Sodium bicarbonate and intubation in severe diabetic ketoacidosis: are we too quick to dismiss them?

Management of diabetic ketoacidosis (DKA) has internationally established guidelines. However, management of severe, refractory DKA with multiple contributors to acidosis, and management of DKA in patients with altered mentation, remain ambiguous. Use of sodium bicarbonate and intubation in DKA are unpopular treatment practices, but warrant consideration in these unique clinical scenarios. This paper describes a 61-year-old Sri Lankan female who presented with severe DKA, seizures and altered level of consciousness. In her case, the acidosis was secondary to DKA, hyperlactatemia, hyperchloraemic acidosis and acute kidney injury (AKI). Intravenous sodium bicarbonate was used in the management of acidosis. She was intubated due to altered level of consciousness with inadequate respiratory drive to compensate for metabolic acidosis. The outcome in her case was favorable. Intravenous sodium bicarbonate in DKA should be considered for patients with severe, refractory acidosis with hemodynamic instability, hyperkalemia and compounding acidosis due to normal anion gap acidosis or AKI. Intubation should be considered for patients with obtunded mentation unable to achieve respiratory compensation and obtunded mentation where reversal of DKA is unlikely to improve consciousness. Both strategies should be personalized with consideration of individual risk vs benefit.

There are clearly established international guidelines for management of diabetic ketoacidosis (DKA). In these guidelines, fluid resuscitation and insulin therapy appear at the forefront of management [1,2,3]. However, there are clinical scenarios when DKA is severe and refractory, and complicated with alternate pathologies contributing to acidosis, and altered level of consciousness. Management of these complex clinical scenarios are not clearly outlined in guidelines. In such instances, unpopular management options such as the use of sodium bicarbonate and mechanical ventilation may need to be considered.

Use of sodium bicarbonate is generally frowned upon in the management of DKA. United States (US) guidelines recommend its use if pH is < 6.9 [1]. However, multiple studies have found no overall benefit of the use of sodium bicarbonate in patients with DKA. Studies have in fact, identified multiple risks of its use [4]. Intubation in DKA is also associated with multiple risks including cardiac arrest during intubation. Existing guidelines are not clear on the indications for intubation in DKA and the dos and don’ts of intubation in DKA [5].

This case report will describe the case of a 61-year-old Sri Lankan female who presented with severe DKA, seizures and altered level of consciousness. She had refractory acidosis with combined normal and high anion gap acidosis. Contributors to acidosis in her case were DKA, hyperlactatemia, hyperchloraemic acidosis due to use of normal saline and acute kidney injury (AKI).

Two questions arose during the management of this patient. One was the place for early initiation of sodium bicarbonate in DKA, as she had refractory acidosis with haemodynamic instability and alternate contributors to acidosis apart from DKA. The second question, was the place for intubation in DKA.

The author hopes that the discussion that follows will answer questions regarding these ambiguous areas in DKA management, and will generate more studies leading to changes in management practices.

A 61-year-old Sri Lankan female presented to the emergency department with several episodes of vomiting and drowsiness over 6 h. There was no fever, headache or an identifiable focus of infection. There was no trauma to the head and no history of toxin ingestion.

Her comorbidities included ketosis prone diabetes mellitus, bronchial asthma and hypertension. There was a recent history of missing insulin doses.

On examination, her Glasgow Coma Score (GCS) was 5/15 and pupils were bilaterally reactive. There was no recorded temperature and no neck stiffness. Pulse rate was 101 beats per minute with cold peripheries and a blood pressure of 92/58 mmHg. Lungs were clear with a saturation of 96% on room air. She was hyperpnoeic with a respiratory rate was 32 cycles per minute. The abdomen was soft and a limited neurological examination revealed no focal neurological deficits.

Capillary blood sugar on admission was high index. Initial venous blood gas (VBG) showed a severe high anion gap metabolic acidosis, with serum ketone bodies of 6 mmol/L. Thus, a diagnosis of severe DKA was established and management was started according to standard guidelines with fluid resuscitation and insulin infusion. The blood gas trends during the management are shown in Table 1.

In the first hour, important treatments were fluid resuscitation with 30 ml/hour of normal saline, insulin infusion at 6 units per hour and standard hyperkalaemia management.

In the second hour, she was started on inotropic support with noradrenaline due to persistent haemodynamic instability and the insulin infusion was increased to 8 units/hour due to inadequate decrease in glucose. Additionally, in the second hour, she developed 2 episodes of generalized tonic–clonic seizures which were managed with benzodiazepines and intravenous leveteracetam.

