Cell death and barrier disruption by clinically used iodine concentrations

Anne Steins, Christina Carroll, Fui Jiun Choong, Amee J. George, Jin Shu He, Kate M. Parsons, Shouya Feng, Si Ming Man, Cathelijne Kam, Lex M. van Loon, Perlita Poh, Rita Ferreira, Graham J. Mann, Russell L. Gruen, Katherine M. Hannan, Ross D. Hannan, Klaus Martin Schulte*

*Corresponding author for this work

Research output: Contribution to journalArticlepeer-review

2 Citations (Scopus)

Abstract

Povidone-iodine (PVP-I) inactivates a broad range of pathogens. Despite its widespread use over decades, the safety of PVP-I remains controversial. Its extended use in the current SARS-CoV-2 virus pandemic urges the need to clarify safety features of PVP-I on a cellular level. Our investigation in epithelial, mesothelial, endothelial, and innate immune cells revealed that the toxicity of PVP-I is caused by diatomic iodine (I2), which is rapidly released from PVP-I to fuel organic halogenation with fast first-order kinetics. Eukaryotic toxicity manifests at below clinically used concentrations with a threshold of 0.1% PVP-I (wt/vol), equalling 1 mM of total available I2. Above this threshold, membrane disruption, loss of mitochondrial membrane potential, and abolition of oxidative phosphorylation induce a rapid form of cell death we propose to term iodoptosis. Furthermore, PVP-I attacks lipid rafts, leading to the failure of tight junctions and thereby compromising the barrier functions of surface-lining cells. Thus, the therapeutic window of PVP-I is considerably narrower than commonly believed. Our findings urge the reappraisal of PVP-I in clinical practice to avert unwarranted toxicity whilst safeguarding its benefits.

Original languageEnglish
Article numbere202201875
Number of pages10
JournalLife Science Alliance
Volume6
Issue number6
DOIs
Publication statusPublished - 2023

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