| Literature DB >> 30703478 |
Giuseppina Focà1, Emanuela Iaccarino1, Annalia Focà1, Luca Sanguigno2, Gustavo Untiveros3, Maria Cuevas-Nunez4, Luigi Strizzi3, Antonio Leonardi2, Menotti Ruvo5, Annamaria Sandomenico6.
Abstract
Human Cripto-1 (Cripto-1), the founding member of the EGF-CFC superfamily, is a key regulator of many processes during embryonic development and oncogenesis. Cripto-1 is barely present or even absent in normal adult tissues while it is aberrantly re-expressed in various tumors. Blockade of the CFC domain-mediated Cripto-1 functions is acknowledged as a promising therapeutic intervention point to inhibit the tumorigenic activity of the protein. In this work, we report the generation and characterization of murine monoclonal antibodies raised against the synthetic folded CFC [112-150] domain of the human protein. Through subtractive ELISA assays clones were screened for the ability to specifically recognize "hot spot" residues on the CFC domain, which are crucial for the interaction with Activin Type I receptor (ALK4) and GRP78. On selected antibodies, SPR and epitope mapping studies have confirmed their specificity and have revealed that recognition occurs only on a conformational epitope. Furthermore, FACS analyses have confirmed the ability of 1B4 antibody to recognize the membrane-anchored and soluble native Cripto-1 protein in a panel of human cancer cells. Finally, we have evaluated its functional effects through in vitro cellular signaling assays and cell cycle analysis. These findings suggest that the selected anti-CFC mAbs have the potential to neutralize the protein oncogenic activity and may be used as theranostic molecules suitable as tumor homing agents for Cripto-1-overexpressing cancer cells and tissues and to overcome drug-resistance in routine cancer therapies.Entities:
Keywords: Cancer biomarker; Cripto-1; Neutralizing monoclonal antibodies
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Year: 2019 PMID: 30703478 DOI: 10.1016/j.biochi.2019.01.016
Source DB: PubMed Journal: Biochimie ISSN: 0300-9084 Impact factor: 4.079