key: cord-0073373-sudqq19h
authors: Kho, Sze Shyang; Nyanti, Larry Ellee; Muhammad, Noorul Afidza; Nasaruddin, Mona Zaria; Abdul Rahaman, Jamalul Azizi
title: The more you give, the worse it gets
date: 2021-09-03
journal: Breathe (Sheff)
DOI: 10.1183/20734735.0083-2021
sha: 50ca9eb85e7f6ce0b977723307afb099c467790a
doc_id: 73373
cord_uid: sudqq19h

Persistent tachypnoea despite resolution of bronchospasm in a patient with acute asthma exacerbation after administration of inhaled short acting β(2)-receptor agonist should alert the clinician to this potential diagnosis. https://bit.ly/385VU2Q

A 33-year-old, female nonsmoker presented to our unit with 2 days of worsening breathlessness associated with sore throat, nonproductive cough, wheezing and chest tightness. She was a homemaker with three children, of whom the eldest had asthma. Further questioning revealed a pattern of intermittent and variable symptoms frequently triggered by exposure to cold and dust, with clear symptom-free intervals. Four of her episodes required outpatient visits for nebulisation in the preceding 2 months, resulting in transient control of her symptoms. Despite this, she was not on maintenance therapy and had only self-administered continuous doses of inhaled salbutamol prior to current presentation. She had no other chronic medical illnesses, was not on any prescribed medications and denied taking supplements or illicit substances.

On physical examination, she was conscious and orientated but spoke in short phrases, demonstrated audible wheezing and was visibly tachypnoeic, with a respiratory rate of 40 breaths per min. She had a blood pressure of 175/125 mmHg, heart rate of 110 beats per min, oxygen saturation (SpO 2 ) of 94% under room air and temperature of 36.5°C. Lung auscultation revealed generalised polyphonic wheeze with reduced air entry bilaterally. As all potential cough-inducing respiratory testing was suspended due to the COVID-19 pandemic in our local setting, her peak expiratory flow rate (PEFR) was not evaluated throughout the admission [1] . A plain chest radiograph was performed in the emergency unit (figure 1). Laboratory investigations revealed normal haemoglobin level with slightly raised total white cell and platelet counts. Renal and liver function tests were normal. Most serum electrolytes were within the normal range except for low serum phosphate and magnesium levels. The initial laboratory investigations are presented in 

Describe the plain chest radiograph in figure 1. A diagnosis of severe acute exacerbation of bronchial asthma was made. The PCO 2 was slightly lower than the expected level of 35.6±2 mmHg (4.7±0.2 kPa) as calculated by Winter's formula, suggesting respiratory overcompensation [2] .

Initial resuscitation in the emergency department consisted of 200 mg intravenous hydrocortisone and 5 mg nebulised salbutamol, followed by another 5 mg nebulised salbutamol and 0.25 mg ipratropium. In view of raised serum lactate (4.40 mmol·L −1 ), 500 mL intravenous 0.9% normal saline was administered. Upon reassessment, her vital signs stabilised with reduction of heart rate to 88 beats per min, blood pressure of 143/85 mmHg, saturation of 100% under room air and respiratory rate of 20 breaths per min. She was able to speak in full sentences with improved air entry on lung auscultation. However, repeat arterial blood gas analyses showed worsening metabolic acidosis with pH of 7.30, PO 2 85.5 mmHg (11.4 kPa), PCO 2 20.0 mmHg (2.6 kPa), HCO 3 − 9.7 mmol·L, base excess −14.1 mEq·L −1 and lactate of 8.21 mmol·L −1 with calculated anion gap of 26.8 mmol·L −1 . Clinically, she was well hydrated, as evidenced by a capillary refilling time <2 s, good skin turgor and noncollapsible inferior vena cava on ultrasound assessment. Urgent plasma paracetamol (<4.00 mg·L −1 ) and salicylate level (<0.36 mmol·L −1 ) were not detectable.

