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    Advanced photodynamic therapy with an engineered M13 phage targeting EGFR: Mitochondrial localization and autophagy induction in ovarian cancer cell lines

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    Advanced photodynamic therapy_FreeRadical.pdf (4.330Mb)
    Date
    2022-02-01
    Author
    Barbara, Bortot
    Apollonio, Maura
    Baj, Gabriele
    Andolfi, Laura
    Zupin, Luisa
    Crovella, Sergio
    di Giosia, Matteo
    Cantelli, Andrea
    Saporetti, Roberto
    Ulfo, Luca
    Petrosino, Annapaola
    Di Lorenzo, Giovanni
    Romano, Federico
    Ricci, Giuseppe
    Mongiat, Maurizio
    Danielli, Alberto
    Calvaresi, Matteo
    Biffi, Stefania
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    Abstract
    Photodynamic therapy (PDT) is a potential synergistic approach to chemotherapy for treating ovarian cancer, the most lethal gynecologic malignancy. Here we used M13 bacteriophage as a targeted vector for the efficient photodynamic killing of SKOV3 and COV362 cells. The M13 phage was refactored (M13r) to display an EGFR binding peptide in its tip that is frequently overexpressed in ovarian cancer. The refactored phage was conjugated with chlorin e6 (Ce6), one of the most widely used photosensitizers (M13r-Ce6). The new platform, upon irradiation, generated ROS by type I mechanism and showed activity in killing SKOV3 and COV362 cells even at concentrations in which Ce6 alone was ineffective. A microscopy analysis demonstrated an enhanced cellular uptake of M13r-Ce6 compared to free Ce6 and its mitochondrial localization. Western blot analysis revealed significant downregulation in the expression of EGFR in cells exposed to M13r-Ce6 after PDT. Following PDT treatment, autophagy induction was supported by an increased expression of LC3II, along with a raised autophagic fluorescent signal, as observed by fluorescence microscopy analysis for autophagosome visualization. As a conclusion we have herein proposed a bacteriophage-based receptor targeted photodynamic therapy for EGFR-positive ovarian cancer.
    URI
    https://www.sciencedirect.com/science/article/pii/S0891584921008169
    DOI/handle
    http://dx.doi.org/10.1016/j.freeradbiomed.2021.11.019
    http://hdl.handle.net/10576/25924
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