Host-parasite interaction as a toxicity test endpoint using asymmetrical exposures

Karel Douda; Shuran Zhao; Barbora Vodáková; Pavel Horký; Kateřina Grabicová; Kristýna Božková; Roman Grabic; Ondřej Slavík; Tomáš Randák

doi:10.1016/j.aquatox.2019.04.006

Host-parasite interaction as a toxicity test endpoint using asymmetrical exposures

Aquat Toxicol. 2019 Jun:211:173-180. doi: 10.1016/j.aquatox.2019.04.006. Epub 2019 Apr 8.

Authors

Karel Douda¹, Shuran Zhao², Barbora Vodáková², Pavel Horký², Kateřina Grabicová³, Kristýna Božková², Roman Grabic³, Ondřej Slavík², Tomáš Randák³

Affiliations

¹ Department of Zoology and Fisheries, FAFNR, Czech University of Life Sciences Prague, Kamýcká 129, 165 00 Prague, Czech Republic. Electronic address: k.douda@gmail.com.
² Department of Zoology and Fisheries, FAFNR, Czech University of Life Sciences Prague, Kamýcká 129, 165 00 Prague, Czech Republic.
³ University of South Bohemia in České Budějovice, Faculty of Fisheries and Protection of Waters, South Bohemian Research Center of Aquaculture and Biodiversity of Hydrocenoses, Zátiší 728/II, 389 25 Vodňany, Czech Republic.

PMID: 30991163
DOI: 10.1016/j.aquatox.2019.04.006

Abstract

Interspecific relationships frequently determine the effect a pollutant can have on an organism, and this is especially true in closely interacting species such as hosts and parasites. The high spatial and temporal variability of contaminant concentrations combined with the movement of aquatic biota can further influence the consequences that are associated with contamination. We used a full factorial design for the exposed and unexposed partners of the relationship between the parasitic larvae (glochidia) of the European freshwater mussel (Anodonta anatina) and its host fish (Squalius cephalus) to identify the sources of variation in the sublethal endpoints of species interaction (the intensity of parasite attachment, the spatial position of glochidia on the host body, and encapsulation success). We used the water-borne human pharmaceutical compounds methamphetamine (a central nervous system stimulant) and tramadol (an opioid) at environmentally relevant concentrations (˜ 6.7 and 3.8 nmol L^-1 of methamphetamine and tramadol, respectively) as a proxy for contaminant exposure because these compounds are emerging aquatic stressors that are known for high spatial and temporal variability in their detected concentration levels. The relationship between the bivalve and the fish species was influenced by the preceding contact with both methamphetamine and tramadol, but this effect was highly asymmetric. Our experimental design enabled us to identify the specific changes in the relationship outcome that are elicited by the exposure of individual partners, such as the significant increase in glochidia infection success rate from 59.6 ± 3.9% to 78.7 ± 2.8% (means ± s.e.) that was associated with host exposure to methamphetamine. Additionally, the significant interaction effect of the exposure was demonstrated by the lowered proportion of glochidia attached to gills after the coexposure of both partners to tramadol. The impact of pharmaceuticals on wild aquatic host-parasite relationships provides an example of the risks that are associated with the unintentional discharge of biologically active compounds into freshwater habitats. Given the increasing evidence showing the ecological impact of waste pharmaceuticals, the use of multitrophic interaction endpoints after joint and unilateral exposures provides an important step towards the realistic risk assessment of these compounds.

Keywords: Fish; Freshwater mussels; Glochidia; Interspecific relationships; Methamphetamine; Tramadol.

MeSH terms

Animals
Anodonta / drug effects
Anodonta / growth & development*
Cyprinidae / parasitology*
Environmental Monitoring / methods*
Fresh Water / chemistry
Gills / parasitology
Host-Parasite Interactions / drug effects*
Larva / growth & development
Toxicity Tests
Water Pollutants, Chemical / toxicity*

Substances

Water Pollutants, Chemical