A Case Report of Hyperosmolar Hyperglycemic State
A Case Report of Hyperosmolar Hyperglycemic State
A Case Report of Hyperosmolar Hyperglycemic State
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Cho, Young Min MD; Park, Byung Sung MD; Kang, Min Jae MD, PhD*
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Abstract
Rationale:
A hyperosmolar hyperglycemic state (HHS) is a rare presentation of a hyperglycemic crisis in children with
diabetes mellitus. As this condition can be fatal and has high morbidity, early recognition and proper
management are necessary for a better outcome. Here, we report a rare case of HHS as the first
presentation of type 1 diabetes mellitus (T1DM) in a 7-year-old girl.
Patient concerns:
The patient was admitted due to polyuria and weight loss in the past few days. The initial blood glucose
level was 1167mg/dL.
Diagnoses:
On the basis of clinical manifestations and laboratory results, she was diagnosed with T1DM and HHS.
Interventions:
Treatment was started with intravenous fluid and regular insulin.
Outcomes:
She was discharged without any complications related to HHS and is being followed up in the outpatient
clinic with split insulin therapy.
Lessons:
As the incidence of T1DM is increasing, emergency physicians and pediatricians should be aware of HHS to
make an early diagnosis for appropriate management, as it can be complicated in young children with
T1DM.
1 Introduction
Type 1 diabetes mellitus (T1DM) is characterized by low or no endogenously produced insulin due to
autoimmune destruction of pancreatic beta-cells. The incidence of T1DM in children and adolescents <15
years old has increased worldwide.[1,2] The incidence varies greatly among countries, with the highest
incidence in Finland, and a very low incidence in Asia.[1] However, countries with a traditionally low
incidence of T1DM have shown a tendency for a rapid increase in children and adolescents.[3] One study
showed a 2.33-fold increase in the incidence of T1DM in Korea during 1995 to 2000 and 2012 to 2014.[4]
As T1DM is increasing significantly, diabetic ketoacidosis (DKA) and hyperosmolar hyperglycemic state (HHS)
are emerging as a life-threatening hyperglycemic crisis. The prevalence of DKA among children <15 years of
age with T1DM in the EURODIAB study was 33%.[5] However, the incidence of DKA with new-onset T1DM is
15% to 67% depending on the country and geographical region.[6] Most cases of HHS are seen in elderly
patients with type 2 diabetes, and HHS is extremely uncommon as the first presentation of T1DM.[7,8] It is
not easy to distinguish DKA and HHS from a patient's history because of their similar characteristic
features. However, there are definite differences between their diagnostic criteria. HHS presents as severe
hyperglycemia, hyper-osmolality, with no evidence of severe ketosis or acidosis. Although HHS is a rare
presentation of childhood diabetes, the importance of proper management cannot be emphasized enough
due to the high mortality rate.[9]
Here, we report a rare case of HHS as the first presentation of T1DM in a 7-year-old child, which is younger
than previous reports,[10] and discuss the importance of early identification of hyperglycemic crisis in
severely dehydrated children.
2 Case description
A 7-year-old girl visited the emergency department with severe polyuria. She had a 3-day history of
frequent urination (3–4 times every hour), polydipsia, and lethargy. Although she drank more beverage than
usual, she felt excessive thirst and lost weight from 22 to 19.6 kg in 7 days. She had recently moved to a new
house and was having a hard time fitting in at the new school. She was previously healthy with no past
admissions or serious illness. She had no change of eating habits and lifestyle recently. No history or
family history of endocrine disease including diabetes mellitus was reported. At admission, her height was
127.4 cm (50th–75th percentile), weight was 19.6 kg (5th–10th percentile), and body mass index (BMI) was
12.08 kg/m2 (<first percentile). Her temperature was 37.2°C, heart rate was 88 beats/min, respiratory rate
was 18 beats/min, blood pressure was 100/60 mm Hg, and pulse oximetry was 100% on room air. Her
mental status was alert, sensation was intact, and motor strength was quite good considering her
condition. However, she looked cachectic and lethargic. Her glucose level was too high to check with a
capillary blood glucose meter, so a blood test was performed and rehydration therapy with intravenous
fluid (isotonic saline 10 mL/kg loading dose for 1 hour) was started immediately (Table 1). Initial
biochemistry results demonstrated severe hyperglycemia (1167 mg/dL), hyperosmolality of 350 mOsm/kg
(effective osmolality 311 mOsm/kg), mild acidosis (venous pH 7.34), hyponatremia (sodium 123 mmol/L;
corrected for blood glucose: 140 mmol/L), severe glycosuria, and mild ketonuria.
