Isolated Peptide from Spider Venom Modulates Dendritic Cells In Vitro: A Possible Application in Oncoimmunotherapy for Glioblastoma

Author:

de Mato Felipe Cezar12,Barreto Natália12ORCID,Cordeiro Gabriel12,Munhoz Jaqueline3ORCID,Bonfanti Amanda Pires12ORCID,da Rocha-e-Silva Thomaz A. A.4,Sutti Rafael5ORCID,Cruz Priscilla B. M.4,Sanches Livia R.4,Bombeiro André Luis2ORCID,Chalbatani Ghanbar Mahmoodi6ORCID,Verinaud Liana2,Rapôso Catarina12

Affiliation:

1. Faculdade de Ciências Farmacêuticas, Universidade Estadual de Campinas (UNICAMP), Campinas 13083-871, SP, Brazil

2. Departamento de Biologia Estrutural e Funcional, Instituto de Biologia, UNICAMP, Campinas 13083-862, SP, Brazil

3. Department of Agricultural, Food and Nutritional Sciences (AFNS), University of Alberta, Edmonton, AB T6G 2R3, Canada

4. Department of Physiological Sciences, Faculdade Israelita de Ciências da Saúde Albert Einstein, São Paulo 05653-120, SP, Brazil

5. Valer Laboratórios Eireli, São Paulo 13347-633, SP, Brazil

6. Department of Immunology, Mayo Clinic, Scottsdale, AZ 85259, USA

Abstract

Dendritic cells (DCs) vaccine is a potential tool for oncoimmunotherapy. However, it is known that this therapeutic strategy has failed in solid tumors, making the development of immunoadjuvants highly relevant. Recently, we demonstrated that Phoneutria nigriventer spider venom (PnV) components are cytotoxic to glioblastoma (GB) and activate macrophages for an antitumor profile. However, the effects of these molecules on the adaptive immune response have not yet been evaluated. This work aimed to test PnV and its purified fractions in DCs in vitro. For this purpose, bone marrow precursors were collected from male C57BL6 mice, differentiated into DCs and treated with venom or PnV-isolated fractions (F1—molecules < 3 kDa, F2—3 to 10 kDa and F3—>10 kDa), with or without costimulation with human GB lysate. The results showed that mainly F1 was able to activate DCs, increasing the activation-dependent surface marker (CD86) and cytokine release (IL-1β, TNF-α), in addition to inducing a typical morphology of mature DCs. From the F1 purification, a molecule named LW9 was the most effective, and mass spectrometry showed it to be a peptide. The present findings suggest that this molecule could be an immunoadjuvant with possible application in DC vaccines for the treatment of GB.

Funder

São Paulo Research Foundation—FAPESP

National Council for Scientific and Technological Development—CNPq;

Education, Research and Extension Support Fund—FAEPEX

Coordination for the Improvement of Higher Education—CAPES

Publisher

MDPI AG

Subject

General Medicine

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