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Inhibiting mechanotransduction for the treatment of pancreatic cancer

Project description

Blocking mechanical forces between cells and microenvironment for cancer treatment

Mechanical forces between cells and their microenvironment regulate cell functions and are involved in tumorigenesis. The interaction between the cytoskeletal molecules vinculin and talin can be inhibited by a vinculin fragment known as VD1. This blocks cell response to mechanical forces and the activation of oncogene yes-associated protein (YAP) that occurs in tissue with abnormally high mechanical stiffness. The increased tissue stiffness and YAP activation drive tumour progression, meaning that inhibition of talin/vinculin interaction could be a potential therapeutic approach in several solid cancer types. The EU-funded TALVIN project aims to valorise synthetic peptidomimetic drugs, reproducing the action of VD1, in the case of pancreatic cancer.

Objective

Mechanical forces transmitted between cells and their microenvironment drive cell function and regulate tumorigenesis. Due to this importance, our FET PROACTIVE project MECHANOCONTROL aims to understand the molecular mechanisms by which forces exert their role, and their implications in the specific application of breast cancer. In this context, we have recently identified that the interaction between the cytoskeletal molecules vinculin and talin can be inhibited by a vinculin fragment (VD1) which blocks cell response to mechanical forces, and the activation of the major oncogene YAP that occurs in tissues with abnormally high mechanical stiffness. Both increased tissue stiffness and YAP activation drive tumor progression in most solid tumors, and thus inhibiting talin/vinculin interactions has a major potential as a therapeutic approach in several solid cancer types. We have designed and synthesized peptido-mimetic drugs reproducing the action of VD1. Among those synthesized, we have identified one that inhibits the metabolism of cell lines from pancreatic, colon and prostate tumors. Our aim is to valorize these drugs in the specific case of pancreatic cancer, which is a clear unmet clinical need since it is the one with the least therapeutic alternatives and worst prognosis. Specifically, the funding from this project will pay for the national phases of the current patent (PCT/EP2017/056410), regulatory pharmacokinetics/pharmacodynamics and toxicity tests in mouse animal models, as well as for developing contacts of potential license-takers to close a license agreement. Because the focus is on pancreatic rather than breast cancer, and on bringing a specific drug to the market rather than carrying out research, this project is related to but falls out of the scope of the FET MECHANOCONTROL project.

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CSA - Coordination and support action

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Call for proposal

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(opens in new window) H2020-FETOPEN-2016-2017

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Coordinator

FUNDACIO INSTITUT DE BIOENGINYERIA DE CATALUNYA
Net EU contribution

Net EU financial contribution. The sum of money that the participant receives, deducted by the EU contribution to its linked third party. It considers the distribution of the EU financial contribution between direct beneficiaries of the project and other types of participants, like third-party participants.

€ 100 000,00
Address
CARRER BALDIRI REIXAC PLANTA 2A 10-12
08028 Barcelona
Spain

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Region
Este Cataluña Barcelona
Activity type
Research Organisations
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Total cost

The total costs incurred by this organisation to participate in the project, including direct and indirect costs. This amount is a subset of the overall project budget.

€ 100 000,00
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