T1-84
On the basis of the laboratory results, intensive intravenous fluid and regular insulin were administered
and laboratory examinations were performed every 2 hours to check and modulate electrolyte changes.
Serum glucose level decreased approximately 60 mg/dL/h and normalized to 115 mg/dL 17 hours after
treatment started, which led a gradual decrease in serum osmolality (Fig. 1). No evidence of acidosis or
severe ketosis confirmed the diagnosis of HHS. A neurological examination and brain computed
tomography scan were performed to check for complications of HHS, but no cerebral edema was found.
F1-84
The laboratory results that confirmed the diagnosis of T1DM were as follows: glycated hemoglobin (HbA1c),
15.6% (reference, <5.6%); C-peptide, 0.12 ng/mL (reference, 1.10–4.40 ng/ml); anti-GAD antibody, 2.4 U/mL
(reference, ≤9.0 U/mL); anti-insulin antibody, 4.9% (reference, ≤7.0%); anti-islet cell antibody, negative; and
24-hour urine c-peptide, 4.5 μg/day (reference, 17.2–181.0 μg/day). All parameters of other hormone group
were within normal range; triiodothyronine, 86.23 ng/dL (reference, 80.00–200.00 ng/dL); free thyroxine,
1.40 ng/dL (reference, 0.70–2.00 ng/dL); thyroid-stimulating hormone (TSH), 2.78 μIU/mL (reference, 0.5–4.5
μIU/mL); anti-thyroglobulin, 25.30 IU/mL (reference, ≤115.00 IU/mL); anti-microsome, 5.19 IU/mL (reference,
≤34.0 IU/mL); anti-TSH receptor 0.40 IU/L (reference, ≤1.75 IU/L).
After a 13-day hospital stay that included blood glucose control and T1DM education, she was discharged
without any symptoms. Anthropometric measurements at discharge were height, 127.0 cm (50th–75th
percentile); weight, 24.0 kg (25th–50th percentile); and BMI, 14.88 (29th percentile). She is being followed-up
in the outpatient clinic regularly with split insulin therapy (Neutral protamine Hagedorn and regular
insulins) and self-glucose monitoring. At recent visits (4 months after discharge), her HbA1c level was 7.1%,
and she was maintaining blood glucose within the target range.
3 Discussion
A rise in the incidence of T1DM has been observed globally in recent decades.[1,6] Approximately 86,000
children <15 years old are estimated to develop T1DM annually worldwide.[11] In Asia, particularly Korea, the
incidence of T1DM was very low compared with other continents and nations (approximately 1.36 per
100,000 person-years in 1995–2000). [12] However, 1 study reported a significant increase of 3.19 per 100,000
person-years in 2012 to 2014,[4] which means Korea will not remain a diabetes-safe country in a few years.
DKA and HHS are the most serious acute hyperglycemic emergencies among DM complications.
Hyperglycemia in a patient with DKA results from increased hepatic and renal glucose production and
impaired peripheral glucose utilization leading to osmotic diuresis and electrolyte imbalance. Ketonemia
and metabolic acidosis are the consequences of increased lipolysis and ketoacid production.[13] Different
from DKA, HHS commonly occurs after a prolonged and gradual increase in polyuria and polydipsia,
resulting in profound dehydration, with fluid losses estimated to be twice those of DKA. This is
accompanied by severe electrolyte loss, also greater than that observed in DKA because of the longer
duration of osmotic diuresis.[8] Hypovolemia eventually occurs due to continued osmotic diuresis, which
leads to a progressive decline in glomerular filtration rate and worsening hyperglycemia.[9]
HHS is a rare presentation in T1DM, particularly in children, which bears a high degree of morbidity and
mortality. Mortality due to HHS has been reported as high as 50% to 60%, and a recent cohort study
reported 30-day mortality of 16%.[14] HHS was first described as an extreme elevation in serum glucose
concentration and hyper-osmolality without significant ketosis or acidosis. HHS usually causes greater
morbidity and mortality than DKA, depending on the severity of dehydration, hyper-osmolality, and patient
age.[9] As a result of insulin deficiency and increasing levels of counter-regulatory hormones, increased
gluconeogenesis and conversion of glycogen to glucose create blood hyperglycemia.[9] In a hyperglycemic
state, the glycosuria uses a large volume of water and electrolytes are loss by urination, leading to a
hyperosmolar condition. Thus, osmolality is useful as an indicator of HHS severity and for monitoring the
rate of change with treatment in the hyperosmolar state.[15] If osmolality cannot be measured frequently, it
should be calculated using a formula.[16]
The classic presentation of HHS in children is an obese adolescent with type 2 diabetes. However, recent
studies have reported a few cases of HHS in T1DM or HHS in nonobese patients.[7,8,17] One study reported 71
