Transforming lives: transferring patients with neonatal diabetes from insulin to sulphonylureas
DOI:
https://doi.org/10.1002/edn.60Keywords:
Genetic testing, neonatal diabetes, sulphonylureas, KCNJ11, Kir6.2Abstract
AbstractBackground: Mutations in the KCNJ11 gene encoding Kir6.2 are the most common cause of neonatal diabetes. Although clinically ‘insulin dependent’ these patients may respond to oral sulphonylureas. Families’ experiences of coping with the condition and the impact of transferring from long-term insulin to sulphonylureas have not been explored.
Aim: This study aims to increase understanding of having a child with neonatal diabetes caused by a mutation in the KCNJ11 gene.
Method: In-depth interviews were conducted with parents of 11 UK patients with KCNJ11 gene mutations during 2004–2005. The patients had a median age of 13 years (range 0.5–57 years). Qualitative methodology was used to gain an in-depth understanding of the experiences from diagnosis of diabetes to present day. Interviews were audiotaped, transcribed and subjected to thematic content analysis.
Results: Three key categories were identified: i) difficulties managing diabetes in a baby/young child – highlighting the constant care required and impact on family relationships; ii) recognition and implications of learning difficulties and muscle weakness; iii) impact of transfer from insulin to sulphonylureas – including effect on lifestyle, learning difficulties and glycaemic control.
Conclusion: Having a baby with neonatal diabetes is exhausting and places additional strain on families. Mothers acknowledged feeling overprotective. Before genetic diagnosis learning delay and diabetes had not been related, but had implications for future independent living. Transfer to sulphonylureas greatly improved diabetes control and reduced incidences of hypoglycaemia; this enabled families to normalise the condition and reduced social stigma. Sulphonylurea treatment transformed quality of life for the children and their families, who were able to view the future more positively.
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References
Slingerland AS, Hattersley AT. Mutations in the Kir6.2 subunit of the KA„ channel and permanent neonatal diabetes: new insights and new treatment. Ann Med 2005; 37: 186–195.
Hattersley AT, Ashcroft FM. Activ-ating mutations in Kir6.2 and neonatal diabetes, new clinical syn-dromes, new scientific insights, new therapy. Diabetes 2005; 54(9): 2503–2513.
Iafusco D, Stazi MA, Cotichini R, et al. Permanent diabetes mellitus in the first year of life. Diabetologia 2002; 45: 798–804.
Edghill EL, Dix RJ, Flanagan SE, et al. HLA genotyping supports a non autoimmune etiology in patients diagnosed with diabetes under the age of 6 months. Diabetes 2006; 55(6): 1895–1898.
Gloyn AL, Pearson ER, Antcliff JF, et aL. Activating mutations in the gene encoding the ATP-sensitive Potassium channel subunit Kir6.2 and permanent neonatal diabetes. N Engl J Med 2004; 350: 1838–1849.
Pearson ER, Flechtner I, Njolstad PR, et al. Successful transfer of patients with diabetes due to mutant Kir6.2 from insulin to oral sulfony-lureas. IVEJM 2006; 355(5): 467–477.
Shepherd M, Hattersley AT, Ellard S. Integration of the MODY link nurse project: 20 month evaluation. J Diabetes Nurs 2005; 9(2): 47–52.
John H, Flanagan SE, Corrall R, et al. Neonatal diabetes is more than just a paediatric problem: 57 years of diabetes from a Kir6.2 mutation. Pract Diabetes Int 2005; 22(9): 342–344.
Sullivan-Bolyai S, Deatrick J, Grup-puso P, et al. Constant vigilance: mothers' work parenting young chil-dren with Type 1 diabetes. J Pediatr Nurs 2003; 18(1): 21–29.
Hatton DL, Canam C, Thorne S, et aL. Parents' perceptions of caring for an infant or toddler with diabetes. J Adv Nurs 1995; 22: 569–577.
Lowes L, Gregory JVV, Lyne P. Newly diagnosed childhood diabetes: a psychosocial transition for parents?J Adv Nurs 2005; 50(3): 253–261.
Shepherd M. 'I'm amazed I've been able to come off injections': patients' perceptions of genetic test-ing in diabetes. Pract Diabetes Int 2003; 20(9): 338–342.
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