Interferon-β lipofection I. Increased efficacy of chemotherapeutic drugs on human tumor cells derived monolayers and spheroids

Villaverde, Marcela Solange; Gil-Cardeza, María L.; Glikin, Gerardo C.; Finocchiaro, Liliana M.E.

doi:10.1038/cgt.2012.27

Cited by 11 publications

(9 citation statements)

References 34 publications

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“…Many vectors have been employed for the transfer of type I IFN genes, including for modification of tumor cells or DCs (Table 1 ). Among these vectors, adenovirus, AAV and, more recently, non-viral liposome mediated gene transfer have been used in both basic and clinical research protocols [ 306 – 311 ]. Specifically in the case of IFN-α gene transfer, adenovirus is one of the most commonly employed vectors for in situ treatment models, yet lentivirus is better suited for ex vivo creation of IFN-α secreting cells.…”

Section: Type I Ifns In Cancer Gene Therapy: Targeting Tumor and Dendmentioning

confidence: 99%

Immunomodulatory and antitumor effects of type I interferons and their application in cancer therapy

et al. 2017

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During the last decades, the pleiotropic antitumor functions exerted by type I interferons (IFNs) have become universally acknowledged, especially their role in mediating interactions between the tumor and the immune system. Indeed, type I IFNs are now appreciated as a critical component of dendritic cell (DC) driven T cell responses to cancer. Here we focus on IFN-α and IFN-β, and their antitumor effects, impact on immune responses and their use as therapeutic agents. IFN-α/β share many properties, including activation of the JAK-STAT signaling pathway and induction of a variety of cellular phenotypes. For example, type I IFNs drive not only the high maturation status of DCs, but also have a direct impact in cytotoxic T lymphocytes, NK cell activation, induction of tumor cell death and inhibition of angiogenesis. A variety of stimuli, including some standard cancer treatments, promote the expression of endogenous IFN-α/β, which then participates as a fundamental component of immunogenic cell death. Systemic treatment with recombinant protein has been used for the treatment of melanoma. The induction of endogenous IFN-α/β has been tested, including stimulation through pattern recognition receptors. Gene therapies involving IFN-α/β have also been described. Thus, harnessing type I IFNs as an effective tool for cancer therapy continues to be studied.

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Section: Type I Ifns In Cancer Gene Therapy: Targeting Tumor and Dendmentioning

confidence: 99%

Immunomodulatory and antitumor effects of type I interferons and their application in cancer therapy

et al. 2017

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“…Escherichia coli b-galactosidase (bgal: psCMVb), herpes simplex thymidine kinase (psCMVtk), canine interferon-b (psCMVcIFNb), human interleukin-2 (psCMVhIL2), and hGM-CSF (psCMVhGM-CSF) genes were subcloned, amplified, purified, and diluted to a final concentration of 2.0 mg/ml in sterile PBS as described. 8,14 Liposomes preparation and in vivo local lipofection Liposomes for in vitro experiments 12 and liposomes for in vivo injection 8 were made as previously reported. The latest ones were composed of equimolar amounts of 1,2-dimyristyl oxypropyl-3-dimethyl-hydroxyethylammonium bromide (DMRIE) and 1,2-dioleoyl-sn-glycero-3-phosphatidyl ethanolamine (DOPE).…”

Section: Plasmidsmentioning

confidence: 99%

“…12 Regardless the chosen approach, the presence of local disease substantially shortened patients' median overall survival. 8,11,13 In a different background, local expression of interferon-b induced direct tumor cells cytotoxicity both in vitro 14 and in vivo. 15,16 In canine soft tissue sarcoma-and osteosarcoma-bearing patients, we successfully applied a treatment that combined the local antiproliferative effects of interferon-b and HSVtk suicide gene therapy with the systemic effects triggered by a subcutaneous vaccine composed of formolized tumor extracts and irradiated xenogeneic cells genetically modified to slowly release human interleukin-2 (hIL2) and human granulocytemacrophage colony-stimulating factor (hGM-CSF).…”

