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Clinical Toxicology Volume 59, 2021 - Issue 4
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Short Communications

The clinical toxicity of imidacloprid self-poisoning following the introduction of newer formulations

Varan Perananthana Royal Prince Alfred Hospital, Drug Health Services, Camperdown, Australia;b The University of Sydney School of Medicine, Sydney, Australia;c Clinical Pharmacology and Toxicology Research Group, Discipline of Pharmacology, Sydney Medical School, University of Sydney, Sydney, AustraliaCorrespondence[email protected]
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Fahim Mohamedc Clinical Pharmacology and Toxicology Research Group, Discipline of Pharmacology, Sydney Medical School, University of Sydney, Sydney, Australia;d South Asian Clinical Toxicology Research Collaboration, Peradeniya, Sri Lanka;e Department of Pharmacy, Faculty of Allied Health Science, University of Peradeniya, Peradeniya, Sri LankaORCID Iconhttps://orcid.org/0000-0003-2849-7269View further author information
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Seyed Shahmyf South Asian Clinical Toxicology Research Collaboration, Faculty of Medicine, University of Peradeniya, Peradeniya, Sri LankaORCID Iconhttps://orcid.org/0000-0002-2339-1572View further author information
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Indika Gawarammanaf South Asian Clinical Toxicology Research Collaboration, Faculty of Medicine, University of Peradeniya, Peradeniya, Sri Lanka;g Faculty of Medicine, University of Peradeniya, Peradeniya, Sri LankaView further author information
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Andrew Dawsona Royal Prince Alfred Hospital, Drug Health Services, Camperdown, Australia;c Clinical Pharmacology and Toxicology Research Group, Discipline of Pharmacology, Sydney Medical School, University of Sydney, Sydney, Australia;h Sydney Medical School, The University of Sydney, Sydney, AustraliaORCID Iconhttps://orcid.org/0000-0002-8047-397XView further author information
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Nicholas Buckleyc Clinical Pharmacology and Toxicology Research Group, Discipline of Pharmacology, Sydney Medical School, University of Sydney, Sydney, Australia;i Pharmacology, Sydney University, Sydney, AustraliaORCID Iconhttps://orcid.org/0000-0002-6326-4711View further author information
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Pages 347-350 | Received 13 Apr 2020, Accepted 23 Aug 2020, Published online: 22 Sep 2020
 
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Abstract

Background

Self-poisoning with imidacloprid has been previously shown to have low toxicity in humans. Since 2007 newer formulations of Imidacloprid with unknown solvents have been introduced and the potential clinical consequences of these products have not been described.

Methods

Clinical and demographic data were prospectively collected from admissions following oral ingestion of imidacloprid from seven hospitals in Sri Lanka. Data was collected from 2002 to 2007 in an already published study. We compared this data on poisonings collected from 2010 to 2016 following the introduction of new formulations of imidacloprid.

Results

From 2002–2007, there were 56 patients with ingestion to imidacloprid compared to 67 patients post 2010 The median time to presentation prior to 2007 was 4 h (IQR 2.3–6.0 hrs) and post 2010 was only 2.0 hr (IQR 1.5 to 3.1 hrs). The median amount ingested was 15 ml (IQR 10.0-50.0mls) prior to 2007 and 27.5mls (IQR 5.0–71.8mls) post 2010. In both studies most patients developed non-specific symptoms including nausea, vomiting, epigastric pain and headache. However, prior to 2007 only 1.9% of the cohort required mechanical ventilation due to respiratory failure and there were no reported deaths. In contrast, post 2010; deaths occurred in 3.0% of the cohort and 6.0% required mechanical ventilation for respiratory failure. The cause of mortality was due to one case of cardiorespiratory failure and the other due to a prolonged admission complicated with lobar pneumonia leading to decompensated liver failure on the background of undiagnosed liver cirrhosis.

Conclusion

Although acute exposure to imidacloprid is usually associated with mild non-specific symptoms, since the introduction of new formulations of imidacloprid, the toxic profile has changed with reported cases of death as well as an increase in cases requiring mechanical ventilation. The change in toxicity could be due to the solvents used in the newer formulations but also due to higher dose of imidacloprid described in our latter cohort. Further research into these solvents needs to be done and continued toxicovigilance is required.

Disclosure statement

No potential conflict of interest was reported by the author(s).

Table 1. General characteristics of both 2002–07 and 2010–16 cohorts [Citation1].

Additional information

Funding

This work is supported by Translational Australian Clinical Toxicology (TACT) program, University of Sydney.

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