Type A lactic acidosis was unlikely as there were no features to suggest hypoperfusion or hypovolaemia. Furthermore, as serum lactate level continues to rise despite improved respiratory effort after resuscitation, hypophosphataemia and respiratory muscle fatigue contributing to worsening lactic acidosis were deemed less likely. Laboratory assessment also confirmed normal liver and renal function, which ruled out lactic acidosis secondary to liver and renal dysfunction. In the absence of illicit substance use or prescription medicines such as antidepressants, antiepileptics or metformin, accidental drug overdose was ruled out. Thus, the most likely diagnosis to explain the worsening high anion gap lactic acidosis was SILA.

Inhaled salbutamol was immediately halted, while metered-dose inhaler (MDI) ipratropium bromide was continued via a valve holding chamber. Nasal prong oxygen was initiated at 2 L·min −1 . She was empirically commenced on broad spectrum intravenous antibiotic (ceftriaxone 2 g once daily) for occult sepsis in view of the hyperlactataemia. 

What is the most likely explanation of the worsening high anion gap lactic acidosis?

What is the next most appropriate course of treatment?

What is the provisional diagnosis?

What would be the initial treatment for this patient? The more you give, the worse it gets

The patient improved gradually and was eventually started on maintenance and reliever therapy with budesonide 160 μg/formoterol 4.5 μg, two puffs twice daily and as needed, via dry-powder inhaler on the ward. 8 h after admission, venous blood gas analysis showed further improvement, with serum HCO 3 − 20 mmol·L −1 and serum lactate of 2.00 mmol·L −1 . Blood, sputum culture and nasopharyngeal swab for SARS-CoV-2 PCR were negative. The patient was discharged well 48 h after admission.

Acute exacerbation of asthma is a potentially lifethreatening condition that requires prompt action with close monitoring. Management of asthma exacerbation consists of early introduction of systemic corticosteroids, controlled oxygen therapy and repetitive administration of inhaled SABA [3] . Although highly effective, SABA are not without side-effects, due to increased β-adrenergic drive. Commonly reported side-effects of SABA include tremor, palpitation, tachyarrhythmias, anxiety and hypokalaemia. SILA is rare and has been reported not only in salbutamol overdose but also in therapeutic range doses [4] .

The proposed mechanism of SILA lies in the hyperadrenergic state it induces [5] . Salbutamolinduced hyperadrenergic drive promotes glycolysis, glycogenolysis and gluconeogenesis, which leads to overproduction of pyruvate. Under normal aerobic circumstances, pyruvate is metabolised aerobically through the Krebs cycle and oxidative phosphorylation. However, once this pathway is saturated, pyruvate is shunted and metabolised through the anaerobic pathway into lactate [6] . This hyperadrenergic state also enhances lipolysis, resulting in free fatty acids that inhibit the entrance of pyruvate into the Krebs cycle via inhibition of pyruvate dehydrogenase, thus shunting pyruvate into the anaerobic pathway [6, 7] . Moreover, systemic corticosteroid use frequently induces a state of hyperglycaemia, which potentially provides more substrate for lactic acid production [5] . Corticosteroids also enhance β 2 -receptor sensitivity, perpetuating the vicious cycle of a hyperadrenergic state and increased lactate production [7] .

