Diabetic Ketoacidosis and New Onset Diabetes
Diabetic Ketoacidosis and New Onset Diabetes
Diabetic Ketoacidosis and New Onset Diabetes
Hadil A Al Otair1*, Eman Sheshah2, Bashayer Zuhair Al Shirah1 and Anwar Jammah1
1
Department of Medicine, King Khalid University Hospital-King Saud University Medical City, Saudi Arabia
2
Endocrinology and Diabetes Center, King Salman Hospital, Saudi Arabia
Submission: August 17, 2020; Published: August 24, 2020
*Corresponding author: Hadil A Al Otair, MBBS, MRCP (UK), EDRM, Consultant- Internal Medicine, Department of Medicine, King Khalid University
Hospital, King Saud University Medical City, PO Box 2925, Riyadh 11461, Saudi Arabia
Abstract
Background: Diabetes Mellitus have been reported frequently in patients with the new corona virus disease- 2019, COVID- 19. It has been
associated with progressive course and worse outcome. Recently, case reports and small cross-sectional studies described diabetic patients
who develop diabetic ketoacidosis (DKA) when infected with COVID -19. The incidence of DKA has been found to be high in patients with type 1
(T1DM) and type 2 diabetes Mellitus (T2DM) admitted to hospital with COVID-19.
Case presentation: We present a 47-year-old patient who was not known to have DM but presented with generalized body aches, fatigue
and nocturia 4 days prior to admission. His lab results showed high blood glucose, high anion gap metabolic acidosis and ketonuria diagnostic
of DKA. He also tested positive for COVID-19 and his Chest X-Ray was consistent with Covid 19 Pneumonia. He was successfully managed with
Intravenous fluids and Insulin as per DKA protocol. He required intravenous antibiotics, steroids and high flow oxygen for COVID 19 pneumonia.
He was discharged after 16 days in stable condition.
Conclusion: COVID-19 infection can be complicated by DKA and development of DM in previously non-diabetic individuals. Very few cases
have been reported in the literature on COVID-19 infection precipitating DKA in a newly diagnosed patient of diabetes mellitus type II.
Abbreviation: DKA: Diabetic Ketoacidosis; DM: Diabetes Mellitus; T1DM: Diabetes Mellitus Type 1; T2DM: Diabetes Mellitus Type 2; ACE2:
Angiotensin-Converting Enzyme 2; SARS-CoV-2: Severe Acute Respiratory Syndrome-Coronavirus-2; COVID-19: Corona Virus -19; ICU: Intensive
Care Unit; CRP: C-Reactive Protein; LDH: Lactate Dehydrogenase; Na: Sodium; Cl: Chloride; K: Potassium; BUN: Blood Urea Nitrogen; Hgb:
hemoglobin; ECG: Electrocardiogram; ED: Emergency Department
Introduction
in 2006 [6]. Binding of ACE2 by SARS-CoV-2 in COVID-19 may
During COVID-19 pandemic, patients with previous history
play an important in the pathogenesis of the disease on one hand
or underlying cardiovascular condition were at higher risk for
and could predispose patients to hyperglycemia and development
developing severe symptoms and poor prognosis. Diabetes Mellitus
of DM on the other hand. Herein, we describe a patient who was
in particular, was found to be a risk factor for severe disease [1].
previously healthy, but presented with DKA and new onset of DM
A history of diabetes was associated with 22.5% of COVID-19 ICU
complicating COVID-19 pneumonia.
admissions in one case series [2] and a mortality rate up to 16%
among people with diabetes and without other comorbidities [3]. Case Presentation
The development of DKA can in itself add to this high mortality
A 47 years old, gentleman, medically free has presented to the
in COVID -19 patients, Recent studies have demonstrated that
emergency department (ED) with fatigue and decrease in activity
COVID-19 can utilize angiotensin-converting enzyme 2 (ACE2) on
for 4 days along with generalized body aches and nocturia (about
the surfaces of epithelial cells to bind and gain entry to infected
6-7 times/day). He went to a private health-care centre, where his
cells [4,5]. Similar findings were reported during SARS outbreak
blood sugar was measured and was 15.5mmol/l.
h) Lymphocytes: 0.20 x 10^9/L. The patient in this case report presented with DKA and newly
diagnosed type 2 DM triggered by COVID 19 pneumonia. The
i) Hgb: 166gm/L, normal range (130-180). underlying pathophysiology of glucose intolerance and its severe
j) platelets: 177.9 x 10^9/L, normal range (140-450). form DKA in Patients with COVID 19 is still not well understood.
k) Chest x-ray: showed bilateral infiltration. The severe acute respiratory syndrome-coronavirus-2 (SARS-
CoV-2), responsible for COVID‐19, uses ACE2 receptor to bind
l) Insulin 14.9mIU/L, normal range (2.6-37.6mIU/L). and enter to infected cells as a viral complex [5]. ACE2 is located
m) C-peptide 0.5(nmol/L), normal range (0.16-1.68nmol/L). in many organs including the heart, kidney, lung, and intestinal
tissues where it converts angiotensin II to angiotensin 1. The
n) HbA1C: 6.2 %. clinical manifestations of SARS can be explained by the expression
Oronasal swab was positive for Covid-19 by real-time reverse of ACE2 in various organs. In the pancreas, it was found that
transcription-polymerase chain reaction (rRT -PCR) test (this ACE2 is expressed in the endocrine part of the pancreas. This
is used with Roche MagNA Pure-96 (MP96) using MagNA Pure suggests that SARS coronavirus enters islets cells using ACE2 as
96 DNA and Viral NA Small Volume Kit and Applied Biosystems its receptor and damages B-cell islets leading to insulin deficiency
QuantStudio7 Flex (QS7). and development of acute diabetes [6]. This is supported by the
findings of strong immunopositivity for ACE2 in pancreatic islets
Inflammatory markers:
while exocrine tissues were only weakly positive [9]. Similarly,
a) D dimer: 0.60mcg/ml, normal range (0.22-0.45). evidence in diabetic mice demonstrated that ACE2 activity levels
were enhanced in the pancreas [9,10].
b) LDH: 193unit/L, normal range (87-241).
In addition to the direct B cell injury, the expression of
c) Ferritin: 1694.2mcg/L, normal range (30-400).
ACE2 on the surface of the pancreas is downregulated following
d) CRP: 124mg/L, normal range (< 10mg/l Negative, endocytosis of the virus-ACE2 receptor complex This in turn
How to cite this article: Hadil A A O, Eman S, Bashayer Zuhair A S, Anwar J. Diabetic Ketoacidosis and New Onset Diabetes Mellitus Precipitated by
0070
COVID-19 Infection. JOJ Case Stud. 2020; 11(3): 555815. DOI: 10.19080/JOJCS.2020.11.555815
Juniper Online Journal of Case Studies
can lead to increase concentration of angiotensin II and inhibit factor for the progression and prognosis of COVID‐19. Diabetes Metab
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explain the underlying mechanism and pathophysiology of DKA. of COVID-19-associated diabetic ketoacidosis in UK secondary care.
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(2020) SARS‐CoV‐2 Cell Entry Depends on ACE2 and TMPRSS2 and
Whether these changes are transient or permanent remains to be Is Blocked by a Clinically Proven Protease Inhibitor. Cell 181(2): 271.
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How to cite this article: Hadil A A O, Eman S, Bashayer Zuhair A S, Anwar J. Diabetic Ketoacidosis and New Onset Diabetes Mellitus Precipitated by
0071
COVID-19 Infection. JOJ Case Stud. 2020; 11(3): 555815. DOI: 10.19080/JOJCS.2020.11.555815