Direct antitumoral effects of sulfated fucans isolated from echinoderms: a possible role of neuropilin-1/β1 integrin endocytosis and focal adhesion kinase degradation

Author:

Lima Antonio G F12,Mignone Viviane W1,Vardiero Francisco1,Kozlowski Eliene O2,Fernandes Laila R1,Motta Juliana M2ORCID,Pavão Mauro S G2,Figueiredo Camila C1,Mourão Paulo A S2,Morandi Verônica1ORCID

Affiliation:

1. Laboratório de Biologia da Célula Endotelial e da Angiogênese (LabAngio), Departamento de Biologia Celular/IBRAG, Universidade do Estado do Rio de Janeiro (UERJ) , Rio de Janeiro, 20550-013, Brazil

2. Laboratório do Tecido Conjuntivo, Instituto de Bioquímica Médica (IBqM) - Universidade Federal do Rio de Janeiro (UFRJ), Hospital Universitário Clementino Fraga Filho , Rio de Janeiro, 21941-913, Brazil

Abstract

Abstract Hypercoagulability, a major complication of metastatic cancers, has usually been treated with heparins from natural sources, or with their synthetic derivatives, which are under intense investigation in clinical oncology. However, the use of heparin has been challenging for patients with risk of severe bleeding. While the systemic administration of heparins, in preclinical models, has shown primarily attenuating effects on metastasis, their direct effect on established solid tumors has generated contradictory outcomes. We investigated the direct antitumoral properties of two sulfated fucans isolated from marine echinoderms, FucSulf1 and FucSulf2, which exhibit anticoagulant activity with mild hemorrhagic potential. Unlike heparin, sulfated fucans significantly inhibited tumor cell proliferation (by ~30–50%), and inhibited tumor migration and invasion in vitro. We found that FucSulf1 and FucSulf2 interacted with fibronectin as efficiently as heparin, leading to loss of prostate cancer and melanoma cell spreading. The sulfated fucans increased the endocytosis of β1 integrin and neuropilin-1 chains, two cell receptors implicated in fibronectin-dependent adhesion. The treatment of cancer cells with both sulfated fucans, but not with heparin, also triggered intracellular focal adhesion kinase (FAK) degradation, with a consequent overall decrease in activated focal adhesion kinase levels. Finally, only sulfated fucans inhibited the growth of B16-F10 melanoma cells implanted in the dermis of syngeneic C57/BL6 mice. FucSulf1 and FucSulf2 arise from this study as candidates for the design of possible alternatives to long-term treatments of cancer patients with heparins, with the advantage of also controlling local growth and invasion of malignant cells.

Funder

National Council for Scientific and Technology Development—CNPq

Ministry of Science, Technology and Innovation

Foundation for the Support of Scientific Research of the State of Rio de Janeiro

Rio de Janeiro State Government

National Institutes for Science and Technology for Cancer Control

Coordination for the Improvement of Higher Education Personnel

Publisher

Oxford University Press (OUP)

Subject

Biochemistry

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