Dear Sir

We thank Professor Marchetti for his comments on our article in ADC (1). He raises two important questions we wish to comment on.

Regarding which dose of aspirin to use, we are also interested in the suggestion that anti-aggregant doses of aspirin might be a preferred option for the acute inflammatory phase of Kawasaki disease (KD). It is indeed possible that future guidance may recommend low dose aspirin (3-5 mg/kg/day) at all stages of KD, as suggested by the retrospective data referred to by Professor Marchetti (2). Whilst we acknowledge the potential merits of such an approach, particularly in relation to avoidance of toxicity, there has never been a prospective controlled clinical trial to support this and therefore no high-level evidence on which to base firm guidance. Two other practical considerations are worthy of highlighting in relation to aspirin. Firstly, nonsteroidal anti-inflammatory drugs such as ibuprofen, which antagonize platelet inhibition induced by aspirin (3), should be avoided in patients with KD receiving anti-aggregant doses of aspirin. Secondly, although the risk of low dose aspirin (3-5 mg/kg) in being associated with Reye syndrome is unknown, usual advice is to discontinue in the event of inter-current infection.

Regarding the use of corticosteroids for primary treatment of KD, we have been strong advocates of this for several years, as reflected in previously published guidance (4, 5). This is now brought into sharp focus in the light of emerging data from several countries regarding poor coronary artery outcomes despite Intravenous immunoglobulin (IVIG) (1, 6-9). Indeed, the use of corticosteroids as primary adjunctive treatment of patients with severe KD has an increasingly compelling evidence-base.  Despite that and UK guidance that was published halfway during the BPSU survey (5), our study demonstrates that UK paediatricians are not yet widely using corticosteroids for the treatment of KD (1). The soon-to-be published European SHARE (single hub access for rheumatology in Europe) guidance hopefully will improve that situation for high risk cases, but there clearly remains significant equipoise over the use of corticosteroids as adjunctive therapy for unselected cases of KD. Thus, at the time of writing we are currently setting up a major international clinical trial of corticosteroids as adjunctive treatment for unselected KD cases in the UK and Europe, KDCAAP (the Kawasaki Disease Coronary Artery Aneurysm Prevention trial). It is possible that the added potent anti-inflammatory effect of adjunctive corticosteroids for the primary treatment of KD will obviate the need for any further discussion about anti-inflammatory doses of aspirin. We hope that the UK and European paediatric community will recruit patients to this important clinical trial to resolve this issue once and for all.

Professor Robert Tulloh, Bristol Royal Hospital for Children, Bristol, UK

Professor Paul Brogan, Great Ormond Street Hospital, London, UK

1. Tulloh RMR, Mayon-White R, Harnden A, Ramanan AV, Tizard EJ, Shingadia D, Michie CA, Lynn RM, Levin M, Franklin OD, Craggs P, Davidson S, Stirzaker R, Danson M, Brogan PA. Kawasaki disease: a prospective population survey in the UK and Ireland from 2013 to 2015. Archives of Disease in Childhood. 2018.

2. Ho LGY, Curtis N. What dose of aspirin should be used in the initial treatment of Kawasaki disease? Archives of Disease in Childhood. 2017;102(12):1180-2.

3. Catella-Lawson F, Reilly MP, Kapoor SC, Cucchiara AJ, DeMarco S, Tournier B, Vyas SN, FitzGerald GA. Cyclooxygenase inhibitors and the antiplatelet effects of aspirin. N Engl J Med. 2001;345(25):1809-17.

4. Brogan PA, Bose A, Burgner D, Shingadia D, Tulloh R, Michie C, Klein N, Booy R, Levin M, Dillon MJ. Kawasaki disease: an evidence based approach to diagnosis, treatment, and proposals for future research. Arch Dis Child. 2002;86(4):286-90.

5. Eleftheriou D, Levin M, Shingadia D, Tulloh R, Klein NJ, Brogan PA. Management of Kawasaki disease. Arch Dis Child. 2014;99(1):74-83.

6. Mossberg M, Segelmark M, Kahn R, Englund M, Mohammad AJ. Epidemiology of primary systemic vasculitis in children: a population-based study from southern Sweden. Scand J Rheumatol. 2018;47(4):295-302.

7. Lyskina G, Bockeria O, Shirinsky O, Torbyak A, Leontieva A, Gagarina N, Satyukova A, Kostina J, Vinogradova O. Cardiovascular outcomes following Kawasaki disease in Moscow, Russia: A single center experience. Global cardiology science & practice. 2017;2017(3):e201723.

8. Jakob A, Whelan J, Kordecki M, Berner R, Stiller B, Arnold R, von KR, Neumann E, Roubinis N, Robert M, Grohmann J, Hohn R, Hufnagel M. Kawasaki Disease in Germany: A Prospective, Population-based Study Adjusted for Underreporting. Pediatr Infect Dis J. 2016;35(2):129-34.

