26th January 2022

To the Editor

Archives of Disease in Childhood

re Diagnosing urinary tract infection in children: time to ditch the pad?

Harkensee C, Clennett J, Wilkinson S, et al

Arch Dis Child 2021; 106: 935-936

We read with interest the article by Harkensee et al, (1) suggesting that the urinary collection pad (UCP) no longer had a role in obtaining samples for diagnosis of urinary tract infections (UTI). Whilst it is well established that there is an unacceptably high rate of contamination with UCPs making them unsuitable for microbiological culture, and that the preferred (non-invasive) method for obtaining a sample for culture is by 'clean catch' +/- stimulation or Quick-Wee method, we would suggest that the UCP has a role in screening for UTI, by dipstick analysis of the aspirated pad sample for leucocyte esterase (LE) and nitrites (2). It would be useful, in a paediatric 'acute referral clinic' or Emergency Department, in infants or children, with non-specific abdominal pain, or fever without a focus, where a combination of a negative test for both LE and nitrites can be reasonably used to exclude UTI, and equally a positive LE and nitrite result would indicate a high likelihood of a UTI and the need to obtain a 'clean catch' or catheter specimen for microbiological analysis (3). The advantages of the UCP are that it allows 'point of care' dipstick analysis with information to guide clinical decision-making immediately, is passive with minimal parental effort and disruption to the child, there is less likelihood of missing a sample (compared with 'clean catch') and is the preferred collection method of parents.

Perhaps, it's not time to ditch the pad: pads have a place!

Mervyn S Jaswon

James Diviney

Dept of Paediatrics, Whittington Hospital, London1.Diagnosing urinary tract infection in children: time to ditch the pad?

1.Diagnosing urinary tract infection in children: time to ditch the pad?

   Clennett J, Wilkinson S, et al Arch Dis Child 2021; 106: 935-936

2. Urine collection methods and dipstick testing in non-toilet-trained children.

    Diviney J, Jaswon M S, Pediatric Nephrology 2021; 36; 1697-1708

3. Clinical effectiveness and cost-effectiveness of tests for the diagnosis and investigation of UTI in children: a systematic review and economic model.

    Whiting P, Westwood M, et al HEalth Technol Assess 10:iii-iv, xi-xiii"     "

Dear Editor,

We read with great interest recent study by Vergnano et al.1 investigating the epidemiology, age at infection, clinical characteristics, and outcome of listeria infection in the young infant. We congratulate the authors on providing a novel and interesting study that is relevant to the UK population and agree that the empirical use of amoxicillin in the paediatric infant should be reconsidered given the conclusions of their data.

However, when considering how we might be able to incorporate your novel findings into our centres practice, we required further clarification on table 2. The table describes increased oxygen requirement/respiratory support in 2/27 infants and yet, within results, report a prevalence of increased oxygen requirement/respiratory support of 89%. Furthermore, hypotension requiring inotropes is reported to occur in 4/27 infants but has a reported prevalence of 115%. These reported data appear to be miscalculated.

Clinical identification of invasive listeriosis through the understanding of symptoms within the infant is a key finding of this study given its poor description within the current literature2. We conducted a focused literature search and found scarce information on infant symptom prevalence; one notable exception includes the MONALISA study by Charlier et al.3 which recorded detailed clinical features (appendix p 21). Early diagnosis of invasive listeriosis has been demonstrated to have key prognostic value in the literature4. Consequently, we submit that clearly described clinical presentations, and an understanding of their respective prevalence, could reduce the high mortality associated with invasive listeriosis3 and improve patient outcomes in the future.

Given the relative lack of understanding and the debate within the literature relating to the symptomatic presentation and clinical picture of listeria infection in the infant, especially in a UK population, your article has the potential to clarify clinical signs of useful predictive value. We would be very grateful for clarification on this matter to incorporate into our own practice.

