Investigating myotoxicity following Australian red-bellied black snake (Pseudechis porphyriacus) envenomation

Suchaya Sanhajariya; Stephen B Duffull; Geoffrey K Isbister

doi:10.1371/journal.pone.0256653

Investigating myotoxicity following Australian red-bellied black snake (Pseudechis porphyriacus) envenomation

PLoS One. 2021 Sep 10;16(9):e0256653. doi: 10.1371/journal.pone.0256653. eCollection 2021.

Authors

Suchaya Sanhajariya^{1

2}, Stephen B Duffull², Geoffrey K Isbister¹

Affiliations

¹ Clinical Toxicology Research Group, University of Newcastle, Newcastle, New South Wales, Australia.
² School of Pharmacy, University of Otago, Dunedin, New Zealand.

Abstract

Background: Myotoxicity is one of the common clinical manifestations of red-bellied black snake (Pseudechis porphyriacus) envenomation characterised by elevated creatine kinase (CK) concentrations of greater than 1000 U/L. This study aimed to investigate the occurrence of myotoxicity in patients following envenomation.

Methods/principal findings: Patient characteristics and serial blood samples (timed venom concentrations and CK concentrations, pre- and post- antivenom) from 114 patients (median age 41, 2-90y; 80 male) were extracted from the Australian Snakebite Project database. Patients were categorised into three groups based on peak CK concentrations [no myotoxicity (<1000 U/L), mild (1000-10,000 U/L) and severe (>10,000 U/L)]. The odds of (mild or severe) myotoxicity was lower in patients that received early antivenom (within 6 hours post-bite) compared to those that received late or no antivenom (odd ratio was 0.186; 95% confidence interval, 0.052-0.664). A population pharmacokinetic-pharmacodynamic (PKPD) model was developed to describe the relationship between the time course of venom (a mixture of toxins) and effect (elevated CK). In addition, a kinetic-pharmacodynamic (KPD) model was developed to describe the relationship between time course of a theoretical toxin and effect. Model development and parameter estimation was performed using NONMEM v7.3. No single set of parameter values from either the PKPD or KPD models were found that could accurately describe the time course of different levels of severity of myotoxicity. The predicted theoretical toxin half-life from the KPD model was 11 ± 3.9 hours compared to the half-life of venom of 5.3 ± 0.36 hours. This indicates that the putative causative toxin's concentration-time profile does not parallel that of venom.

Conclusion: Early antivenom administration reduces the incidence of myotoxicity. The venom concentration profile does not appear to be the driver for myotoxicity following envenomation. Additional factors that affect the sensitivity of the patient to snake venom/toxins must be explored to understand the relationship with myotoxicity.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Adult
Aged
Aged, 80 and over
Antivenins / administration & dosage*
Australia
Child
Child, Preschool
Elapid Venoms* / antagonists & inhibitors
Elapid Venoms* / blood
Female
Humans
Immunologic Factors / administration & dosage*
Male
Middle Aged
Myotoxicity
Neurotoxins* / antagonists & inhibitors
Neurotoxins* / blood
Snake Bites* / drug therapy
Snake Bites* / epidemiology
Young Adult

Substances

Antivenins
Elapid Venoms
Immunologic Factors
Neurotoxins
Pseudechis venom

Grants and funding

SS is supported by the Australian Government Research Training Program Scholarship. GKI is supported by a National Health and Medical Research Council Senior Research Fellowship, ID 1061041. The Australian Snakebite Project is funded by a National Health and Medical Research Council Centre for Research Excellence (ID 1110343).