9. Friedman KG, Gauvreau K, Hamaoka-Okamoto A, Tang A, Berry E, Tremoulet AH, Mahavadi VS, Baker A, deFerranti SD, Fulton DR, Burns JC, Newburger JW. Coronary Artery Aneurysms in Kawasaki Disease: Risk Factors for Progressive Disease and Adverse Cardiac Events in the US Population. Journal of the American Heart Association. 2016;5(9).

Dear Sir/ Editor,

Dr Smith makes relevant and interesting points regarding the terminology used for fluids, which can be used for both “resuscitation” purposes and “maintenance” therapy, and we thank him for his interest and response.

The purpose of this clinical question was to review the current evidence for paediatric patients in relation to “ balanced fluids”, a term emerging in the medical literature. NICE recommends using any isotonic crystalloid, which covers a wide range of sodium concentration from 130 to 154mmol/L (reference 1 in the article).

The loss of electrolytes, either from the gut or as a result of renal impairment, needs regular clinical review. We observe that repeated bicarbonate measurements are not regularly undertaken after initial assessment or following admission and it is important to remind trainees to consider these losses, hence our recommendation of daily monitoring of electrolytes. By following this approach, appropriate individualised adjustments can be made to the fluid prescription of patients as necessary.

Our conclusion from this question highlighted that research needs to be undertaken in the paediatric population of bicarbonate/ lactate containing fluids to determine whether this may affect acute kidney injury and other specific clinical outcomes. We agree attention to detail is always necessary when caring for infants and children receiving intravenous fluids of any type.

Yours sincerely,

Dr Patel & Dr Hulton

Dear authors,

We are kindly observing that the study on hospitalizations for infection due to respiratory syncytial virus should be conducted on infants aged <1 year old [1], and not on infants aged <2 years old. Such a choice is motivated by medical literature and since the prescription of palivizumab on the general population of preterm infants is up to 1 year of age. Moreover, the study does not tightly classify the hospitalization depending on the gestational age, a lack of information that exclude the possibility of a punctual statistical analysis on the infants whose gestational age is between 29-35 weeks, population matter of the analysis, impacted by the AIFA reimbursement limitations.
In the study infants aged <2 years old have been considered, the same subjects are statistically contributing to two consecutive seasons with different ages. The algebraic sum of the season 2014-2015 / 2015-2016 perpetuate the complexity of analysis of hospitalization for a specific season, if the infant is hospitalized in the season of his/her birth or next year.
As reported by Medici et al. [2], respiratory syncytial virus infection has a 2-years evolution, with a less critical year following a year with more abundant virus diffusion. By algebraically summing the data from two consecutive years the seasonality, so the stochasticity, is lost. Eventually the season 2016-2017 appear to be the less critical season. Environmental and patient conditions such as: birth order, birth weight, gestational age, age at onset of the RSV season, passive smoke [3-4]; these have not been taken into account in the study.
Administrative databases, e.g. CEDAP, Drug Claims Registry and Hospital Information System, may hide some more detail information offered instead by clinical studies.

1. Lanari, M., Giovannini, M., Giuffre, L., Marini, A., Rondini, G., Rossi, G. A., ... & Salvioli, G. P. (2002). Prevalence of respiratory syncytial virus infection in Italian infants hospitalized for acute lower respiratory tract infections, and association between respiratory syncytial virus infection risk factors and disease severity. Pediatric pulmonology, 33(6), 458-465.
2. Medici, M. C., Arcangeletti, M. C., Rossi, G. A., Lanari, M., Merolla, R., Di Luzio Paparatti, U., & Chezzi, C. (2006). Four year incidence of respiratory syncytial virus infection in infants and young children referred to emergency departments for lower respiratory tract diseases in Italy: the" Osservatorio VRS" study (2000-2004). MICROBIOLOGICA-BOLOGNA-, 29(1), 35.
3. Rossi, G. A., Medici, M. C., Arcangeletti, M. C., Lanari, M., Merolla, R., Paparatti, U. D. L., ... & Osservatorio RSV Study Group. (2007). Risk factors for severe RSV-induced lower respiratory tract infection over four consecutive epidemics. European journal of pediatrics, 166(12), 1267-1272.
4. Lanari, M., Giovannini, M., Giuffre, L., Marini, A., Rondini, G., Rossi, G. A., ... & Salvioli, G. P. (2002). Prevalence of respiratory syncytial virus infection in Italian infants hospitalized for acute lower respiratory tract infections, and association between respiratory syncytial virus infection risk factors and disease severity. Pediatric pulmonology, 33(6), 458-465.

Having just read this article I am concerned about the terminology used as I am not sure it truly reflects the clinical problem posed. The article refers to "maintenance" fluids but the question asked relates more to “resuscitation” fluids.

