Treatment of metastatic neuroblastoma with systemic oncolytic virotherapy delivered by autologous mesenchymal stem cells: an exploratory study

García‐Castro, Javier; Alemany, Ramón; Cascalló, Manel; Martínez-Quintanilla, Jordi; Arriero, Mar; Lassaletta, Álvaro; Madero, Luís; Ramı́rez, Manuel

doi:10.1038/cgt.2010.4

Cited by 126 publications

(99 citation statements)

References 33 publications

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“…The treatment was found to be safe and at 3 months, a bone marrow biopsy indicated a minimal number of tumor cells in a mostly healthy marrow (Pesonen et al, 2010). In the other study, four children with metastatic neuroblastoma refractory to first-line therapies received several doses of autologous mesenchymal stem cells loaded with oncolytic adenovirus (Garcia-Castro et al, 2010). The adenovirus used in this case was an Ad5 virus with an RGD peptide in the fiber knob, which binds to cellular integrin, and it had the 24-bp deleted (D24) E1A gene driven by the E2F-1 promoter.…”

Section: Discussionmentioning

confidence: 96%

“…Oncolytic adenoviruses have already been clinically used at two centers for the treatment of children with metastatic neuroblastoma (Garcia-Castro et al, 2010;Pesonen et al, 2010). In one study, a 6-year-old boy with lymph node and bone marrow metastases was treated by injection of Ad5/3-Cox2LD24 oncolytic adenovirus, which is an Ad5 virus with Ad3 fiber knob and a 24-bp deleted (D24) E1A gene driven by the cyclooxygenase-2 (COX2) promoter.…”

Section: Discussionmentioning

confidence: 99%

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Tat-PTD-Modified Oncolytic Adenovirus Driven by the SCG3 Promoter and ASH1 Enhancer for Neuroblastoma Therapy

Jin

Čančer

et al. 2013

Human Gene Therapy

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Secretogranin III (SGC3) belongs to the granin family and is highly expressed in endocrine and neural tissues. The human SCG3 promoter has not yet been characterized. We identified that a 0.5-kb DNA fragment upstream of the SCG3 gene can selectively drive transgene expression in neuroblastoma cell lines. The strength of transgene expression was further increased, with specificity maintained, by addition of the human achaete-scute complex homolog 1 (ASH1) enhancer. We developed an oncolytic serotype 5-based adenovirus, in which the SCG3 promoter and ASH1 enhancer drive E1A gene expression. The virus was further modified with a cell-penetrating peptide (Tat-PTD) in the viral capsid, which we have previously shown results in increased adenovirus transduction efficiency of many neuroblastoma cell lines. The virus, Ad5PTD(ASH1-SCG3-E1A), shows selective and efficient killing of neuroblastoma cell lines in vitro, including cisplatin-, etoposide-, and doxorubicin-insensitive neuroblastoma cells. Furthermore, it delays tumor growth and thereby prolonged survival for nude mice harboring subcutaneous human neuroblastoma xenograft. In conclusion, we report a novel oncolytic adenovirus with potential use for neuroblastoma therapy.

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Section: Discussionmentioning

confidence: 96%

Section: Discussionmentioning

confidence: 99%

Tat-PTD-Modified Oncolytic Adenovirus Driven by the SCG3 Promoter and ASH1 Enhancer for Neuroblastoma Therapy

Jin

Čančer

et al. 2013

Human Gene Therapy

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show abstract

“…In short duration from now for active immunity against tumor will be introduced by modifying the use of MSCs and NSCs whose aim is the establishment of the safety and efficacy of MSCs that expresses IL-12 (GX-051) and the route of administration of these drugs are intra-tumorally in patients suffering from head and neck cancer. Garcia-Castro and their co-workers demonstrated that using auto-logous MSCs laden with oncolytic adenovirus (ICOVIR-5) in a sample of four children shows efficacy and safety with metastatic neuroblastoma in several doses via infusion administration [223]. A single case was documented about the reduction of disease in a child after three years of therapy.…”

Section: Doorway Of Therapeutic Stem Cells In Clinical Trialsmentioning

confidence: 99%

Development of Anti-Cancer Stem Cells as Theranostic Agents in the Treatment of Different Cancer Types: An Update

Malik¹,

Rasool²,

Khan³

et al. 2017

J Carcinog Mutagen

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Various unprecedented anti-tumor potential targets that robustly target cancer cells while sparing normal cells have been produced by biomedical research in cancer therapeutic intervention for interrupting disease progression and their cure. Stem cells characterize an accessible cell source for novel cell based clinical therapies by inhibiting tumor progression signalling pathways. They carry distinctive characteristics of isolation and migration to tissue inflammation site, inherited modifiability and protein expression. Stem cells are also used in immune-reconstitution and tissue regeneration. Implication of different types of stem cells as an attractive candidate for targeted delivery of anti-neoplastic agents has emerged as a promising field in anticancer therapy. Mutual interaction between cancer cells and stem cells results in effective and safer clinical therapy for tumors. Keeping in view, this review highlights the potential role of stem cells in the progression of tumor metastasis and also summarizes the role of different signaling pathways in carcinogenesis and their involvement in disease treatment. It also focuses on the current advances in stem cells practice in therapeutics of cancer.

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“…MSCs were recruited and migrated into the tumor. In one of the young patients, the virus destroyed enough tumor cells to generate a CD8 cytotoxic response, the tumor disappeared and the patient was free of the disease (Garcia-Castro et al 2010). Improving oncolytic viruses and adjusting the doses of injected MSCs could therefore have potential as be an alternative therapy in some advanced cancers in the future.…”

Section: Clinical Trials Using Cell Therapymentioning

confidence: 99%

Defining stem cell types: understanding the therapeutic potential of ESCs, ASCs, and iPS cells

Álvarez

García-Lavandeira

García-Rendueles

et al. 2012

Journal of Molecular Endocrinology

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Embryonic, adult, artificially reprogrammed, and cancer.-there are various types of cells associated with stemness. Do they have something fundamental in common? Are we applying a common name to very different entities? In this review, we will revisit the characteristics that define 'pluripotency', the main property of stem cells (SCs). For each main type of physiological (embryonic and adult) or synthetic (induced pluripotent) SCs, markers and functional behavior in vitro and in vivo will be described. We will review the pioneering work that has led to obtaining human SC lines, together with the problems that have arisen, both in a biological context (DNA alterations, heterogeneity, tumors, and immunogenicity) and with regard to ethical concerns. Such problems have led to proposals for new operative procedures for growing human SCs of sufficiently high quality for use as models of disease and in human therapy. Finally, we will review the data from the first clinical trials to use various types of SCs.

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Treatment of metastatic neuroblastoma with systemic oncolytic virotherapy delivered by autologous mesenchymal stem cells: an exploratory study

Cited by 126 publications

References 33 publications

Tat-PTD-Modified Oncolytic Adenovirus Driven by the SCG3 Promoter and ASH1 Enhancer for Neuroblastoma Therapy

Tat-PTD-Modified Oncolytic Adenovirus Driven by the SCG3 Promoter and ASH1 Enhancer for Neuroblastoma Therapy

Development of Anti-Cancer Stem Cells as Theranostic Agents in the Treatment of Different Cancer Types: An Update

Defining stem cell types: understanding the therapeutic potential of ESCs, ASCs, and iPS cells

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