Toxicity and membrane perturbation properties of the ribotoxin-like protein Ageritin

Author:

Lampitella Erosantonio1,Landi Nicola2,Oliva Rosario1,Gaglione Rosa13,Bosso Andrea4,De Lise Federica4,Ragucci Sara2,Arciello Angela13,Petraccone Luigi1,Pizzo Elio4,Del Vecchio Pompea1,Di Maro Antimo2

Affiliation:

1. Department of Chemical Sciences, University of Naples ‘Federico II’, Via Cintia, 80126 Napoli, Italy

2. Department of Environmental, Biological and Pharmaceutical Sciences and Technologies (DiSTABiF), University of Campania ‘Luigi Vanvitelli’, Via Vivaldi 43, 81100 Caserta, Italy

3. Istituto Nazionale di Biostrutture e Biosistemi (INBB), Viale delle Medaglie d'Oro 305, 00136 Roma, Italy

4. Department of Biology, University of Naples Federico II, Via Cintia, 80126 Napoli, Italy

Abstract

Abstract Ageritin is the prototype of a new ribotoxin-like protein family, which has been recently identified also in basidiomycetes. The protein exhibits specific RNase activity through the cleavage of a single phosphodiester bond located at sarcin/ricin loop of the large rRNA, thus inhibiting protein biosynthesis at early stages. Conversely to other ribotoxins, its activity requires the presence of divalent cations. In the present study, we report the activity of Ageritin on both prokaryotic and eukaryotic cells showing that the protein has a prominent effect on cancer cells viability and no effects on eukaryotic and bacterial cells. In order to rationalize these findings, the ability of the protein to interact with various liposomes mimicking normal, cancer and bacterial cell membranes was explored. The collected results indicate that Ageritin can interact with DPPC/DPPS/Chol vesicles, used as a model of cancer cell membranes, and with DPPC/DPPG vesicles, used as a model of bacterial cell membranes, suggesting a selective interaction with anionic lipids. However, a different perturbation of the two model membranes, mediated by cholesterol redistribution, was observed and this might be at the basis of Ageritin selective toxicity towards cancer cells.

Funder

University of Naples ‘Federico II’ and University of Campania ‘Luigi Vanvitelli’. Furthermore

Publisher

Oxford University Press (OUP)

Subject

Molecular Biology,Biochemistry,General Medicine

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