By the third hour, she was haemodynamically stable on inotropes, but glucose level was still high. The insulin infusion was increased to 12 units per hour. There was no improvement in in the GCS and respiratory rate was persistently high (30–40 cycles per minute). The VBG at the third hour showed combined normal and high anion gap metabolic acidosis; this was attributed to be due to fluid resuscitation with 0.9% NaCl. Considering the contribution by normal anion gap acidosis (NAGMA), intravenous 8.4% sodium bicarbonate of 100ml was given over 1 h.

After 4 h of management at the emergency department, the patient was escalated for care at the Intensive Care Unit (ICU). She was intubated due to persistently low GCS and ventilated with synchronized intermittent mandatory ventilation support. Additionally, she was treated with isotonic sodium bicarbonate infusion of 50 ml per hour due to the ongoing NAGMA and newly identified AKI. Summary of her investigations are shown in Table 2.

The patient recovered from DKA 24 h after ICU care, and was extubated 48 h later.

Precipitants for DKA in this admission were poor compliance with insulin and urosepsis. The sepsis was managed with intravenous piperacillin tazobactam.

The discussion will explore the indications for two unpopular management options in DKA: the place for early initiation of sodium bicarbonate and the place for intubation.

Place for sodium bicarbonate in management of DKA

Use of intravenous bicarbonate in DKA and alternate illnesses with metabolic acidosis is controversial. Problems associated with bicarbonate use are reduction of oxygen delivery to tissues by causing a left shift of the oxygen dissociation curve, paradoxical increase in intracellular acidosis and cerebral spinal fluid acidosis, increased risk of hypokalemia, cerebral oedema, delay in the fall in blood lactate: pyruvate ratio and delay in the fall of ketones [2, 6]. On the other hand, the problems with allowing acidosis to persist are negative cardiovascular and pulmonary effects due to myocardial depression, decreased systemic vascular tone, catecholamine resistance and pulmonary vasoconstriction [4]. There is also a resultant impairment of the immune response and leucocyte function, increasing the risk of infection [4].

While there is conflicting evidence for the use of sodium bicarbonate in metabolic acidosis, there seem to be multiple studies that show benefit of its use in instances of AKI.

A multicentre randomized controlled trial conducted among 389 ICU patients with severe metabolic acidosis (pH <  = 7.2) revealed no reduction in mortality or organ failure with sodium bicarbonate, but in a certain stratum of patients with AKI, there was reduction of day 28 mortality and need for renal replacement therapy [6]. Furthermore, there were no life-threatening complications related to the use of sodium bicarbonate in these patients, although metabolic derangements (hypernatremia, hypokalaemia and hypocalcaemia) were more frequently noted in the bicarbonate group [6].

A study of 1718 septic patients carried out by Zhang et al., further supports the use of sodium bicarbonate in septic patients with AKI (stages 2 and 3) and severe acidosis with a pH less than 7.2 [7]. Improved survival was seen in these specific groups of patients with sodium bicarbonate, although this survival benefit was not carried over to patients with pH >  = 7.2 and stage 1 AKI [7].

Similarly, a meta-analysis carried out in 2019, also shows weak evidence for a possible mortality benefit and improved renal outcomes with sodium bicarbonate in critically ill patients with AKI [8].

With regard to the use of bicarbonate in DKA, a handful of studies are available, but there are no randomized control trials with adequately powered sample sizes [9,10,11,12,13,14,15,16,17,18,19]. These studies concluded a lack of benefit with the use of sodium bicarbonate in DKA with severe acidosis, but only with regard to mortality and the time for resolution of acidaemia [9,10,11,12,13,14,15,16,17,18,19]. It is unclear whether bicarbonate may have improved haemodynamic stability and cardiac-related morbidity in these patients. Furthermore, these studies had very small sample sizes, used variable dosing regimens of bicarbonate, and lacked consistent data with regard to alternate contributors to acidosis. A summary of the studies on the use of bicarbonate in DKA is given in Table 3.

Considering the harmful consequences of ongoing metabolic acidosis, some DKA guidelines such as the US guideline and the Sri Lankan guideline make a case in favour of the use of sodium bicarbonate in severe refractory acidosis [1, 3]. Furthermore, it appears that the use of bicarbonate in DKA arises in instances with alternate contributors to acidosis, such as in AKI and hyperchloraemic NAGMA [4]. None of the studies mentioned in Table 3 have adequately looked into the occurrence of these causes as contributors to acidosis and the use of bicarbonate in these instances. Therefore, there is still a dearth of adequate research with randomized controlled trials, using proper patient selection, in this area.

From the available evidence, there is a potential role for sodium bicarbonate in the recovery phase of DKA for these two indications: in instances of hyperchloraemia due to fluid resuscitation that will offset the correction of acidosis resulting from DKA resolution and in the presence of AKI [4].

