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Antidepressants and their metabolites primarily affect lysosomal functions in the marine mussel, Mytilus galloprovincialis

The Science of The Total Environment 2023 14 citations ? Citation count from OpenAlex, updated daily. May differ slightly from the publisher's own count. Score: 50 ? 0–100 AI score estimating relevance to the microplastics field. Papers below 30 are filtered from public browse.

Marco Capolupo, Marco Capolupo, Marco Capolupo, Marco Capolupo, Ayesha Rafiq, Marco Capolupo, Marco Capolupo, Elena Fabbri Paola Valbonesi, Paola Valbonesi, Marco Capolupo, Marco Capolupo, Giulia Addesse, Elena Fabbri Paola Valbonesi, Giulia Addesse, Paola Valbonesi, Paola Valbonesi, Paola Valbonesi, Paola Valbonesi, Paola Valbonesi, Paola Valbonesi, Paola Valbonesi, Paola Valbonesi, Paola Valbonesi, Elena Fabbri Elena Fabbri Elena Fabbri Elena Fabbri Elena Fabbri Paola Valbonesi, Elena Fabbri Paola Valbonesi, Marco Capolupo, Elena Fabbri Elena Fabbri Elena Fabbri Elena Fabbri

Summary

Researchers tested the effects of four antidepressant drugs and two of their metabolites on Mediterranean mussels at environmentally relevant concentrations. The study found that these pharmaceutical contaminants primarily disrupted lysosomal functions in mussel tissues, and that metabolites like norfluoxetine could be even more potent than their parent compounds, raising concerns about the ecological impact of antidepressant pollution in marine waters.

Body Systems

Digestive Nervous Reproductive

Models

Invertebrate other

Study Type In vivo

Antidepressants widely occur as emerging contaminants in marine coastal waters, with concentrations reported in the low ng/L range. Although at relatively lower levels with respect to other pharmaceuticals, antidepressants - fluoxetine (FLX) in particular - have attracted attention because of their striking effects exerted at low doses on marine invertebrates. In this study, the effects of four antidepressants including FLX, sertraline (SER), and citalopram, as members of the selective serotonin reuptake inhibitor (SSRI) class, and venlafaxine (VEN) as a member of the serotonin and norepinephrine reuptake inhibitor (SNRI) class, were evaluated in the mussel Mytilus galloprovincialis. In addition, the effects of two main metabolites of FLX and VEN, i.e., norfluoxetine (NFL) and O-desmethylvenlafaxine (ODV) respectively, were compared to those of the parent compounds. Eight concentrations of each drug (0.5-500 ng/L range) were tested on the early life stage endpoints of gamete fertilization and larval development at 48 h post fertilization (hpf). Egg fertilization was reduced by all compounds, except for VEN. Larval development at 48 hpf was affected by all SSRIs, but not by SNRIs. The above effects were significant but never exceeded 20 % of control values. Adult mussels were exposed in vivo for 7 days to environmental concentrations of the drugs (0.5, 5, and 10 ng/L) and a battery of eight biomarkers was assessed. Antidepressants primarily targeted lysosomal functions, decreasing haemocyte lysosome membrane stability (up to 70 % reduction) and increasing of the lysosome/cytosol ratio (up to 220 %), neutral lipid (up to 230 %), and lipofuscin (up to 440 %) accumulation in digestive gland. Only SER and NFL significantly affected catalase and glutathione-S-transferase activities in gills and digestive gland. NFL and ODV, were effective and sometimes more active than the parent compounds. All compounds impaired mussel health status, as indicated by the low to high stress levels assigned using the Mussel Expert System.

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