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Data on the inhibition of cell proliferation and invasion by the D2A-Ala peptide derived from the urokinase receptor

Authors :
Gabriele Eden
Bernard Degryse
Valentina Citro
Ralitsa Arnaudova
Federico Furlan
Marco Archinti
Maria Vittoria Cubellis
Andrea Motta
Giuseppina Andreotti
Furlan, Federico
Eden, Gabriele
Archinti, Marco
Arnaudova, Ralitsa
Andreotti, Giuseppina
Citro, Valentina
Cubellis, Maria Vittoria
Motta, Andrea
Degryse, Bernard
Source :
Data in Brief, Data in brief 22 (2019): 903–908. doi:10.1016/j.dib.2019.01.009, info:cnr-pdr/source/autori:Furlan F.; Eden G.; Archinti M.; Arnaudova R.; Andreotti G.; Citro V.; Cubellis M.V.; Motta A.; Degryse B./titolo:Data on the inhibition of cell proliferation and invasion by the D2A-Ala peptide derived from the urokinase receptor/doi:10.1016%2Fj.dib.2019.01.009/rivista:Data in brief/anno:2019/pagina_da:903/pagina_a:908/intervallo_pagine:903–908/volume:22, Data in Brief, Vol 22, Iss, Pp 903-908 (2019)
Publication Year :
2019
Publisher :
Elsevier, 2019.

Abstract

The data presented in this article are connected to our research article entitled “D2A-Ala peptide derived from the urokinase receptor exerts anti-tumoural effects in vitro and in vivo” (Furlan et al., 2018). These data further extend our understanding of the inhibitory effects of D2A-Ala peptide. Dose-response curve using a wide range of concentrations of D2A-Ala shows that this peptide has no effects per se on proliferation of rat smooth muscle cells (RSMC). However, D2A-Ala dose-dependently inhibits epidermal growth factor (EGF)-induced RSMC proliferation. Kinetics lasting up to seven days revealed that D2A-Ala peptide completely blocked EGF-promoted RSMC proliferation. Moreover, D2A-Ala peptide inhibited invasion of HT 1080 cells towards RSMC. Keywords: Peptide, Urokinase receptor, Cell proliferation, Cell invasion

Details

Language :
English
ISSN :
23523409
Volume :
22
Database :
OpenAIRE
Journal :
Data in Brief
Accession number :
edsair.doi.dedup.....04f01f61f8b210da1ca32a5618e5d450