Lactic acidosis is generally classified into type A and B [8] . The more common type A lactic The more you give, the worse it gets acidosis is associated with tissue hypoxia and hypoperfusion, while the normovolaemic type B is usually associated with drugs or other metabolic derangements such as a hyperadrenergic state [8] . Assessment of lactate to pyruvate ratio (L/P) can be helpful in distinguishing type A from B lactic acidosis. A high L/P ratio signifies impaired tissue oxygenation (type A) while a normal L/P ratio occurs in nonhypoxic states when pyruvate fails to be metabolised at the mitochondrial level (type B) [9, 10] . As pyruvate level was not assessed in our case due to technical difficulties, a hypoxic mechanism leading to lactic acidosis cannot be precisely ruled out. Nevertheless, we postulate that our patient had a predominant type B lactic acidosis as she was not hypoxic during presentation, as evidenced by a PO 2 of 91.7 mmHg (12.2 kPa). Furthermore, there were no clinical features to suggest hypoperfusion, serum lactate also continues to rise despite improvement of respiratory distress. Our hypothesis is also in consistent with a study of paediatric patients admitted to the intensive care unit with severe exacerbation of asthma and concurrent lactic acidosis, in which the majority (88%) of them were found to have a L/P ratio <25, indicating a type B lactic acidosis [11] . In our case, the temporal relationship between the resolution of high serum lactate level with salbutamol withdrawal supports the diagnosis of SILA. Although our patient presented with systemic inflammatory response syndrome with elevated inflammatory markers (raised total white blood cells, C-reactive protein and erythrocyte sedimentation rate), there was no clinical evidence of sepsis and she responded well to initial resuscitation. Furthermore, the patient's blood and sputum cultures were negative; hence, sepsis as a cause of worsening hyperlactataemia is very unlikely. Hyperlactataemia may also be explained by respiratory muscle fatigue from increasing respiratory effort, as well as hypophosphataemia [10, [12] [13] [14] . It is known that hypophosphataemia leads to reduced muscle ATP synthesis, resulting in muscle weakness, impairing diaphragmatic contractility and increasing haemoglobin affinity for oxygen due to decrease in 2,3-diphosphoglycerate level [10, 13, 14] . All these factors eventually lead to tissue hypoxia, perpetuating lactic acidosis in patients with asthmatic exacerbation. We postulate that respiratory muscle fatigue, as a result of respiratory distress and hypophosphataemia, contributed to the initial raised blood lactate level (4.40 mmol·L −1 ) in our patient upon presentation. However, despite initial SABA administration and improving respiratory effort, serum lactate level continued to rise. This temporal relationship is highly suggestive of SILA as the predominant culprit of the subsequent worsening hyperlactataemia in our patient.

Sporadic case reports on SILA have been documented in literature [6, 7, 15, 16] . As there are no specific diagnostic criteria for this rare condition, vigilant clinical assessment and judgement is of utmost importance. The clinician should suspect SILA when a patient demonstrates persistent or worsening tachypnoea despite resolution of bronchospasm after administration of SABA. Lack of awareness of this condition may put patients at risk of the vicious cycle of worsening lactic acidosis and increasing salbutamol administration. Cautious interpretation of blood gas results and clinical correlation is paramount. To the best of our knowledge, risk factors and prevalence of SILA in the adult population have yet to be elucidated in the literature. However, among the paediatric population, 87% of moderate to severe asthma patients had evidence of raised serum lactate level >2.2 mmol·L −1 in a prospective observational study. In that study, older age, higher blood glucose level and salbutamol administered through nebulisation were found to be independent risk factors associated with SILA [5] .

SILA is a rare but recognised adverse effect of inhaled salbutamol. The use of inhaled salbutamol should not be discouraged during an asthma exacerbation as life-saving bronchodilator effects outweigh the risk of this rare adverse event. However, clinicians should be aware of this potential complication and act promptly, keeping in mind that the more you give, the worse it gets.

This chest radiograph in anterior-posterior projection shows mild hyperinflation as evidenced by visualisation of six anterior ribs and 10 posterior ribs above the diaphragm, with no evidence of lobar consolidation, collapse or pneumothorax.

Severe acute exacerbation of asthma with compensated high anion gap metabolic (lactic) acidosis.

The more you give, the worse it gets 

Association for Respiratory Technology and Physiology. Guidelines for recommencing physiological services during the Coronavirus Disease 2019 (COVID-19) endemic phase

Quantitative displacement of acid-base equilibrium in metabolic acidosis

Global Initiative for Asthma. Global Strategy for Asthma Management and Prevention

PubChem Compound Summary for CID 2083

Prevalence and risk factors of lactic acidosis in children with acute moderate and severe asthma, a prospective observational study

Lessons of the month 1: salbutamol induced lactic acidosis: clinically recognized but often forgotten

Beware of beta! A case of salbutamolinduced lactic acidosis in severe asthma

Lactic acidosis

Lactic acidosis: recognition, kinetics, and associated prognosis

Acid-base disturbances in patients with asthma: a literature review and comments on their pathophysiology

Mechanism of lactic acidosis in children with acute severe asthma

Hypophosphatemia promotes lower rates of muscle ATP synthesis

Effect of hypophosphatemia on diaphragmatic contractility in patients with acute respiratory failure

Albuterolinduced lactic acidosis

Salbutamol-induced lactic acidosis in status asthmaticus survivor

None declared.