patients with HHS from 2001 to 2008; 49 were obese adolescents as a classic presentation of HHS. However,
the remaining patients were not obese and younger than those in the obese group. Although T1DM was
predominant in nonobese survivors, T2DM was overwhelmingly present in the obese group.[8]
Some differences exist in the treatment of DKA and HHS; however, intensive fluid hydration is important as
initial management for both conditions. Hydration by isotonic solution is recommended at 10 to 20
mL/kg/h during the first hour. Initial hydration usually decreases the glucose concentration by reducing
counter-regulatory hormones and improving renal perfusion. During this process, plasma sodium levels
should be monitored to prevent cerebral edema or central pontine myelinolysis as a complication given the
rapid correction in blood osmolarity. Serum sodium level can change on the basis of the pre-existing high
glucose level and therefore needs to be corrected to reflect the actual situation in the body. Increased
extracellular fluid (ECF) osmolality in hyperglycemic states forces water to move to the ECF, which decreases
serum sodium in proportion to dilution of the ECF. This mechanism is called translational hyponatremia
and returns to normal when glucose drops (Fig. 2). Fluid deficits should be corrected gradually over 48
hours, aiming for 12% to 15% correction with a goal of promoting a gradual decline in serum sodium and
osmolality. Serum osmolality in our case was maintained at a similar level for several hours and then
decreased gradually (Fig. 1).
Figure 2: Serum sodium and corrected sodium levels during treatment are
shown. Initial serum sodium level was low at 123 mmol/L, but the
corrected sodium level was in the normal range at 140 mmol/L. Sodium
level was normalized after serum glucose level was lowered.*Corrected Na
= Na + (Glucose – 100) × 0.016.
After initial hydration therapy is completed, intravenous rapid insulin should be administered to decrease
the glucose level and resolve the metabolic acidosis. Insulin should be started after the initial fluid
expansion to avoid the risks of severe hypokalemia and an excessive decrease in serum osmolality.[18] The
management strategy may differ with insulin infusion rates of 0.1 unit/kg/h in patients with DKA and 0.05
unit/kg/h in those with HHS. [18] Although our patient started with insulin infused at 0.1 unit/kg/h as for
DKA, we lowered the insulin rate after diagnosing HHS considering no evidence of severe acidosis and the
rapidly improved mild ketonuria.
HHS can cause serious complications, such as brain edema and rhabdomyolysis.[19] Although cerebral
edema is rarely seen in these cases except in children or in patients with pure HHS,[20] a neurological
examination and radiological study should be considered, as the condition can be fatal. Severe
dehydration and hyperviscosity of the blood increase the risk of thromboembolism in patients with HHS.
Rhabdomyolysis, acute renal failure, and malignant hyperthermia are other reported complications and
warrant monitoring of renal function and creatine kinase levels.[18]
The limitation of this case was that the reason of the sudden onset of T1DM was obscure. The gene study
including human leukocyte antigen (HLA) typing was not performed due to the high cost. She recently had
some social stress, but this is hard to prove. Therefore, further genetic evaluation might be needed
especially in nonautoimmune T1DM. Nevertheless, our case is valuable, as we experienced that nonobese
children with T1DM can present with HHS at a young age. Therefore, emergency physicians and
pediatricians should be aware of HHS and to make an accurate diagnosis of the hyperglycemic crisis, which
could be complicated in children with T1DM.
Acknowledgment
The authors thank the patient for permitting us to report this case.
References
[1]. The DIAMOND Project Group. Incidence and trends of childhood type 1 diabetes worldwide 1990-1999. Diabet Med
2006;23:857–66.
Cited Here
[2]. Patterson CC, Gyürüs E, Rosenbauer J, et al. Trends in childhood type 1 diabetes incidence in Europe during 1989-2008:
evidence of non-uniformity over time in rates of increase. Diabetologia 2012;55:2142–7.
Cited Here
[3]. Craig ME, Jefferies C, Dabelea D, et al. ISPAD Clinical Practice Consensus Guidelines 2014. Definition, epidemiology, and
classification of diabetes in children and adolescents. Pediatr Diabetes 2014;15(suppl 20):4–17.
Keywords:
child; diabetes mellitus type 1; hyperglycemic hyperosmolar nonketotic coma
Copyright © 2017 The Authors. Published by Wolters Kluwer Health, Inc. All rights reserved.
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