2020
DOI: 10.3390/ijms21217867
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Doxorubicin Improves Cancer Cell Targeting by Filamentous Phage Gene Delivery Vectors

Abstract: Merging targeted systemic gene delivery and systemic chemotherapy against cancer, chemovirotherapy, has the potential to improve chemotherapy and gene therapy treatments and overcome cancer resistance. We introduced a bacteriophage (phage) vector, named human adeno-associated virus (AAV)/phage or AAVP, for the systemic targeting of therapeutic genes to cancer. The vector was designed as a hybrid between a recombinant adeno-associated virus genome (rAAV) and a filamentous phage capsid. To achieve tumor targetin… Show more

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Cited by 16 publications
(24 citation statements)
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“…GFP lacking the RGD4C mutation, as control for targeting, that we produced with a non‐targeted (NT) M13KO7 helper phage. We subsequently subjected the cell‐lysate to qPCR with primers specific to the AAV‐2 ITRs, 2‐h post‐transduction, as previously reported (Aurnhammer et al , 2012 ; Tsafa et al , 2016 , 2020 ). RGD4C.TPA.…”
Section: Resultsmentioning
confidence: 99%
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“…GFP lacking the RGD4C mutation, as control for targeting, that we produced with a non‐targeted (NT) M13KO7 helper phage. We subsequently subjected the cell‐lysate to qPCR with primers specific to the AAV‐2 ITRs, 2‐h post‐transduction, as previously reported (Aurnhammer et al , 2012 ; Tsafa et al , 2016 , 2020 ). RGD4C.TPA.…”
Section: Resultsmentioning
confidence: 99%
“…Quantification of the ITR cis elements in the cytoplasm and nucleus of cells treated with TPA or AAVP particles was carried out using a modified protocol from previous reports (Aurnhammer et al , 2012 ; Tsafa et al , 2016 , 2020 ). The nuclear and cytosolic fractions isolated from TPA or AAVP‐transduced cells were diluted (1 in 20) in TE buffer, then used as templates for qPCR analysis by using primers specifics for the ITR elements (Table EV2 ).…”
Section: Materials and Methodsmentioning
confidence: 99%
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“…The increase in drug resistance in leukemic cells in high-density cultures was marked earlier [ 50 , 51 ]; however, the mechanism of this phenomena remains unclear. The results of our work show the great increase in the resistance of different AML cells (lines HL-60, THP-1, MV411, U937) in high-density cultures to inhibitors of topoisomerases, etoposide and topotecan [ 52 , 53 ]; an antimetabolite, cytarabine [ 54 ]; DNA targeting antitumor drugs doxorubicin and cisplatin [ 55 , 56 , 57 ]; as well as to antitumor recombinant protein izTRAIL [ 58 ]. It was important that the increase in the drug resistance of AML cells in high-density cell culture was reversible and that the transfer of the AML cells from high-density to low-density cultures decreased the resistance to an initial state.…”
Section: Discussionmentioning
confidence: 99%
“…The suicidal gene cassette codes for an HSVtk enzyme that is known to inhibit cell doubling and subsequently induce target cell death. The authors established an efficient synergistic cancer cell killing by the combined effect of Dox and the suicidal gene by utilizing the phage vector [ 107 ]. In yet another study by the same group, the investigators customized the phage capsid to display the RGD4C ligand on the pIII minor coat proteins for targeting purposes and a human tumor necrosis factor alpha (TNFα) therapeutic transgene was fused into the phage genome.…”
Section: Using Phages To Target and Regulate Tumor And Its Microenvironmentmentioning
confidence: 99%