Immune response of human cultured cells towards macrocyclic Fe2PO and Fe2PC bioactive cyclophane complexes

Author:

Salazar-Medina Alex J.1,Velazquez-Contreras Enrique F.23,Sugich-Miranda Rocio3,Santacruz Hisila2,Navarro Rosa E.2,Rocha-Alonzo Fernando3,Islas-Osuna Maria A.24ORCID,Chen Patricia L.5,Christian Sarah G.B.5,Romoser Amelia A.6,Dindot Scott V.6,Sayes Christie M.7ORCID,Sotelo-Mundo Rogerio R.8ORCID,Criscitiello Michael F.5ORCID

Affiliation:

1. Cátedra CONACYT-Departamento de Investigación en Polímeros y Materiales, Universidad de Sonora, Hermosillo, Sonora, Mexico

2. Departamento de Investigación en Polímeros y Materiales, Universidad de Sonora, Hermosillo, Sonora, Mexico

3. Departamento de Ciencias Químico Biológicas, Universidad de Sonora, Hermosillo, Sonora, Mexico

4. Centro de Investigación en Alimentación y Desarrollo, A.C., Hermosillo, Sonora, Mexico

5. Comparative Immunogenetics Laboratory, Department of Veterinary Pathobiology, Texas A&M University, College Station, TX, USA

6. Department of Veterinary Pathobiology, Texas A&M University, College Station, TX, USA

7. Nanotoxicology and Nanopharmacology, RTI International, Research Triangle, MC, USA

8. Biomolecular Structure Laboratory, Centro de Investigación en Alimentación y Desarrollo, A.C., Hermosillo, Sonora, Mexico

Abstract

Synthetic molecules that mimic the function of natural enzymes or molecules have untapped potential for use in the next generation of drugs. Cyclic compounds that contain aromatic rings are macrocyclic cyclophanes, and when they coordinate iron ions are of particular interest due to their antioxidant and biomimetic properties. However, little is known about the molecular responses at the cellular level. This study aims to evaluate the changes in immune gene expression in human cells exposed to the cyclophanes Fe2PO and Fe2PC. Confluent human embryonic kidney cells were exposed to either the cyclophane Fe2PO or Fe2PC before extraction of RNA. The expression of a panel of innate and adaptive immune genes was analyzed by quantitative real-time PCR. Evidence was found for an inflammatory response elicited by the cyclophane exposures. After 8 h of exposure, the cells increased the relative expression of inflammatory mediators such as interleukin 1; IRAK, which transduces signals between interleukin 1 receptors and the NFκB pathway; and the LPS pattern recognition receptor CD14. After 24 h of exposure, regulatory genes begin to counter the inflammation, as some genes involved in oxidative stress, apoptosis and non-inflammatory immune responses come into play. Both Fe2PO and Fe2PC induced similar immunogenetic changes in transcription profiles, but equal molar doses of Fe2PC resulted in more robust responses. These data suggest that further work in whole animal models may provide more insights into the extent of systemic physiological changes induced by these cyclophanes.

Funder

Mexico National Research Council for Science and Technology

Basic Science

Texas A&M-CONACYT Collaborative

Universidad de Sonora

Publisher

PeerJ

Subject

General Agricultural and Biological Sciences,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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