References

1. Vergnano S, Godbole G, Simbo A, et al. Listeria infection in young infants: results from a national surveillance study in the UK and Ireland. Archives of Disease in Childhood 2021;106(12):1207-10. doi: 10.1136/archdischild-2021-321602
2. de Noordhout CM, Devleesschauwer B, Angulo FJ, et al. The global burden of listeriosis: a systematic review and meta-analysis. The Lancet Infectious Diseases 2014;14(11):1073-82. doi: https://doi.org/10.1016/S1473-3099(14)70870-9
3. Charlier C, Perrodeau É, Leclercq A, et al. Clinical features and prognostic factors of listeriosis: the MONALISA national prospective cohort study. The Lancet Infectious Diseases 2017;17(5):510-19. doi: https://doi.org/10.1016/S1473-3099(16)30521-7
4. Hof H. An update on the medical management of listeriosis. Expert Opinion on Pharmacotherapy 2004;5(8):1727-35. doi: 10.1517/14656566.5.8.1727

This review1, listing all the pros and cons of covid vaccinations for children, is to be welcomed but the authors have omitted some important questions on the downside. They rightly state that a large proportion of children might already be immune and point to waning immunity after vaccinations, suggesting that primary infection at young age with boosting exposure over time might be a better strategy. But they do not cite recent evidence that people who are first vaccinated then exposed afterwards, appear to mount brisk IgG response to the spike protein since this is already in their immune memory, but may fail to mount the broader response associated with natural infection, including N-antibodies2. For those children (>75%) already immune, there is no significant benefit to vaccination with an emergency use authorised product. For otherwise healthy children who are not yet immune, they can obtain this by natural infection over the months ahead, at minimal risk to themselves or to the vaccinated adults around them.
Under the heading ‘Long-term safety’, the authors rightly quote concerns of possible ongoing effects of myocarditis, but they make no mention of any other potential as yet unknown effects of these novel technologies. If there are effects on T-cell function, then there is risk for autoimmune diseases3 and also for potential cancer cells4 to pass unchecked. There are also no adequate animal reproductive studies and the nanoparticles have been shown by Pfizer to concentrate in the ovaries and testes5 in rats. These more theoretical risks may be of less concern to adults, particularly those a relatively high risk from covid. But for children, with their whole lives ahead of them, we absolutely must remember the maxim, ‘First do no harm’.
Most importantly, the authors state that, ‘Subjecting children to potential risk of vaccine adverse effects to drive indirect effects with little or no direct benefit might be ethically questionable’. I would contest that is unethical to ask children to take a vaccine to boost herd immunity or to offset political decisions such as school closures, at a stage when the drug trials have still to be completed. Policy makers would do well to re-read the Universal Declaration on Bioethics and Human Rights6 and to follow the authors’ guidance to ‘weigh up the risks and benefits with caution and to proceed with care’.
1. Zimmermann P, Pittet LF, Finn A, et al. Should children be vaccinated against COVID-19? Archives of Disease in Childhood Published Online First: 03 November 2021. https://doi.org/10.1136/archdischild-2021-323040
2. UK Health Security Agency. COVID-19 vaccine surveillance report Week 44 https://assets.publishing.service.gov.uk/government/uploads/system/uploa...
3. Ishay Y, Kenig A, Tsemach-Toren T, et al. Autoimmune phenomena following SARS-CoV-2 vaccination. Int Immunopharmacol. 2021;99:107970. https://doi.org/10.1016/j.intimp.2021.107970
4. Jiang, H, Mei, Y-F. SARS–CoV–2 Spike Impairs DNA Damage Repair and Inhibits V(D)J Recombination In Vitro. Viruses 2021, 13, 2056. https://doi.org/10.3390/v13102056
5. Pfizer biodistribution data. https://www.naturalnews.com/files/Pfizer-bio-distribution-confidential-d...
6. Universal Declaration on Bioethics and Human Rights (2005). http://portal.unesco.org/en/ev.php-URL_ID=31058&URL_DO=DO_TOPIC&URL_SECT...