Congenital hyperinsulinism: 2 case reports with different rare variants in ABCC8

Article information

Ann Pediatr Endocrinol Metab. 2021;26(1):60-65
Publication date (electronic) : 2020 August 7
doi : https://doi.org/10.6065/apem.2040042.021
1Pediatric Endocrinology and Diabetology Unit, Ser vice of Pediatrics, Lausanne University Hospital and University of Lausanne, Lausanne, Switzerland
2Department of Pediatrics, Hôpitaux Neuchâtelois, Neuchâtel, Switzerland
3Diabetology, Neuchâtel, Switzerland
4Departement of Clinical Genetics, Odense University Hospital, Odense, Denmark
5Hans Christian Andersen Children’s Hospital, Odense University Hospital, Odense, Denmark
6D e velopmental Endocr inology Research Group, Clinical and Molecular Genetics Unit, Institute of Child Health, University College London, London, UK
7Boston College, William F. Connell School of Nursing, Chestnut Hill, MA, USA
8Service of Neonatology, Lausanne University Hospital and University of Lausanne, Lausanne, Switzerland
Address for correspondence: Michael Hauschild Pediatric Endocrinology and Diabetology Unit, Service of Pediatrics, Lausanne University Hospital and University of Lausanne, Chemin de Montétan 16 1004 Lausanne, Switzerland Email: Michael.Hauschild@chuv.ch
Received 2020 March 18; Revised 2020 May 9; Accepted 2020 May 19.

Abstract

Congenital hyperinsulinism (CHI) is a rare glucose metabolism disorder characterized by unregulated secretion of insulin that leads to hyperinsulinemic hypoglycemia (HH). Most cases are caused by mutations in the KATP-channel genes ABCC8 and KCNJ11. We report 2 patients that experienced severe HH from the first day of life. Patient 1 developed midgut volvulus after initiating diazoxide and required intestinal resection. He was subsequently managed with a high-dose octreotide and glucose-enriched diet. Consistent with diffuse type CHI by 18F-dihydroxyphenylalanine positron emission tomography-computed tomography, genetic testing revealed a homozygous ABCC8 variant, c.1801G>A, p.(Val601Ile). The rare variant was previously reported to be diazoxide-responsive, and the patient responded well to diazoxide monotherapy, with clinical remission at 2 years of age. Patient 2 responded to diazoxide with spontaneous clinical remission at 15 months of age. However, an oral glucose tolerance test at 7 years of age revealed hyperinsulinism. Genetic testing revealed that the proband and several seemingly healthy family members harbored a novel, heterozygous ABCC8 variant, c.1780T>C, p.(Ser594Pro). Genetic findings identified previously unrecognized HH in the proband’s mother. The proband’s uncle had been diagnosed with monogenic ABCC8-diabetes and was successfully transitioned from insulin to glibenclamide therapy. We report findings of intestinal malrotation and volvulus occurring 2 days after initiation of diazoxide treatment. We also report a novel, heterozygous ABCC8 variant in a family that exhibited cases of CHI in infancy and HH and monogenic diabetes in adult members. The cases demonstrate the importance and clinical utility of genetic analyses for informing and guiding treatment and care.

Highlights

We report 2 patients with CHI caused by novel DNA variants in ABCC8. Intestinal malrotation occurred after diazoxide treatment in one patient. Genetic analysis should be performed in all patients and family members that present with CHI to define the best treatment approaches.

Introduction

Congenital hyperinsulinism (CHI) is a rare disease that can result in potentially life-threatening hyperinsulinemic hypoglycemia (HH), caused by inadequate insulin secretion by pancreatic β-cells. The incidence is estimated to be 1:50,000 live births, and 1:2500 live births in communities with founder mutations [1]. Rapid diagnosis and treatment are essential to prevent persistent or recurrent hypoglycemia and neurological damage [2-5]. CHI can be classified as either transient or permanent and has 3 histologic subtypes: focal, diffuse or atypical CHI. Standard treatment for focal CHI is selective partial pancreatectomy, while diffuse CHI necessitates long-term drug therapy or subtotal pancreatectomy [3,6].