It is important to be clear as to the aim of treatment in the individual patient when prescribing fluids rather than just following a guideline. The paper debates the relative merits of 0.9% sodium chloride and balanced fluids as “maintenance” fluids. To my mind “maintenance” fluids are administered to patients who have a replete extracellular fluid (ECF) volume. If ECF volume is low then “resuscitation” fluids are required. “Maintenance” and “resuscitation” fluids have different roles and therefore might be expected to have different characteristics.

As the article refers to “maintenance” fluids I will deal with these first. This fluid is needed to replicate the fluid that the patient would normally be drinking but for a variety of reasons may not be able to ingest. It should be differentiated in turn from "replacement" fluid which is the fluid given on top of the "maintenance" fluid when patients have fluid losses in excess of those normally anticipated. This includes diarrhoea, vomiting and fluid from surgical drains. The fluid used for "replacement" needs to match the composition and volume of the fluid being lost. Once "resuscitation" and "replacement" fluids have been taken care of and the ECF compartment is full, "maintenance" fluid needs to be prescribed. This equates to insensible water losses and urine output and will be the same as the fluid and electrolytes we take in orally each day. Current guidelines propose the use of a fluid containing 154 mmol/l of sodium. This article questions whether this should be accompanied by chloride or a mix of chloride and potential bicarbonate. However none of us would dream of drinking such a fluid and the recommended sodium intake for infants is around 3 mmol/kg/day which for a 10 kg child given the standard 1 litre of maintenance fluid equates to a solution containing 30 mmol/l or 0.18% sodium chloride. This is the sodium concentration you will find in total parenteral nutrition (TPN). Using 0.9% sodium chloride gives 154 mmol of sodium or 15.4 mmol/kg! The concern about using hypotonic solutions as “maintenance” fluid centres around the notion that the syndrome of inappropriate anti-diuretic hormone secretion (SIADH) is a common phenomenon and administration of hypotonic solutions will cause hyponatraemia. However SIADH is overdiagnosed and when ADH levels are raised it is almost always appropriate i.e. ADH is being produced in response to ECF volume contraction. In that situation an isotonic solution is required. Once ECF volume has been restored ADH production will almost always be switched off and continuing use of isotonic solutions will risk causing hypernatraemia.

The question that should have been asked was which fluid was more appropriate for “resuscitation” purposes? In the scenario described it is the administration of a 20ml/kg bolus of 0.9% sodium chloride that has led to a hyperchloraemic metabolic acidosis. We have recently had this discussion in our department and as in this article, have had to look primarily at evidence from adult studies. At this meeting the use of isotonic crystalloid as "maintenance" fluid was questioned and subsequently we have seen three cases of hypernatraemia as a result of 0.9% sodium chloride “maintenance” therapy.

"Resuscitation" fluid is given to restore ECF volume. To achieve this it would make sense to use a fluid that matches the composition of ECF and unfortunately 0.9% saline only goes part of the way to achieving this. ECF contains 140 mmol/l of sodium, 4 mmol/l of potassium, 113 mmol/l of chloride and 26 mmol/l of bicarbonate and as a result, when using 0.9% sodium chloride to correct a deficit there is an excess of chloride and a lack of bicarbonate. This creates a metabolic acidosis. It therefore makes sense to use balanced fluids containing potential bicarbonate. The studies quoted in this article are primarily related to severely ill patients many with sepsis in whom ongoing problems with ECF volume will be an issue and cannot be extrapolated to children on a general paediatric ward.

In summary, prescription of intravenous fluids should only be made after a careful assessment of the patient, in particular their ECF volume status. If that is reduced an isotonic solution should be administered. A balanced solution makes more sense physiologically but the evidence supporting its use over 0.9% saline is limited, particularly in the paediatric population. If there are ongoing losses they should be replaced by a solution best matching the fluid being lost. If it is not possible to establish the electrolyte content of the fluid losses an isotonic solution is advised. Once ECF volume is replete then a hypotonic solution should be given and on our ward we would use 0.45% saline + 2.5% dextrose. This is still providing more sodium than is normally recommended if giving fluids orally or in TPN. Unfortunately ECF volume status is notoriously difficult to assess and if there is doubt isotonic solutions will be safer. However if 0.9% sodium chloride continues to be administered as "maintenance" fluid we will see more cases of hypernatraemia. Whatever strategy is adopted it is essential to monitor serum electrolytes at least daily in children receiving a significant (>50%) proportion of their fluids intravenously.

I have not mentioned the ongoing debate about the volume of "maintenance" fluid we should be giving children. Currently this is based on recommendations made by Holliday and Segar in the 1950’s, matching fluid requirement to energy expenditure. It is now recognised that these do not reflect the fluid requirements of unwell children lying in bed and as a result “maintenance” fluid volume prescriptions may be twice what they should be. The prescription of more water than is needed is potentially a contributing factor to hypotonic solutions producing hyponatraemia - the prescribing of too much water rather than too little sodium. It is also likely that the cases of hyponatraemia reported in the literature were the result of the prescribing of hypotonic solutions to patients who were deplete of ECF in which case isotonic solutions should have been given.