Abstract

The antimicrobial peptide (AMP) piscidin was identified from Epinephelus lanceolatus and demonstrated to possess antimicrobial and immune-related functions. Supplementation of feed with recombinant Epinephelus lanceolatus piscidin (rEP)-expressing yeast pellets may minimize the excessive use of antibiotics and control pathogens in aquaculture or animal husbandry. However, before implementing rEP as a supplement, it is necessary to understand whether it harbors any toxicity. Since toxicological information on the topic is scarce, the present investigation was carried out to test whether rEP exhibits allergenic and/or toxic effects. In an oral acute toxicity test (OECD 425), Sprague Dawley (SD) rats were administered rEP dissolved in reverse osmosis water, yielding an LD50 > 5000 mg/kg (no observed animal death). The compound was therefore classified as non-toxic by oral administration. In an acute respiratory toxicity test (OECD 403), heads and noses of SD rats were exposed to liquid aerosol for 4 h (the highest concentration that could be administered without causing any animal death), and a lethal concentration (LC50) > 0.88 mg/L was obtained. The mass medium aerodynamics diameter (MMAD) of rEP aerosol particles was 8.18 μm and mass medium aerodynamics diameter (GSD) was 3.04, which meant that 25.90% could enter the airway (<4 μm) of a rat, and 58.06% (<10 μm) could be inhaled by humans. An ocular irritation test (OECD 405) with rEP powder was performed on New Zealand White (NZW) rabbits. Signs of irritation included conjunctival swelling and diffuse flushing 1 h after administration. The signs were less apparent after 24 h and disappeared after 72 h. The classification assigned to the powder was mild eye irritation. Skin sensitization was performed for a local lymphoproliferative test (OECD 442B) using BALB/c mice, with the highest soluble concentration of the rEP considered to be 100% test substance; formulations were diluted to 50% and 25%, and bromodeoxyuridine (BrdU) incorporation was used to measure the degree of lymphocyte proliferation. The stimulation indexes (SIs) were 1.06 (100%), 0.44 (50%), and 0.77 (25%), all of which were less than the cutoff value for a positive sensitization result (1.6). Negative response was also seen in the bacterial reverse mutation test (OECD 471), and no chromosomal effects on Chinese hamster ovary (CHO)-K1 cells were observed (OECD 487). Based on these six toxicity tests, rEP showed neither acute toxic effects in experimental animals nor mutagenicity. Thus, rEP can be considered safe for use in subsequent research on its application as a feed additive for poultry, cattle, or aquatic animals.

Highlights

  • The emergence of multidrug-resistant pathogens has necessitated the development of antibiotic alternatives to control deadly pathogens in humans and animals [1]

  • The World HealthOrganization (WHO) has defined a category of drug-resistant pathogens (Enterococcus faecium, Staphylococcus aureus, Klebsiella pneumoniae, Acinetobacter baumannii, Pseudomonas aeruginosa, and Enterobacter spp.; abbreviated ESKAPE) that represent the most likely to cause a substantial increase in infectious cases around the globe [3]

  • We have described the isolation, subcloning of the expressed vector, and expression of the piscidin isolated from Epinephelus lanceolatus in Pichia pastoris and identified the biological function of recombinant Epinephelus lanceolatus piscidin (rEP) in Gallus domesticus in our previous research [25]. rEP supplementation increased G. g. domesticus weight gain, feed efficiency, and IL-10 and IFN-γ production

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Summary

Introduction

The emergence of multidrug-resistant pathogens has necessitated the development of antibiotic alternatives to control deadly pathogens in humans and animals [1]. Organization (WHO), an alarming rise in death due to infections with multidrug-resistant pathogens is expected by the middle of this century [2]. Several instances of polymicrobial infections with necrotizing fasciitis have been reported. In this condition, the microbial population feeds on the soft tissues in the infected individual, which may be fatal if left untreated for a sufficient duration [4]. There is an alarming rise in multidrug-resistant and pan-drug-resistant microbial species, along with a drying up of the drug discovery pipeline. Together, these developments have created an emergent need for potential antimicrobial therapeutics [5]. Antimicrobial peptides (AMPs) can be considered as a promising category of therapeutic agents due to their significant antimicrobial activity against drug-resistant pathogens [6]

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