Department of Diabetes and Endocrinology, Mater Misericordiae University Hospital, Dublin, Ireland.
Department of Molecular Genetics, Royal Devon and Exeter NHS Foundation Trust, Exeter, UK.
Diabet Med. 2020 May;37(5):876-884. doi: 10.1111/dme.14145. Epub 2019 Oct 21.
To examine the phenotypic features of people identified with ABCC8-maturity-onset diabetes of the young (MODY) who were included in the adult 'Mater MODY' cohort and to establish their response to sulfonylurea therapy.
Ten participants with activating ABCC8 mutations were phenotyped in detail. A 2-hour oral glucose tolerance test was performed to establish glycaemic tolerance, with glucose, insulin and C-peptide measurements taken at baseline and 30-min intervals. Insulin was discontinued and sulfonylurea therapy initiated after genetic diagnosis of ABCC8-MODY. A blinded continuous glucose monitoring sensor was used to establish glycaemic control on insulin vs a sulfonylurea.
The mean age at diagnosis of diabetes was 33.8 ± 11.1 years, with fasting glucose of 18.9 ± 11.5 mmol/l and a mean (range) HbA of 86 (51,126) mmol/mol [10.0 (6.8,13.7)%]. Following a genetic diagnosis of ABCC8-MODY three out of four participants discontinued insulin (mean duration 10.6 ± 1.69 years) and started sulfonylurea treatment. The mean (range) HbA prior to genetic diagnosis was 52 (43,74) mmol/mol (6.9%) and the post-treatment change was 44 (30,57) mmol/mol (6.2%; P=0.16). Retinopathy was the most common microvascular complication in this cohort, occurring in five out of 10 participants.
Low-dose sulfonylurea therapy resulted in stable glycaemic control and the elimination of hypoglycaemic episodes attributable to insulin therapy. The use of appropriate therapy at the early stages of diabetes may decrease the incidence of complications and reduce the risks of hypoglycaemia associated with insulin therapy.
研究成年“Mater MODY”队列中被诊断为 ABCC8-青年发病型糖尿病(MODY)的患者的表型特征,并确定他们对磺酰脲类药物治疗的反应。
详细表型分析 10 名携带激活 ABCC8 突变的参与者。进行 2 小时口服葡萄糖耐量试验以建立血糖耐量,在基线和 30 分钟间隔测量血糖、胰岛素和 C 肽。在基因诊断为 ABCC8-MODY 后,停止使用胰岛素并开始使用磺酰脲类药物治疗。使用盲法连续血糖监测传感器在胰岛素与磺酰脲类药物之间建立血糖控制。
糖尿病诊断时的平均年龄为 33.8 ± 11.1 岁,空腹血糖为 18.9 ± 11.5mmol/L,平均(范围)HbA 为 86(51,126)mmol/mol [10.0(6.8,13.7)%]。在基因诊断为 ABCC8-MODY 后,4 名参与者中有 3 名停止使用胰岛素(平均持续时间 10.6 ± 1.69 年)并开始使用磺酰脲类药物治疗。基因诊断前的平均(范围)HbA 为 52(43,74)mmol/mol(6.9%),治疗后的变化为 44(30,57)mmol/mol(6.2%;P=0.16)。在这个队列中,最常见的微血管并发症是视网膜病变,发生在 10 名参与者中的 5 名。
低剂量磺酰脲类药物治疗可实现稳定的血糖控制,并消除与胰岛素治疗相关的低血糖发作。在糖尿病早期使用适当的治疗方法可能会降低并发症的发生率,并降低与胰岛素治疗相关的低血糖风险。