Section: Introductionmentioning

confidence: 99%

Cytokine-Enhanced Vaccine and Interferon-β plus Suicide Gene Therapy as Surgery Adjuvant Treatments for Spontaneous Canine Melanoma

et al. 2015

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We present here a nonviral immunogene therapy trial for canine malignant melanoma, an aggressive disease displaying significant clinical and histopathological overlapping with human melanoma. As a surgery adjuvant approach, it comprised the co-injection of lipoplexes bearing herpes simplex virus thymidine kinase and canine interferon-b genes at the time of surgery, combined with the periodic administration of a subcutaneous genetic vaccine composed of tumor extracts and lipoplexes carrying the genes of human interleukin-2 and human granulocyte-macrophage colony-stimulating factor. Following complete surgery (CS), the combined treatment (CT) significantly raised the portion of local disease-free canine patients from 11% to 83% and distant metastases-free (M0) from 44% to 89%, as compared with surgery-only-treated controls (ST). Even after partial surgery (PS), CT better controlled the systemic disease (M0: 82%) than ST (M0: 48%). Moreover, compared with ST, CT caused a significant 7-fold (CS) and 4-fold (PS) rise of overall survival, and > 17-fold (CS) and > 13-fold (PS) rise of metastasis-free survival. The dramatic increase of PS metastasis-free survival ( > 1321 days) and CS recurrence-and metastasis-free survival (both > 2251 days) demonstrated that CT was shifting a rapidly lethal disease into a chronic one. In conclusion, this surgery adjuvant CT was able of significantly delaying or preventing postsurgical recurrence and distant metastasis, increasing disease-free and overall survival, and maintaining the quality of life. The high number of canine patients involved in CT (301) and the extensive follow-up ( > 6 years) with minimal or absent toxicity warrant the long-term safety and efficacy of this treatment. This successful clinical outcome justifies attempting a similar scheme for human melanoma.

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“…In support of this hypothesis, the proteomic signature of human tumor spheroids and 3D scaffold models can be readily distinguished from equivalent cells maintained in monolayer culture. This appears to hold true for ES as well, as cells grown within spheroids or 3D scaffolds (natural and synthetic) more closely approximate the protein expression pattern of human tumors than do cell monolayers cells [53, 54, 80, 86, 90]. …”

Section: Applications For Cancer Biology and Preclinical Drug Testingmentioning

confidence: 97%

“…As such, ES spheroids have been used extensively to judge the effectiveness of chemotherapeutic and biologically targeted drugs (Figure 3) [53, 67, 80, 86, 87], to study the impact of cell signaling pathways that regulate ES cell proliferation [53, 80, 88], to investigate the effects of tumor architecture upon immune cell function, and to identify suitable antigens for immunotherapeutic strategies [89, 90]. ES MCTS have also proven useful for modeling micrometastatic disease, contributed to our understanding of anoikis (a form of cell death that results from lost ECM contact) [53, 88], and served as a platform to evaluate heterotypic interactions between tumor cells and vascular progenitor cells responsible for angiogenesis [77].…”

Section: Tumor Structures and Ecm Generation Intrinsic To The Cancmentioning

confidence: 99%

3D tissue-engineered model of Ewing's sarcoma

Lamhamedi-Cherradi

Santoro

Ramammoorthy

et al. 2014

Advanced Drug Delivery Reviews

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Despite longstanding reliance upon monolayer culture for studying cancer cells, and numerous advantages from both a practical and experimental standpoint, a growing body of evidence suggests more complex three-dimensional (3D) models are necessary to properly mimic many of the critical hallmarks associated with the oncogenesis, maintenance and spread of Ewing sarcoma (ES), the second most common pediatric bone tumor. And as clinicians increasingly turn to biologically-targeted therapies that exert their effects not only on the tumor cells themselves, but also on the surrounding extracellular matrix, it is especially important that preclinical models evolve in parallel to reliably measure antineoplastic effects and possible mechanisms of de novo and acquired drug resistance. Herein, we highlight a number of innovative methods used to fabricate biomimetic ES tumors, encompassing both the surrounding cellular milieu and extracellular matrix (ECM), and suggest potential applications to advance our understanding of ES biology, preclinical drug testing, and personalized medicine.

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Interferon-β lipofection I. Increased efficacy of chemotherapeutic drugs on human tumor cells derived monolayers and spheroids

Cited by 11 publications

References 34 publications

Immunomodulatory and antitumor effects of type I interferons and their application in cancer therapy

Immunomodulatory and antitumor effects of type I interferons and their application in cancer therapy

Cytokine-Enhanced Vaccine and Interferon-β plus Suicide Gene Therapy as Surgery Adjuvant Treatments for Spontaneous Canine Melanoma

3D tissue-engineered model of Ewing's sarcoma

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