To date, underlying genetic mutations for CHI are identified in 45%–55% of cases. Fourteen genes have been identified (ABCC8, KCNJ11, GLUD1, GCK, HADH, HNF1A, HNF4A, SLC16A1, UCP2 and more recently CACNAID, FOXA2, HK1, PGM1, and PMM2) [7]. That approximately half of the cases do not have an identifiable genetic etiology suggests that additional loci are undiscovered [8,9]. Notably, CHI most frequently results from mutations in KATP-channel genes, ABCC8 or KCNJ11 [2,3,9,10]. Diazoxide-unresponsive CHI can be caused by homozygous or heterozygous KATP-channel mutations leading to diffuse CHI. Alternatively, a paternal KATP-channel mutation and somatic loss of heterozygosity of chromosome 11p15 lead to focal diazoxide-unresponsive CHI. CHI can be nonsyndromic or associated with a range of syndromes, including Beckwith-Wiedemann, Turner, and Kabuki syndrome [11]. Novel manifestations in apparently non-syndromic CHI patients can represent a novel syndromic association, unrecognized medical side effects, or chance findings [10]. Notably, spontaneous CHI remission and reversion to diabetes in adulthood have been reported in patients harboring mutations in ABCC8, HNF4A, or HNF1A [12]. Many patients with monogenic diabetes can be effectively treated with oral antidiabetic medication instead of insulin, which underscores the importance of a genetic diagnosis [13].

According to recent American College of Medical Genetics guidelines [14], novel changes should be considered variants of unknown significance (VUS) and should not be considered pathogenic until the variant is verified in other patients. Accordingly, identifying novel variants associated with reversal of CHI to diabetes in adult life has implications for genetic cascade screening of family members.

We describe 2 patients with novel ABCC8 mutations associated with spontaneous clinical remission.

Case reports

1. Case 1

A Caucasian male patient was born via normal vaginal delivery at 331/7 weeks gestation to nonconsanguineous parents (Fig. 1A). The pregnancy was unremarkable with no gestational diabetes mellitus. The patient was large-for-gestational age (birthweight, 3,150 g; length, 51 cm; both >97th percentile) with no dysmorphic features. Apgar scores were 5, 8, and 8 (at 1, 5, and 10 minutes, respectively). At 2 hours of life, he developed severe symptomatic hypoglycemia (blood glucose <0.1 mmol/L) with hypotonia. A critical blood sample was drawn, and intravenous (IV) glucose infusion (up to 19 mg/kg/min) was initiated to maintain normoglycemia.

Fig. 1.

Pedigrees showing inheritance of ABCC8 mutations in both families. Squares represent males and circles represent females. The arrow depicts the proband with CHI. The individual lVa of family B underwent genetic testing and was confirmed not to be a carrier of ABCC8 mutation. (A) Family A: parents (IIIa/b) are asymptomatic carriers. (B) Family B: variable presentation of individuals harboring the heterozygous ABCC8 mutation, including symptomatic hyperinsulinemic hypoglycemia (IIIb), monogenic diabetes (IIIc), and diabetes of unknown origin (IId).

During hypoglycemia, serum insulin, and C-peptide levels were elevated in the setting of suppressed β-hydroxybutyrate and free fatty acids (Table 1). Cortisol, growth hormone, and thyroid hormones were within normal limits, and metabolic and infection screening were negative. Analysis with 18F-dihydroxyphenylalanine positron emission tomography-computed tomography (Discovery 690, GE Healthcare, Chicago, IL, USA) showed general uptake of glucose from the pancreas, suggestive of diffuse CHI (Fig. 2). Oral diazoxide (10 mg/kg/day) was initiated on day 7 of life. Diazoxide combined with high-rate IV glucose infusion (12 mg/kg/min) maintained blood glucose level within normal range. Oral feeding was difficult, and the child developed emesis. Intestinal malrotation, and volvulus of the ileum were diagnosed on day 9 of life. Diazoxide was discontinued, and 76 cm of necrotic ileum/jejunum was resected with intestinal stoma. Octreotide (up to 48 µg/kg/day subcutaneous, continuously) and amlodipine (0.1 mg/kg/day) were introduced 7 days after surgery, which stabilized blood glucose level with a persistent need for IV glucose in the high-normal range (6–7 mg/kg/min).

Clinical and genetic characteristics

Fig. 2.

Axial fluorine-18L-3,4hydroxyphenylalanine positron emission tomography image. Diffuse uptake of F-fluoro-L-DOPA by the pancreas is visualized by the hot spot (white arrow). Physiological distribution of the radiotracer is observed with higher accumulation in the kidneys and lower accumulation in the liver.

