocrinología, Diabetes y Nutrición (English ed.) MODY 3 diabetes, not every early onset diabetes is type 1 diabetes
Journal Information
Vol. 66. Issue 4.
Pages 271-272 (April 2019)
Vol. 66. Issue 4.
Pages 271-272 (April 2019)
Scientific letter
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MODY 3 diabetes, not every early onset diabetes is type 1 diabetes
Diabetes tipo MODY-3, no todo debut es diabetes tipo 1
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María José Sánchez Maloa,
Corresponding author
mjsanchezmalo@gmail.com

Corresponding author.
, Marta Arrudi Morenoa, Gracia María Lou Francésb
a Servicio de Pediatría, Hospital Universitario Miguel Servet, Zaragoza, Spain
b Unidad de Diabetes Pediátrica, Hospital Universitario Miguel Servet, Zaragoza, Spain
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Hyperglycemia is an increasingly common cause of consultation in paediatrics. Many clinical entities are included under the term of diabetes mellitus.1

Type 1 diabetes mellitus is the most common form of childhood diabetes. It represents 95% of all cases of diabetes in Spain among patients under 20 years of age.2 Maturity onset diabetes of the young (MODY) is a monogenic form of familial early onset diabetes. The diagnosis of MODY requires a high degree of suspicion, with the family history of the patient being taken into account. This disorder is characterized by a dominant autosomal hereditary trait, insulinopenia, and the absence of obesity and insulin resistance and immune markers.3 Many patients with MODY are mistakenly diagnosed with type 1 or type 2 diabetes.1

Maturity onset diabetes of the young is the most common type of monogenic diabetes. All known subtypes of MODY are caused by heterozygous mutations in genes that are crucial for the development or proper functioning of the pancreatic β cells.4 Developments in molecular genetics have allowed MODY to be classified and diagnosed, with the description to date of at least 14 different genes causing the disease.5 The most common subtype in the first two decades of life is MODY-2.1 Patients with the MODY-3 subtype have a more severe defect in insulin secretion, with a greater risk of microvascular complications and a greater need for treatment with oral antidiabetic drugs or insulin.6 For this reason, and since this disease is unusual in paediatrics, we consider it worthwhile to publish the present case.

A male currently 14 years old was attending and referred from another centre where he had been initially diagnosed with type 1 diabetes at 12 years of age. He had blood glucose 203mg/dl in the absence of ketoacidosis, and associated polydipsia, polyuria and a three month history of polyphagia, with no weight loss. Initial glycosylated haemoglobin (HbA1c) was 8.9%, with glycosuria and negative glutamic acid decarboxylase (GAD) antibodies. There was no ketonuria. The celiac disease markers were negative, and the thyroid profile was normal. Microalbuminuria proved negative. The other study findings at the start of diabetes, with cardiological, ophthalmological and neurological evaluations were normal. His body weight was 51kg, with a height of 156cm, and a body mass index (BMI) of 20.96kg/m2. He was at Tanner stage III. The rest of the physical examination proved normal. The patient had a history of hyperglycemic episodes, which were classified as stress hyperglycemia.

The family history revealed type 2 diabetes mellitus in the mother and maternal grandmother.

Treatment was started in the form of multiple-dose insulin with basal insulin (glargine) and bolus insulin (lispro fast-acting insulin analogue), resulting in acceptable blood glucose levels.

In view of the negative GAD antibodies, the study was completed by having blood samples of the child, mother, maternal grandmother and maternal great uncle sent to the Research Unit of Hospital de Cruces (Bilbao, Spain) for the analysis of insulin autoantibodies, GAD autoantibodies and AI2 autoantibodies, all of which proved negative. The patient has a male sibling three years younger, with apparently normal glycemia; no sample was therefore sent at that time.

During the follow-up of our patient, which has been irregular due to localization and transport difficulties, there has been a progressive decrease in his insulin requirements while adequate glycemic control has been maintained, with a rapid decrease in HbA1c (5.8% at 4 months). After negative antibodies were confirmed, and together with the described family history, a MODY study was made, which revealed a heterozygous mutation in exon 4 of the HNF1A gene, consisting of a thiamine duplication in position 789. The mother was also found to present this alteration in heterozygosis. The maternal grandmother and great uncle did not have the mutation. This mutation has not been previously described, but since it results in the formation of an abnormal protein it is likely to be responsible for the disease, this hypotheses being corroborated by the maternal involvement.

With the confirmed diagnosis of MODY-3, rapid insulin was discontinued, the dose of basal insulin was lowered, and treatment with sulfonylureas (gliclazide) 15mg every 24h with progressive dose increments was started simultaneously. The patient currently maintains adequate HbA1c levels. In the most recent blood test, blood glucose was 135mg/dl, and HbA1c 7%, with a dose increase up to 45mg daily.

The patient is currently controlled by the diabetes unit of our hospital, with a good clinical course and adequate control of the disease.

One year later, the male sibling was admitted due to a random blood glucose level of 214mg/dl, glycosuria and HbA1c 8%. Given the background of our patient, and with the suspicion of MODY-3 onset, treatment with sulfonylureas was started. Four days after admission the glycemia values were found to be adequate. The results of the genetic study are pending confirmation.

Since MODY-3 is an unusual form of diabetes in paediatric patients, we consider the publication of this case to be of considerable interest, especially as several members of the same family are affected. We underline the importance of clinical suspicion in establishing a proper diagnosis, since it allowed the treatment to be modified and the disease to be adequately controlled, leading to an improvement in patient quality of life.

Collaboration with the Research Unit of Hospital de Cruces (Bilbao, Spain) proved essential in obtaining a correct diagnosis.

References
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L. Tapia, E. Córdoba, B. Picazo, P. Ranchal.
Diabetes MODY. Una causa frecuente de hiperglucemia.
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[2]
M. Thunander, C. Petersson, K. Jonzon, J. Fornander, B. Ossiansson, C. Torn.
Incidence of type 1 and type 2 diabetes in adults and children in Kronoberg, Sweden.
Diabetes Res Clin Pract, 82 (2008), pp. 247-255
[3]
R. Barrio.
Diabetes mellitus en la edad pediátrica: diabetes tipo 1, diabetes tipo 2 y MODY.
Endocrinol Nutr, 51 (2004), pp. 31-37
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S.S. Fajans, G.I. Bell.
MODY.
Diabetes Care, 34 (2011), pp. 1878-1884
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H. Ræder, S. Johansson, P.I. Holm, I.S. Haldorsen, E. Mas, V. Sbarra, et al.
Mutations in the CEL VNTR cause a syndrome of diabetes and pancreatic exocrine dysfunction.
Nat Genet, 38 (2006), pp. 54-62
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E. Martín-Campagne, C. Roa-Llamazares, M.J. Ballester-Herrera, E. Palomo-Atance, P. Giralt-Muiña.
Diagnóstico inusualmente precoz de diabetes MODY-3 condicionado por la obesidad.
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Please cite this article as: Sánchez Malo MJ, Arrudi Moreno M, Lou Francés GM. Diabetes tipo MODY-3, no todo debut es diabetes tipo 1. Endocrinol Diabetes Nutr. 2019;66:271–272.

Copyright © 2019. SEEN and SED
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