It is difficult to comment on whether sodium bicarbonate played a role in the improvement of this patient, who had compounding AKI and NAGMA, in addition to ketoacidosis. In either case, it certainly raises interesting questions with regard to the place for sodium bicarbonate in DKA.

The author feels that while fluid resuscitation and insulin therapy must remain at the forefront of DKA management, sodium bicarbonate may be considered (not necessarily always given), early rather than late, in patients that have severe metabolic acidosis with haemodynamic instability, AKI, NAGMA and hyperkalemia. Calculation of the delta ratio must therefore be routinely done to identify co-existent NAGMA.

The recommended administration of sodium bicarbonate is 50 mmol in 200 ml of sterile water to be administered over 1 h [6]. This can be doubled and infused over 2 h until pH is > 7 [6]. 10 mmol of KCL can also be considered to be added to each 200 ml due to the expected hypokalaemia with sodium bicarbonate [6].

Place for intubation in DKA

Patients with DKA are at risk of respiratory failure due to pneumonia, acute respiratory distress syndrome (ARDS) and pulmonary edema [20]. Two types of pulmonary edema have been recognized in DKA: one due to raised pulmonary venous pressure and one due to increased capillary permeability [20].

During DKA, patients develop hyperventilation as a compensatory mechanism, and once they reach the point of Kussmaul’s breathing, they are at risk of respiratory muscle fatigue and ARDS, due to hyperpnoea [16]. Furthermore, a certain percentage of patients who are comatose either due to the severity of DKA or due to an alternate insult, may be unable to generate respiratory alkalosis sufficient enough to compensate for the existing metabolic acidosis [20]. These patients are candidates to be considered for intubation.

However, multiple problems exist with intubation of DKA patients. These are presence of acidosis and hypotension in DKA, worsening of acidosis during sedation and/or paralysis due to rise in carbon dioxide, high risk of aspiration due to gastroparesis and vomiting, possible worsening of hyperkalaemia when using succinylcholine for rapid sequence intubation, difficulty matching the degree of respiratory compensation with ventilator settings and risk of lung injury with high pressure ventilator settings [20, 22].

Steps to overcome the above are [20,21,22]:

1. 1.

   Best possible resuscitation with fluids, insulin and if indicated sodium bicarbonate prior to intubation

2. 2.

   Placement of a nasogastric tube and aspiration prior to intubation

3. 3.

   Rapid sequence intubation with cricoid pressure

4. 4.

   Use of drugs with minimal effects on cardiovascular stability

5. 5.

   Tidal volume of 8 ml/kg based on ideal body weight and respiratory rate similar to the patient’s compensating respiratory rate

The author suggests consideration of intubation for patients with obtunded mentation unable to achieve respiratory compensation and alternate indications for intubation (for example, status epilepticus or alternate pathologies that hinder recovery of GCS despite resolution of DKA). However, it is important to bear in mind the risks of intubation and follow the above steps in order to mitigate said risks.

Use of sodium bicarbonate and intubation in DKA have remained poorly explored treatment areas in literature and guidelines. The use of sodium bicarbonate in DKA should be considered for patients with severe refractory acidosis with hemodynamic instability, hyperkalemia and alternate contributors for acidosis through NAGMA or AKI. The author recommends routine calculation of the delta ratio to help guide management in this regard. Consideration of intubation should be reserved for patients unable to achieve respiratory compensation due to obtunded mentation and patients with altered level of consciousness due to alternate pathologies where DKA reversal is unlikely to improve GCS. Both treatment strategies should be considered on an individual basis with a careful reflection of risk vs benefit.

All data generated or analyzed during this study are included in this published article [and its supplementary information files].

AKI:

Acute Kidney Injury

CRP:

C Reactive Protein

DKA:

Diabetic ketoacidosis

GCS:

Glasgow Coma Score

Hb:

Haemoglobin

ICU:

Intensive Care Unit

INR:

International Normalised Ratio

NAGMA:

Normal Anion Gap Metabolic Acidosis

NCCT:

Non Contrast Computed Tomography

PaCO2:

Partial pressure of carbon dioxide

PLT:

Platelet count

S.Cr:

Serum creatinine

UFR:

Urine Full Report

US:

United States

VBG:

Venous Blood Gas

WBC:

White Blood cell Count

None.

None.

Authors and Affiliations

1. Professorial Medical Unit, National Hospital of Sri Lanka, Colombo, Sri Lanka

   Manudi Vidanapathirana

Contributions

MV-Conceptualization and writing the main manuscript.

Corresponding author

Correspondence to Manudi Vidanapathirana.

Ethics approval and consent to participate

Not applicable.

Consent for publication

Informed written consent for publication was obtained from the patient (The authors are able to provide proof if required).

Competing interests

None.

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