Molecular analysis (International Clinical Laboratory of University of Exeter, Exeter,UK) revealed that the proband harbored a homozygous missense DNA variant, c.1801G>A, p.(Val601Ile), in exon 12 of ABCC8 (reference sequence: NM_001287174.1) (Fig. 3). Amino acids in this residue are evolutionary conserved. Both PolyPhen-2 (http://genetics.bwh.harvard.edu/pph2/) and PANTHER (http://pantherdb.org/tools/csnpScoreForm.jsp) in silico algorithms predicted the rare variant to be pathogenic (Table 1).

Fig. 3.

Three-dimensional modelled structure of a pancreatic ATP-sensitive potassium channel. (A) The KATP-channel is a hetero-octameric complex composed of 4 Kir6.2 subunits and 4 SUR1 units. The transmembrane domains are highlighted. (B) The genetic variants in our 2 cases are located on the same transmembrane domain (TMD1) of the SUR1 subunit.

The unaffected parents were both heterozygous carriers of the ABCC8 variant. To our knowledge, only 1 case harboring this mutation has been reported [15]. In this report, the ABCC8 mutation in the male newborn was paternally inherited, and diazoxide was discontinued after 14 months. In the current case, octreotide was weaned after 3 days, and diazoxide treatment was reintroduced followed by a progressive decrease in IV glucose infusion, which was finally stopped at day 54 of life. The intestinal stoma was reversed at 67 days of life with no evidence of short bowel syndrome.

At follow-up at 2 years of life, the patient had no hypoglycemic episodes, and diazoxide was discontinued. A subsequent fasting tolerance test was age-appropriate, and he exhibited normal growth and neurological development.

2. Case 2

A Hispanic male patient and his healthy, dizygotic twin brother were born via emergency Caesarian section at 344/7 weeks gestation due to abnormal fetal heart rate on cardiotocographic monitoring. The pregnancy was uneventful without gestational diabetes, and no formal glucose tolerance testing was performed. The nonconsanguineous parents had a healthy 3-year-old daughter, and family history revealed several maternal family members with diabetes mellitus (Fig. 1B).

The newborn infant had a birth weight of 2,150 g (50th percentile), while his twin brother weighed 2,550 g. The patient had moderate asphyxia and required noninvasive ventilator support for several days. On his first day of life, he experienced severe hypoglycemia (blood glucose<0.1 mmol/L) and required IV glucose (up to 21 mg/kg/min) to maintain normoglycemia. Physical examination was unremarkable. The diagnosis of CHI was based on hypoglycemic episodes (<2.4 mmol/L) on the first day of life, unsuppressed insulin level during hypoglycemia, and high carbohydrate requirements to maintain normal glycemic level (Table 1). Diazoxide treatment promptly resolved the hypoglycemia.

Molecular testing (Odense University Hospital, Odense, Denmark) identified a novel, heterozygous DNA variant, c.1780T>C, p.(Ser594Pro), in exon 12 of ABCC8 (reference sequence: NM_000352) (Fig. 3). The residue is evolutionarily conserved, and 1 of 2 in silico algorithms predicted the variant to be likely deleterious (Table 1). Based on the American College of Medical Genetics guidelines, we considered the change to be a VUS. Diazoxide was discontinued at 15 months of age. Follow-up at 7 years of age revealed normal growth and psychomotor development. He had age-appropriate fasting tolerance without hypoglycemic events. However, a subsequent oral glucose tolerance test (OGTT) revealed moderate hyperinsulinism (+30 minutes: insulin, 58.8 µU/L [normal range, 30–50 mUl/L]; glucose, 7.7 mmol/L) followed by marginal, nonsymptomatic hypoglycemia at +120 minutes (insulin, 7.37 µU/L; glucose, 3.1 mmol/L) (Table 2).

Case 2: Oral glucose tolerance test

Interestingly, the mother (Fig. 1B, lllb) reported frequent episodes of lightheadedness. Subsequently, an OGTT revealed hyperinsulinism in the mother at +30 minutes (185.5 mU/L) that induced symptomatic HH at +120 minutes (blood glucose, 3 mmol/L; insulin, 27 mU/L) (Table 2). The proband's maternal uncle (Fig. 1B, IIIc) had diabetes mellitus, which was being treated with insulin. Lab testing was negative for antiglutamic acid decarboxylase, anti-insulin, and anti-IA2 antibodies, and serum C-peptide level was 0.68 µg/L, which was only slightly below the normal range (1.0–3.1 µg/L). On insulin therapy, the uncle had good metabolic control (glycated hemoglobin) yet suffered frequent hypoglycemic episodes. The maternal great-grandmother (Fig. 1B, Ib) also had been diagnosed with diabetes mellitus, but no detailed clinical information was available.

Cascade screening in the family revealed that the proband’s older sister (Fig. 1B, IVa), mother (Fig. 1B, lllb), maternal uncle (Fig. 1B, lllc), and maternal grandfather (Fig. 1B, IId) harbored the same heterozygous ABCC8 variant p.(Ser594Pro). Consequent to genetic testing, the proband’s maternal uncle was rediagnosed with monogenic ABCC8-diabetes. He was transitioned from insulin to oral antidiabetic medication (glibenclamide 3×5 mg daily) and experienced no further hypoglycemic episodes.

Discussion

We report 2 patients with CHI caused by novel DNA variants in ABCC8. Patient 1 was diagnosed with CHI due to a homozygous ABCC8 mutation inherited from unaffected parents, which was consistent with an autosomal recessive mode of transmission. The patient was unresponsive to diazoxide treatment, and oral intake was not possible. Subtotal pancreatectomy was considered as a potential treatment option; however, a literature review revealed a case of a patient that harbored the identical missense mutation that had responded to diazoxide treatment [15]. Based on the single case observation, we opted to postpone pancreatectomy and use alternative treatment (octreotide and amlodipine) during the postoperative fasting period prior to resuming oral diazoxide. Thus, detailed clinical investigation and scholarly inquiry led to an appropriate clinical approach and avoided irreversible surgical intervention. Cochrane and GRADE criteria consider case reports to be weak levels of evidence. However, for the present case, this information was the best available evidence and helped guide the therapeutic approach [6]. This example demonstrates how case reports can inform clinical care, particularly in the setting of rare diseases such as CHI.

Intestinal malrotation occurs in approximately 1 in 500 living births. Malrotation is estimated to be symptomatic 1 in 6,000 live births, and up to 80% of symptomatic cases occur in newborns [16]. Risk factors for volvulus include birth defects such as intestinal malrotation, Hirschsprung disease, and isomerism or heterotaxy syndrome. Recently, rare copy number variations (CNVs) have been identified in patients with syndromic intestinal malrotation, suggesting that CNV screening could be informative in cases when intestinal malrotation occurs in a constellation of other malformations [17]. To the best of our knowledge, this is the first report that associated congenital malrotation with neonatal hyperinsulinism. A recent study found 'likely pathogenic' or 'pathogenic' CNVs in 4 of 47 patients (8.5%) with intestinal malrotation [17]. To date, no reports have implicated the 11p15.1 region of ABCC8 in intestinal malrotation. We are not aware of any study that has identified an association between diazoxide therapy with volvulus, and this possibility merits consideration. It is unclear if co-occurrence of malrotation and CHI is merely a coincidence or if there is a true causal association. Therefore, studies in larger patient cohorts are needed to clarify the potential link between ABCC8 mutations and midgut malrotation.

Case 2 documents transient CHI due to a heterozygous mutation in ABCC8, which is consistent with an autosomal dominant (AD) mode of transmission. A detailed, multigenerational family histor y and cascade screening facilitated reclassification of the maternal uncle's diabetes mellitus. Patients with monogenic diabetes can be treated with oral antidiabetic medications instead of insulin [13]. Thus, molecular analysis enabled treatment modification from insulin to oral antidiabetic medication.

As reported by Kapoor and colleagues, siblings harboring the identical AD mutation in ABCC8 exhibit variable phenotypes, which can range from asymptomatic macrosomia to persistent HH in childhood to glucose intolerance or early-onset diabetes mellitus in adulthood [18]. Vieira et al. [19] described a patient carrying a de novo AD mutation in ABCC8 in which HH evolved to gestational diabetes and subsequently into diabetes mellitus.

Gain-of-function mutations in ABCC8 or KCNJ11 lead to KATP-channel hyperactivity causing neonatal diabetes. Conversely, loss-of-function mutations that reduce channel activity cause CHI. These observations can be explained by the variable affinity of mutant sulfonylurea receptors for adenosine triphosphate magnesium salt [20]. However, it remains unclear how the identical mutation can be associated with disparate phenotypes (i.e., CHI and diabetes) within the same pedigree. Some have hypothesized that the primary insulin secretion defect relates to chronically increased intracellular calcium level that activates apoptotic pathways [18].

In the case in this study, the patient and his unaffected older sister (Fig. 1B, IVa) might have increased risk for developing diabetes mellitus later in life. Accordingly, careful long-term medical follow-up is warranted. The genotype-phenotype correlations in pedigree 2 should be interpreted with caution as other family members with diabetes mellitus did not undergo genetic testing. Although clinical evidence supports the pathogenicity of the identified novel mutation, to-date, in silico analyses showed discrepant results, and in vitro functional studies of the identified ABCC8 mutants have not been conducted.

In conclusion, the 2 case reports reported herein illustrate highly variable phenotypes in patients harboring mutations in ABCC8. We report a unique finding of intestinal malrotation and volvulus that occurred 2 days after diazoxide treatment in a patient with CHI harboring a homozygous ABCC8 mutation. Further studies are needed to determine if these entities are pathophysiologically related. The cases demonstrate the importance and clinical utility of genetic analyses for informing and guiding treatment and care. First, only rare cases (case 1) of autosomal recessive, biallelic ABCC8 mutations are diazoxide-responsive. Second, genetic analysis should be performed in all patients that present with CHI to define the best treatment approaches. Finally, patients with heterozygous mutations in ABCC8 and their family members should be closely followed clinically, as they might be at increased risk for developing diabetes mellitus.

Notes

Ethical statement

The parents have given their written and signed consent for publication of the data of their infants.

Conflicts of interest

No potential conflict of interest relevant to this article was reported.

References

1. Bellanné-Chantelot C, Saint-Martin C, Ribeiro MJ, Vaury C, Verkarre V, Arnoux JB, et al. ABCC8 and KCNJ11 molecular spectrum of 109 patients with diazoxide-unresponsive congenital hyperinsulinism. J Med Genet 2010;47:752–9.
2. Kapoor RR, Flanagan SE, Arya VB, Shield JP, Ellard S, Hussain K. Clinical and molecular characterisation of 300 patients with congenital hyperinsulinism. Eur J Endocrinol 2013;168:557–64.
3. Roženková K, Güemes M, Shah P, Hussain K. The diagnosis and management of hyperinsulinaemic hypoglycaemia. J Clin Res Pediatr Endocrinol 2015;7:86–97.
4. Helleskov A, Melikyan M, Globa E, Shcherderkina I, Poertner F, Larsen AM, et al. Both low blood glucose and insufficient treatment confer risk of neurodevelopmental impairment in congenital hyperinsulinism: a multinational cohort study. Front Endocrinol 2017;8:156.
5. R asmussen AG, Melikian M, Globa E, Detlefsen S, Rasmussen L, Petersen H, et al. The difficult management of persistent, non-focal congenital hyperinsulinism: a retrospective review from a single, tertiary center. Pediatr Diabetes 2020;21:441–55.
6. Yorifuji T. Congenital hyperinsulinism: current status and future perspectives. Ann Pediatr Endocrinol Metab 2014;19:57–68.
7. Gillis D. Familial hyperinsulinism. In : Adam MP, Ardinger HH, Pagon RA, Wallace SE, Bean LJ, Stephens K, eds. GeneReviews® [Internet] Seattle (WA): University of Washington, Seattle; 1993-2020. [cited 2019 Nov 20]. Available from: http://www.ncbi.nlm.nih.gov/books/NBK1375/.
8. Vajravelu ME, De León DD. Genetic characteristics of patients with congenital hyperinsulinism. Curr Opin Pediatr 2018;30:568–75.
9. Flanagan SE, Kapoor RR, Hussain K. Genetics of congenital hyperinsulinemic hypoglycemia. Semin Pediatr Surg 2011;20:13–7.
10. Martínez R, Fernández-Ramos C, Vela A, Velayos T, Aguayo A, Urrutia I, et al. Clinical and genetic characterization of congenital hyperinsulinism in Spain. Eur J Endocrinol 2016;174:717–26.
11. Mohamed Z, Arya VB, Hussain K. Hyperinsulinaemic hypoglycaemia:genetic mechanisms, diagnosis and management. J Clin Res Pediatr Endocrinol 2012;4:169–8.
12. Rahman SA, Nessa A, Hussain K. Molecular mechanisms of congenital hyperinsulinism. J Mol Endocrinol 2015;54:R119–29.
13. Misra S, Owen KR. Genetics of monogenic diabetes: present clinical challenges. Curr Diab Rep 2018;18:141.
14. Richards S, Aziz N, Bale S, Bick D, Das S, Gastier-Foster J, et al. Standards and guidelines for the interpretation of sequence variants: a joint consensus recommendation of the American College of Medical Genetics and Genomics and the Association for Molecular Pathology. Genet Med Off J Am Coll Med Genet 2015;17:405–24.
15. Arya VB, Guemes M, Nessa A, Alam S, Shah P, Gilbert C, et al. Clinical and histological heterogeneity of congenital hyperinsulinism due to paternally inherited heterozygous ABCC8/KCNJ11 mutations. Eur J Endocrinol 2014;171:685–95.
16. Strouse PJ. Disorders of intestinal rotation and fixation (« malrotation »). Pediatr Radiol 2004;34:837–51.
17. Salehi Karlslätt K, Pettersson M, Jäntti N, Szafranski P, Wester T, Husberg B, et al. Rare copy number variants contribute pathogenic alleles in patients with intestinal malrotation. Mol Genet Genomic Med 2019;7e549.
18. Kapoor RR, Flanagan SE, James CT, McKiernan J, Thomas AM, Harmer SC, et al. Hyperinsulinaemic hypoglycaemia and diabetes mellitus due to dominant ABCC8/KCNJ11 mutations. Diabetologia 2011;54:2575–83.
19. Vieira TC, Bergamin CS, Gurgel LC, Moisés RS. Hyperinsulinemic hypoglycemia evolving to gestational diabetes and diabetes mellitus in a family carrying the inactivating ABCC8 E1506K mutation. Pediatr Diabetes 2010;11:505–8.
20. Ortiz D, Bryan J. Neonatal diabetes and congenital hyperinsulinism caused by mutations in ABCC8/SUR1 are associated with altered and opposite affinities for ATP and ADP. Front Endocrinol 2015;6:48.

Article information Continued

Fig. 1.

Pedigrees showing inheritance of ABCC8 mutations in both families. Squares represent males and circles represent females. The arrow depicts the proband with CHI. The individual lVa of family B underwent genetic testing and was confirmed not to be a carrier of ABCC8 mutation. (A) Family A: parents (IIIa/b) are asymptomatic carriers. (B) Family B: variable presentation of individuals harboring the heterozygous ABCC8 mutation, including symptomatic hyperinsulinemic hypoglycemia (IIIb), monogenic diabetes (IIIc), and diabetes of unknown origin (IId).

Fig. 2.

Axial fluorine-18L-3,4hydroxyphenylalanine positron emission tomography image. Diffuse uptake of F-fluoro-L-DOPA by the pancreas is visualized by the hot spot (white arrow). Physiological distribution of the radiotracer is observed with higher accumulation in the kidneys and lower accumulation in the liver.

Fig. 3.

Three-dimensional modelled structure of a pancreatic ATP-sensitive potassium channel. (A) The KATP-channel is a hetero-octameric complex composed of 4 Kir6.2 subunits and 4 SUR1 units. The transmembrane domains are highlighted. (B) The genetic variants in our 2 cases are located on the same transmembrane domain (TMD1) of the SUR1 subunit.

Table 1.

Clinical and genetic characteristics

Characteristic Case 1 Case 2 Reference values
Age at presentation 1st day of life 1st day of life
 Clinical signs of CHI LGA None
 Other signs Malrotation, volvulus None
Laboratory results
 Glucose (mmol/L) <0.1 <0.1 2.5–6
 Insulin (mU/L) 349.1 50.4 2.8–13.5
 C-peptide (µg/L) 14.6 ND 1.0–3.1
 BHB (µmol/L) <10 <10 <400
 FFA (mmol/L) <0.1 ND 0.33–0.62
Maximal IV glucose required (mg/kg/min) 19 21
Diazoxide treatment
 Dose (mg/kg/day) 10 5
 Duration 2 Years 15 Months
Genetic characteristics
 Location ABCC8 (exon 12) ABCC8 (exon 12)
 Mutation type Missense Missense
 Nucleotide change c.1801G>A c.1780T>C
 Protein change p.(Val601lle) p.(Ser594Pro)
 Inheritance AR (homozygous) AD (heterozygous)
In silico prediction
 PolyPhen-2 Possibly damaging Benign
 PANTHER Probably damaging Probably damaging

CHI, congenital hyperinsulinism; LGA, large for gestational age; BHB, beta-hydroxybutyrate; FFA, free fatty acid; IV, intravenous; ND, not described; AR, autosomal recessive; AD, autosomal dominant.

Table 2.

Case 2: Oral glucose tolerance test

Time (min) Proband
Proband’s mother
Blood glucose (mmol/L) Insulin (μU/L) Blood glucose (mmol/L) Insulin (μU/L)
0’ 4.8 7.7 5.9 10.7
30’ 7.7 58.8 13.8 185.5
60’ 6.6 33.2 11.1 180.7
120’ 3.1 7.3 3 50.1